Revision as of 06:37, 2 August 2023 editMrfoogles (talk | contribs)Extended confirmed users8,041 edits →Current global policy: Rename headings for clarityTag: Visual edit← Previous edit | Revision as of 06:45, 2 August 2023 edit undoMrfoogles (talk | contribs)Extended confirmed users8,041 edits Move state of research, he jiankui, major studies list under "Research and use" heading; move discussion of clear international regulation out into own section; move global policy list to the bottomTags: Reverted Visual editNext edit → | ||
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==== Detailed description ==== | ==== Detailed description ==== | ||
Embryos for PGD are obtained from IVF procedures in which the oocyte is artificially fertilized by sperm. Oocytes from the woman are harvested following controlled ovarian hyper stimulation (COH), which involves fertility treatments to induce production of multiple oocytes. After harvesting the oocytes, they are fertilized in vitro, either during incubation with multiple sperm cells in culture, or via intracytoplasmic sperm injection(ICSI), where sperm is directly injected into the oocyte.<ref name=":6" /> Such tests include amniocentesis, ultrasounds, and other preimplantation genetic diagnostic tests. These tests are quite common, and reliable, as we talk about them today; however, in the past when they were first introduced, they too were scrutinized.<ref name=":6" /> The resulting embryos are usually cultured for 3–6 days, allowing them to reach the blastomere or blastocyst stage.Once embryos reach the desired stage of development, cells are biopsied and genetically screened. The screening procedure varies based on the nature of the disorder being investigated. | Embryos for PGD are obtained from IVF procedures in which the oocyte is artificially fertilized by sperm. Oocytes from the woman are harvested following controlled ovarian hyper stimulation (COH), which involves fertility treatments to induce production of multiple oocytes. After harvesting the oocytes, they are fertilized in vitro, either during incubation with multiple sperm cells in culture, or via intracytoplasmic sperm injection(ICSI), where sperm is directly injected into the oocyte.<ref name=":6">{{Cite book |last=Stock |first=Gregory |url=https://books.google.com/books?id=XLjJ4AkYWUgC&pg=PR7 |title=Redesigning Humans: Choosing Our Genes, Changing Our Future |date=2003 |publisher=Houghton Mifflin Harcourt |isbn=978-0618340835}}</ref> Such tests include amniocentesis, ultrasounds, and other preimplantation genetic diagnostic tests. These tests are quite common, and reliable, as we talk about them today; however, in the past when they were first introduced, they too were scrutinized.<ref name=":6" /> The resulting embryos are usually cultured for 3–6 days, allowing them to reach the blastomere or blastocyst stage.Once embryos reach the desired stage of development, cells are biopsied and genetically screened. The screening procedure varies based on the nature of the disorder being investigated. | ||
Polymerase chain reaction (PCR) is a process in which DNA sequences are amplified to produce many more copies of the same segment, allowing screening of large samples and identification of specific genes. The process is often used when screening for monogenic disorders, such as cystic fibrosis. | Polymerase chain reaction (PCR) is a process in which DNA sequences are amplified to produce many more copies of the same segment, allowing screening of large samples and identification of specific genes. The process is often used when screening for monogenic disorders, such as cystic fibrosis. | ||
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In a 2019 animal study with Liang Guang Small Spotted pigs, increased muscle mass was achieved with precise editing of the ] signal peptide. Myostatin is a negative regulator of muscle growth, so through mutating the signal peptide regions of the gene, muscle growth could be promoted in the experimental pigs. The Myostatin genes in 955 pig embryos were mutated at several locations with ] and implanted into five surrogates, resulting in 16 piglets. It was found that only specific mutations to the myostatin signal peptide resulted in increased muscle mass in the piglets mainly due to an increase in muscle fibers.<ref>{{Cite journal |last1=Li |first1=Ruiqiang |last2=Zeng |first2=Wu |last3=Ma |first3=Miao |last4=Wei |first4=Zixuan |last5=Liu |first5=Hongbo |last6=Liu |first6=Xiaofeng |last7=Wang |first7=Min |last8=Shi |first8=Xuan |last9=Zeng |first9=Jianhua |last10=Yang |first10=Linfang |last11=Mo |first11=Delin |last12=Liu |first12=Xiaohong |last13=Chen |first13=Yaosheng |last14=He |first14=Zuyong |date=February 2020 |title=Precise editing of myostatin signal peptide by CRISPR/Cas9 increases the muscle mass of Liang Guang Small Spotted pigs |url=http://link.springer.com/10.1007/s11248-020-00188-w |journal=Transgenic Research |language=en |volume=29 |issue=1 |pages=149–163 |doi=10.1007/s11248-020-00188-w |pmid=31927726 |s2cid=255111445 |issn=0962-8819}}</ref> A similar animal study created a knockout in the myostatin gene in mice, which also increased their muscle mass.<ref>{{Cite journal |last=Professor |first=Apostolos Stergioulas, Ph D. |title=Gene doping in modern sport |date=2021-02-04 |url=https://www.biologyofexercise.com/abs_5_1.html |access-date=2022-12-06 |journal=Journal Biology of Exercise |volume=5 |language=en-US |doi=10.4127/jbe.2009.0021}}</ref> This showed that muscle mass could be increased with germline editing, which is likely applicable to humans because humans also have the myostatin gene to regulate muscle growth.<ref>{{Cite journal |last1=Gonzalez-Cadavid |first1=Nestor F. |last2=Taylor |first2=Wayne E. |last3=Yarasheski |first3=Kevin |last4=Sinha-Hikim |first4=Indrani |last5=Ma |first5=Kun |last6=Ezzat |first6=Shereen |last7=Shen |first7=Ruoqing |last8=Lalani |first8=Rukhsana |last9=Asa |first9=Sylvia |last10=Mamita |first10=Mohamad |last11=Nair |first11=Gouri |last12=Arver |first12=Stefan |last13=Bhasin |first13=Shalender |date=1998-12-08 |title=Organization of the human myostatin gene and expression in healthy men and HIV-infected men with muscle wasting |journal=Proceedings of the National Academy of Sciences |language=en |volume=95 |issue=25 |pages=14938–14943 |doi=10.1073/pnas.95.25.14938 |issn=0027-8424 |pmc=24554 |pmid=9843994|doi-access=free }}</ref> Human germline engineering may then result in intentionally increased muscle mass, with applications such as ]. | In a 2019 animal study with Liang Guang Small Spotted pigs, increased muscle mass was achieved with precise editing of the ] signal peptide. Myostatin is a negative regulator of muscle growth, so through mutating the signal peptide regions of the gene, muscle growth could be promoted in the experimental pigs. The Myostatin genes in 955 pig embryos were mutated at several locations with ] and implanted into five surrogates, resulting in 16 piglets. It was found that only specific mutations to the myostatin signal peptide resulted in increased muscle mass in the piglets mainly due to an increase in muscle fibers.<ref>{{Cite journal |last1=Li |first1=Ruiqiang |last2=Zeng |first2=Wu |last3=Ma |first3=Miao |last4=Wei |first4=Zixuan |last5=Liu |first5=Hongbo |last6=Liu |first6=Xiaofeng |last7=Wang |first7=Min |last8=Shi |first8=Xuan |last9=Zeng |first9=Jianhua |last10=Yang |first10=Linfang |last11=Mo |first11=Delin |last12=Liu |first12=Xiaohong |last13=Chen |first13=Yaosheng |last14=He |first14=Zuyong |date=February 2020 |title=Precise editing of myostatin signal peptide by CRISPR/Cas9 increases the muscle mass of Liang Guang Small Spotted pigs |url=http://link.springer.com/10.1007/s11248-020-00188-w |journal=Transgenic Research |language=en |volume=29 |issue=1 |pages=149–163 |doi=10.1007/s11248-020-00188-w |pmid=31927726 |s2cid=255111445 |issn=0962-8819}}</ref> A similar animal study created a knockout in the myostatin gene in mice, which also increased their muscle mass.<ref>{{Cite journal |last=Professor |first=Apostolos Stergioulas, Ph D. |title=Gene doping in modern sport |date=2021-02-04 |url=https://www.biologyofexercise.com/abs_5_1.html |access-date=2022-12-06 |journal=Journal Biology of Exercise |volume=5 |language=en-US |doi=10.4127/jbe.2009.0021}}</ref> This showed that muscle mass could be increased with germline editing, which is likely applicable to humans because humans also have the myostatin gene to regulate muscle growth.<ref>{{Cite journal |last1=Gonzalez-Cadavid |first1=Nestor F. |last2=Taylor |first2=Wayne E. |last3=Yarasheski |first3=Kevin |last4=Sinha-Hikim |first4=Indrani |last5=Ma |first5=Kun |last6=Ezzat |first6=Shereen |last7=Shen |first7=Ruoqing |last8=Lalani |first8=Rukhsana |last9=Asa |first9=Sylvia |last10=Mamita |first10=Mohamad |last11=Nair |first11=Gouri |last12=Arver |first12=Stefan |last13=Bhasin |first13=Shalender |date=1998-12-08 |title=Organization of the human myostatin gene and expression in healthy men and HIV-infected men with muscle wasting |journal=Proceedings of the National Academy of Sciences |language=en |volume=95 |issue=25 |pages=14938–14943 |doi=10.1073/pnas.95.25.14938 |issn=0027-8424 |pmc=24554 |pmid=9843994|doi-access=free }}</ref> Human germline engineering may then result in intentionally increased muscle mass, with applications such as ]. | ||
== |
== Research and use == | ||
⚫ | === State of research === | ||
Human germline engineering is a widely debated topic, and in more than 40 countries, it is formally outlawed.<ref name="NAT-20150312"/> While there is no current legislation explicitly prohibiting germline engineering in the United States, the ''Consolidated Appropriation Act of 2016'' bans the use of ] funds to engage in research regarding human germline modification.<ref>{{cite journal | vauthors = Cohen IG, Adashi EY | title = SCIENCE AND REGULATION. The FDA is prohibited from going germline | journal = Science | volume = 353 | issue = 6299 | pages = 545–6 | date = August 2016 | pmid = 27493171 | doi = 10.1126/science.aag2960 | bibcode = 2016Sci...353..545C | s2cid = 206651381 }}</ref> In April 2015, a research team published an experiment in which they used CRISPR to edit a gene that is associated with blood disease in non-living human embryos. This experiment was unsuccessful, but gene editing tools are used in labs. | Human germline engineering is a widely debated topic, and in more than 40 countries, it is formally outlawed.<ref name="NAT-20150312">{{cite journal |vauthors=Lanphier E, Urnov F, Haecker SE, Werner M, Smolenski J |date=March 2015 |title=Don't edit the human germ line |journal=Nature |volume=519 |issue=7544 |pages=410–1 |bibcode=2015Natur.519..410L |doi=10.1038/519410a |pmid=25810189 |doi-access=free}}</ref> While there is no current legislation explicitly prohibiting germline engineering in the United States, the ''Consolidated Appropriation Act of 2016'' bans the use of ] funds to engage in research regarding human germline modification.<ref>{{cite journal | vauthors = Cohen IG, Adashi EY | title = SCIENCE AND REGULATION. The FDA is prohibited from going germline | journal = Science | volume = 353 | issue = 6299 | pages = 545–6 | date = August 2016 | pmid = 27493171 | doi = 10.1126/science.aag2960 | bibcode = 2016Sci...353..545C | s2cid = 206651381 }}</ref> In April 2015, a research team published an experiment in which they used CRISPR to edit a gene that is associated with blood disease in non-living human embryos. This experiment was unsuccessful, but gene editing tools are used in labs. | ||
Scientists using the CRISPR/cas9 system to modify genetic materials have run into issues when it comes to mammalian alterations due to the complex diploid cells. Studies have been done in microorganisms regarding loss of function genetic screening and some studies have been done using mice as a subject. Because RNA processes differ between bacteria and mammalian cells, scientists have had difficulties coding for mRNA's translated data without the interference of RNA. Studies have been done using the cas9 nuclease that uses a single guide RNA to allow for larger knockout regions in mice, and this was successful.<ref>{{cite journal | last1 = Wang | first1 = Tim | display-authors = etal | year = 2014 | title = Genetic screens in human cells using the CRISPR-Cas9 system | journal = Science | volume = 343 | issue = 6166| pages = 80–4 | doi = 10.1126/science.1246981 | bibcode = 2014Sci...343...80W | pmc = 3972032 | pmid = 24336569 }}</ref> Altering the genetic sequence of mammals is also widely debated, and this creates a difficult FDA regulation standard for such studies. | Scientists using the CRISPR/cas9 system to modify genetic materials have run into issues when it comes to mammalian alterations due to the complex diploid cells. Studies have been done in microorganisms regarding loss of function genetic screening and some studies have been done using mice as a subject. Because RNA processes differ between bacteria and mammalian cells, scientists have had difficulties coding for mRNA's translated data without the interference of RNA. Studies have been done using the cas9 nuclease that uses a single guide RNA to allow for larger knockout regions in mice, and this was successful.<ref>{{cite journal | last1 = Wang | first1 = Tim | display-authors = etal | year = 2014 | title = Genetic screens in human cells using the CRISPR-Cas9 system | journal = Science | volume = 343 | issue = 6166| pages = 80–4 | doi = 10.1126/science.1246981 | bibcode = 2014Sci...343...80W | pmc = 3972032 | pmid = 24336569 }}</ref> Altering the genetic sequence of mammals is also widely debated, and this creates a difficult FDA regulation standard for such studies. | ||
=== |
=== He Jiankui controversy and research === | ||
⚫ | {{Main|He Jiankui affair}} | ||
⚫ | The lack of clear international regulation has led to researchers across the globe attempting to create an international framework of ethical guidelines. Current framework lacks the requisite treaties among nations to create a mechanism for international enforcement. At the first International Summit on Human Gene Editing in December 2015 the collaboration of scientists issued the first international guidelines on genetic research.<ref>{{Cite web|url=http://www8.nationalacademies.org/onpinews/newsitem.aspx?RecordID=12032015a|title=On Human Gene Editing: International Summit Statement|website=www8.nationalacademies.org|access-date=2019-04-18}}</ref> These guidelines allow for the pre-clinical research into the editing of genetic sequences in human cells granted the embryos are not used to implant pregnancy. Genetic alteration of somatic cells for therapeutic proposes was also considered an ethically acceptable field of research in part due to the lack of ability of somatic cells to transfer genetic material to subsequent generations. However citing the lack of social consensus, and the risk of inaccurate gene editing the conference called for restraint on any germline modifications on implanted embryos intended for pregnancy. | ||
⚫ | On 25 November 2018, two days before the Second International Summit on Human Genome Editing in Hong Kong, ], a Chinese researcher of the Southern University of Science and Technology, released a video on YouTube announcing that he and his colleagues have “created” the world’s first genetically altered babies, Lulu and Nana. | ||
⚫ | With the international outcry in response to the first recorded case of human germ line edited embryos being implanted by researcher ], scientists have continued discussion on the best possible mechanism for enforcement of an international framework. On March 13, 2019 researchers ], ], ], ], Paul Bergfrom along with others across the globe published a call for a framework that does not foreclose any outcome but includes a voluntary pledge by nations along with a coordinating body to monitor the application of pledged nations in a moratorium on human germline editing with an attempt to reach social consensus before moving forward into further research.<ref>{{cite journal | title = Germline gene-editing research needs rules | journal = Nature | volume = 567 | issue = 7747 | pages = 145 | date = March 2019 | pmid = 30867612 | doi = 10.1038/d41586-019-00788-5 | bibcode = 2019Natur.567..145. | doi-access = free }}</ref> ] announced on December 18, 2018 plans to convene an intentional committee on clinical germline editing.<ref>{{Cite web|url=https://www.who.int/ethics/topics/human-genome-editing/en/|archive-url=https://web.archive.org/web/20190222155933/https://www.who.int/ethics/topics/human-genome-editing/en/|url-status=dead|archive-date=February 22, 2019|title=WHO {{!}} Gene editing|website=WHO|access-date=2019-04-18}}</ref> | ||
⚫ | He explained the details of his experiment in his address at the Hong Kong conference. He and his team had recruited eight couples through an HIV volunteer group named Baihualin (BHL) China League (one couple later withdrew from the research). All the male participants are HIV-positive, and all female participants are HIV-negative. The participants’ sperm was “washed off” to get rid of HIV and then injected into eggs collected from the female participants. By using clustered regularly interspaced short palindromic repeat (CRISPR)-Cas9, a gene editing technique, they disabled a gene called ] in the embryos, aiming to close the protein doorway that allows HIV to enter a cell and make the subjects immune to the HIV virus. The process led to at least one successful pregnancy and the birth of the twin baby girls, ].<ref name="Statuproar">{{cite news |last1=Begley |first1=Sharon |date=28 November 2018 |title=Amid uproar, Chinese scientist defends creating gene-edited babies |work=STAT News |url=https://www.statnews.com/2018/11/28/chinese-scientist-defends-creating-gene-edited-babies/}}</ref><ref name="sina1127">{{cite web |date=27 November 2018 |title=复盘贺建奎的人生轨迹:是谁给了他勇气 |url=http://news.sina.com.cn/c/2018-11-27/doc-ihpevhck8869227.shtml |access-date=28 November 2018 |publisher=] |language=zh}}</ref> Researcher ] has discovered an impact the ] has on the memory function the brain.<ref>{{Cite web |date=2019-01-21 |title=He Jiankui Fired in Wake of CRISPR Babies Investigation |url=https://www.genengnews.com/news/he-jiankui-fired-in-wake-of-crispr-babies-investigation/ |access-date=2019-04-18 |website=GEN - Genetic Engineering and Biotechnology News}}</ref> | ||
⚫ | == Current global policy == | ||
⚫ | A major concern has been that He Jiankui’s attempts to cripple CCR5, the gene for a protein on immune cells that HIV uses to infect the cells, also made “off-target” changes elsewhere in the girls’ genomes. Those changes could cause cancer or other problems. He contends that the babies have no such off-target mutations, although some scientists are skeptical of the evidence offered so far.<ref>{{Cite web |date=2018-11-28 |title=Amid uproar, Chinese scientist defends creating gene-edited babies |url=https://www.statnews.com/2018/11/28/chinese-scientist-defends-creating-gene-edited-babies/ |access-date=2019-04-18 |website=STAT}}</ref> | ||
⚫ | There is distinction in some country policies, including but not limited to official regulation and legislation, between human germline engineering for reproductive use and for laboratory research. As of October 2020, there are 96 countries that have policies involving the use of germline engineering in human cells.<ref name=":3">{{Cite journal |last1=Baylis |first1=Françoise |last2=Darnovsky |first2=Marcy |last3=Hasson |first3=Katie |last4=Krahn |first4=Timothy M. |date=2020-10-01 |title=Human Germline and Heritable Genome Editing: The Global Policy Landscape |url=https://www.liebertpub.com/doi/10.1089/crispr.2020.0082 |journal=The CRISPR Journal |language=en |volume=3 |issue=5 |pages=365–377 |doi=10.1089/crispr.2020.0082 |pmid=33095042 |s2cid=225053656 |issn=2573-1599}}</ref> | ||
⚫ | People inherit two copies of CCR5, one from each parent. He chose the gene as a target because he knew that about 1% of Northern European populations are born with both copies missing 32 base pairs, resulting in a truncated protein that doesn't reach the cell surface. These people, known as CCR5Δ32 ], appear healthy and are highly resistant to HIV infection. | ||
⚫ | === Reproductive use === | ||
⚫ | In the embryos, He's team designed CRISPR to cut CCR5 at the base pair at one end of the natural deletion. The error-prone cell-repair mechanism, which CRISPR depends on to finish knocking out genes, then deleted 15 base pairs in one of Lulu’s copies of the gene, but none in the other. With one normal CCR5, she is expected to have no protection from HIV. Nana, according to the data He presented in a slide at an international genome-editing summit held in November 2018 in Hong Kong, China, had bases added to one CCR5 copy and deleted from the other, which likely would cripple both genes and provide HIV resistance. | ||
⚫ | Reproductive use of human germline engineering involves implanting the edited embryo to be born. 70 countries currently explicitly prohibit the use of human germline engineering for use in reproduction, while 5 countries prohibit it for reproduction with exceptions. No countries permit the use of human germline engineering for reproduction.<ref name=":3" /> | ||
⚫ | He added the genes for the CRISPR machinery almost immediately after each embryo was created through in vitro fertilization, but several researchers who closely studied the slide caution that it may have done its editing after Nana’s embryo was already past the one-cell stage. That means she could be a genetic “mosaic” who has some unaffected cells with normal CCR5—and ultimately might have no protection from HIV. | ||
⚫ | Countries that explicitly prohibit any use of human germline engineering for reproduction are: ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], the ], the ], ], and the ]<ref name=":3" /> | ||
⚫ | Aside from the primary HIV concerns, the gene edits may have inadvertently altered cognitive function. Researchers showed in 2016 that knocking out one or both CCR5s in mice enhances their memory and cognition. A subsequent study that crippled CCR5 in mice found that, compared with control animals, the mutants recovered from strokes more quickly and had improved motor and cognitive functions following traumatic brain injury. The later study, in the 21 February issue of Cell, also included an analysis of 68 stroke patients who had one copy of CCR5 with the HIV resistance mutation; it concluded they had improved recovery, too. | ||
⚫ | Countries that explicitly prohibit (with exceptions) the use of human germline engineering for reproduction are: ], ], ], ], and the ]<ref name=":3" /> | ||
⚫ | On the night of 26 November, 122 Chinese scientists issued a statement strongly condemning He’s action as unethical. They stated that while CRISPR-Cas is not a new technology, it involves serious off-target risks and associated ethical considerations, and so should not be used to produce gene-altered babies. They described He’s experiment as “crazy” and “a huge blow to the global reputation and development of Chinese science”. The Scientific Ethics Committee of the Academic Divisions of the ] posted a statement declaring their opposition to any clinical use of genome editing on human embryos, noting that “the theory is not reliable, the technology is deficient, the risks are uncontrollable, and ethics and regulations prohibit the action”.<ref name="PC-20150418">{{cite journal |vauthors=Liang P, Xu Y, Zhang X, Ding C, Huang R, Zhang Z, Lv J, Xie X, Chen Y, Li Y, Sun Y, Bai Y, Songyang Z, Ma W, Zhou C, Huang J |date=May 2015 |title=CRISPR/Cas9-mediated gene editing in human tripronuclear zygotes |journal=Protein & Cell |volume=6 |issue=5 |pages=363–372 |doi=10.1007/s13238-015-0153-5 |pmc=4417674 |pmid=25894090}}</ref> The Chinese Academy of Engineering released a statement on 28 November, calling on scientists to improve self-discipline and self-regulation, and to abide by corresponding ethical principles, laws, and regulations. Finally, the Chinese Academy of Medical Sciences published a correspondence in The Lancet, stating that they are “opposed to any clinical operation of human embryo genome editing for reproductive purposes." | ||
⚫ | === |
||
⚫ | Laboratory research use involves human germline engineering restricted to '']'' use, where edited cells will not be implanted to be born. 19 countries currently explicitly prohibit any use of human germline engineering for '']'' use, while 4 prohibit it with exceptions, and 11 permit it.<ref name=":3" /> | ||
⚫ | === Major studies of influence === | ||
⚫ | Countries that explicitly prohibit any use of germline engineering for '']'' use are: ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], and the ]<ref name=":3" /> | ||
⚫ | * The first known publication of research into human germline editing was by a group of Chinese scientists in April 2015 in the Journal "Protein and Cell".<ref name="PC-20150418" /> The scientists used tripronuclear (3PN) zygotes, zygotes fertilized by two sperm and therefore non-viable, to investigate ]-mediated gene editing in human cells, something that had never been attempted before. The scientists found that while ] could effectively cleave the ], the efficiency of homologous recombination directed repair of '']'' was highly inefficient and did not do so in a majority of the trials. Problems arose such as off target cleavage and the competitive recombination of the endogenous delta-globin with the '']'' led to unexpected mutation. The results of the study indicated that repair of '']'' in the embryos occurred preferentially through alternative pathways. In the end only 4 of the 54 zygotes carried the intended genetic information, and even then the successfully edited embryos were mosaics containing the preferential genetic code and the mutation. The conclusion of the scientists was that further effort was needed in to improve the precision and efficiency of ] gene editing. | ||
⚫ | * In March 2017 a group of Chinese scientists claimed to have edited three normal viable human embryos out of six total in the experiment.<ref>{{cite journal |vauthors=Tang L, Zeng Y, Du H, Gong M, Peng J, Zhang B, Lei M, Zhao F, Wang W, Li X, Liu J |date=June 2017 |title=CRISPR/Cas9-mediated gene editing in human zygotes using Cas9 protein |journal=Molecular Genetics and Genomics |volume=292 |issue=3 |pages=525–533 |doi=10.1007/s00438-017-1299-z |pmid=28251317 |s2cid=16358211}}</ref> The study showed that ] is could effectively be used as a gene-editing tool in human 2PN zygotes, which could lead potentially pregnancy viable if implanted. The scientists used injection of Cas9 protein complexed with the relevant sgRNAs and homology donors into human embryos. The scientists found homologous recombination-mediated alteration in '']'' and '']''. The scientists also noted the limitations of their study and called for further research. | ||
⚫ | Countries that explicitly prohibit (with exceptions) the use of germline engineering for '']'' use are: ], ], ], and ]<ref name=":3" /> | ||
⚫ | * In August 2017 a group of scientists from Oregon published an article in ''Nature'' journal detailing the successful use of ] to edit out a mutation responsible for congenital heart disease.<ref>{{cite journal |display-authors=6 |vauthors=Ma H, Marti-Gutierrez N, Park SW, Wu J, Lee Y, Suzuki K, Koski A, Ji D, Hayama T, Ahmed R, Darby H, Van Dyken C, Li Y, Kang E, Park AR, Kim D, Kim ST, Gong J, Gu Y, Xu X, Battaglia D, Krieg SA, Lee DM, Wu DH, Wolf DP, Heitner SB, Belmonte JC, Amato P, Kim JS, Kaul S, Mitalipov S |date=August 2017 |title=Correction of a pathogenic gene mutation in human embryos |journal=Nature |volume=548 |issue=7668 |pages=413–419 |bibcode=2017Natur.548..413M |doi=10.1038/nature23305 |pmid=28783728 |doi-access=free}}</ref> The study looked at heterozygous '']'' mutation in human embryos. The study claimed precise ] and homology-directed repair response with high accuracy and precision. Double-strand breaks at the mutant paternal allele were repaired using the homologous wild-type gene. By modifying the cell cycle stage at which the DSB was induced, they were able to avoid mosaicism, which had been seen in earlier similar studies, in cleaving embryos and achieve a large percentage of homozygous embryos carrying the wild-type '']'' gene without evidence of unintended mutations. The scientists concluded that the technique may be used for the correction of mutations in human embryos. The claims of this study were however pushed back on by critics who argued the evidence was overall unpersuasive. | ||
⚫ | Countries that explicitly permit the use of germline engineering for '']'' use are: ], ], ], ], ], ], ], ], ], the ], and the ]<ref name=":3" /><!-- Global maps would be good to show global policies --> | ||
⚫ | * In June 2018 a group of scientists published and article in "Nature" journal indicating a potential link for edited cells having increased potential turn cancerous.<ref>{{cite journal |vauthors=Haapaniemi E, Botla S, Persson J, Schmierer B, Taipale J |date=July 2018 |title=CRISPR-Cas9 genome editing induces a p53-mediated DNA damage response |journal=Nature Medicine |volume=24 |issue=7 |pages=927–930 |doi=10.1038/s41591-018-0049-z |pmid=29892067 |s2cid=47018050 |hdl-access=free |hdl=10138/303675}}</ref> The scientists reported that genome editing by ] induced DNA damage response and the cell cycle stopped. The study was conducted in human retinal pigment epithelial cells, and the use of ] led to a selection against cells with a functional ] pathway. The conclusion of the study would suggest that ] inhibition might increase efficiency of human germline editing and that ] function would need to be watched when developing ] based therapy. | ||
⚫ | * In November 2018 a group of Chinese scientists published research in the journal "Molecular Therapy" detailing their use of ] technology to correct a single mistaken amino acid successfully in 16 out of 18 attempts in a human embryo.<ref>{{cite journal |vauthors=Zeng Y, Li J, Li G, Huang S, Yu W, Zhang Y, Chen D, Chen J, Liu J, Huang X |date=November 2018 |title=Correction of the Marfan Syndrome Pathogenic FBN1 Mutation by Base Editing in Human Cells and Heterozygous Embryos |url= |journal=Molecular Therapy |language=en |volume=26 |issue=11 |pages=2631–2637 |doi=10.1016/j.ymthe.2018.08.007 |pmc=6224777 |pmid=30166242}}</ref> The unusual level of precision was achieved by the use of a base editor (BE) system which was constructed by fusing the deaminase to the dCas9 protein. The BE system efficiently edits the targeted C to T or G to A without the use of a donor and without DBS formation. The study focused on the ''FBN1'' mutation that is causative for ]. The study provides proof positive for the corrective value of gene therapy for the ''FBN1'' mutation in both somatic cells and germline cells. The study is noted for its relative precision which is a departure from past results of ] studies. | ||
== Lack of clear international regulation == | |||
⚫ | The lack of clear international regulation has led to researchers across the globe attempting to create an international framework of ethical guidelines. Current framework lacks the requisite treaties among nations to create a mechanism for international enforcement. At the first International Summit on Human Gene Editing in December 2015 the collaboration of scientists issued the first international guidelines on genetic research.<ref>{{Cite web|url=http://www8.nationalacademies.org/onpinews/newsitem.aspx?RecordID=12032015a|title=On Human Gene Editing: International Summit Statement|website=www8.nationalacademies.org|access-date=2019-04-18}}</ref> These guidelines allow for the pre-clinical research into the editing of genetic sequences in human cells granted the embryos are not used to implant pregnancy. Genetic alteration of somatic cells for therapeutic proposes was also considered an ethically acceptable field of research in part due to the lack of ability of somatic cells to transfer genetic material to subsequent generations. However citing the lack of social consensus, and the risk of inaccurate gene editing the conference called for restraint on any germline modifications on implanted embryos intended for pregnancy. | ||
⚫ | With the international outcry in response to the first recorded case of human germ line edited embryos being implanted by researcher ], scientists have continued discussion on the best possible mechanism for enforcement of an international framework. On March 13, 2019 researchers ], ], ], ], Paul Bergfrom along with others across the globe published a call for a framework that does not foreclose any outcome but includes a voluntary pledge by nations along with a coordinating body to monitor the application of pledged nations in a moratorium on human germline editing with an attempt to reach social consensus before moving forward into further research.<ref>{{cite journal | title = Germline gene-editing research needs rules | journal = Nature | volume = 567 | issue = 7747 | pages = 145 | date = March 2019 | pmid = 30867612 | doi = 10.1038/d41586-019-00788-5 | bibcode = 2019Natur.567..145. | doi-access = free }}</ref> ] announced on December 18, 2018 plans to convene an intentional committee on clinical germline editing.<ref>{{Cite web|url=https://www.who.int/ethics/topics/human-genome-editing/en/|archive-url=https://web.archive.org/web/20190222155933/https://www.who.int/ethics/topics/human-genome-editing/en/|url-status=dead|archive-date=February 22, 2019|title=WHO {{!}} Gene editing|website=WHO|access-date=2019-04-18}}</ref> | ||
== Ethical and moral debates == | == Ethical and moral debates == | ||
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As it stands, there is controversy surrounding human germline engineering. | As it stands, there is controversy surrounding human germline engineering. | ||
As early in the history of ] as 1990, there have been scientists opposed to attempts to modify the human ] using these new tools,<ref>. cioms.ch</ref> and such concerns have continued as technology progressed.<ref>{{cite journal | |
As early in the history of ] as 1990, there have been scientists opposed to attempts to modify the human ] using these new tools,<ref>. cioms.ch</ref> and such concerns have continued as technology progressed.<ref>{{cite journal |vauthors=Smith KR, Chan S, Harris J |date=October 2012 |title=Human germline genetic modification: scientific and bioethical perspectives |journal=Archives of Medical Research |volume=43 |issue=7 |pages=491–513 |doi=10.1016/j.arcmed.2012.09.003 |pmid=23072719}}</ref><ref>{{cite journal |last1=Reardon |first1=Sara |date=14 February 2017 |title=US science advisers outline path to genetically modified babies |journal=Nature |pages=nature.2017.21474 |doi=10.1038/nature.2017.21474 |doi-access=free}}</ref> With the advent of new techniques like ], in March 2015 a group of scientists urged a worldwide moratorium on clinical use of gene editing technologies to edit the ] in a way that can be inherited.<ref name="NYT-20150319">{{cite news |last=Wade |first=Nicholas |name-list-style=vanc |date=19 March 2015 |title=Scientists Seek Ban on Method of Editing the Human Genome |work=] |url=https://www.nytimes.com/2015/03/20/science/biologists-call-for-halt-to-gene-editing-technique-in-humans.html |access-date=20 March 2015 |quote=The biologists writing in Science support continuing laboratory research with the technique, and few if any scientists believe it is ready for clinical use.}}</ref><ref name="NYT-20150303-AP">{{cite news |last=Pollack |first=Andrew |name-list-style=vanc |date=3 March 2015 |title=A Powerful New Way to Edit DNA |work=] |url=https://www.nytimes.com/2014/03/04/health/a-powerful-new-way-to-edit-dna.html |access-date=20 March 2015}}</ref><ref name="SCI-20150319">{{cite journal |vauthors=Baltimore D, Berg P, Botchan M, Carroll D, Charo RA, Church G, Corn JE, Daley GQ, Doudna JA, Fenner M, Greely HT, Jinek M, Martin GS, Penhoet E, Puck J, Sternberg SH, Weissman JS, Yamamoto KR |date=April 2015 |title=Biotechnology. A prudent path forward for genomic engineering and germline gene modification |journal=Science |volume=348 |issue=6230 |pages=36–8 |bibcode=2015Sci...348...36B |doi=10.1126/science.aab1028 |pmc=4394183 |pmid=25791083}}</ref><ref name="NAT-20150312" /> In April 2015, researchers ] results of ] to edit the ] of non-viable ] using CRISPR, creating controversy.<ref name="PC-20150418" /><ref name="NYT-20150423">{{cite news |last=Kolata |first=Gina |name-list-style=vanc |date=23 April 2015 |title=Chinese Scientists Edit Genes of Human Embryos, Raising Concerns |work=] |url=https://www.nytimes.com/2015/04/24/health/chinese-scientists-edit-genes-of-human-embryos-raising-concerns.html |access-date=24 April 2015}}</ref> A committee of the American ] and ] gave support to human genome editing in 2017<ref>{{Cite news |last=Harmon |first=Amy |name-list-style=vanc |date=2017-02-14 |title=Human Gene Editing Receives Science Panel's Support |newspaper=The New York Times |url=https://www.nytimes.com/2017/02/14/health/human-gene-editing-panel.html |access-date=2017-02-17 |issn=0362-4331}}</ref><ref>{{cite web |last1=Committee on Human Gene Editing: Scientific, Medical, and Ethical Considerations |title=Human Genome Editing: Science, Ethics, and Governance |url=http://nationalacademies.org/gene-editing/consensus-study/index.htm |access-date=21 February 2017 |website=nationalacademies.org |publisher=National Academy of Sciences; National Academy of Medicine}}</ref> once answers have been found to safety and efficiency problems "but only for serious conditions under stringent oversight."<ref>{{Cite web |date=2017-02-14 |title=Scientists OK genetically engineering babies |url=https://nypost.com/2017/02/14/scientists-ok-genetically-engineering-babies/ |access-date=2017-02-17 |website=New York Post |publisher=Reuters}}</ref> | ||
Editing the genes of human embryos raises its own social and ethical concerns. The scientific community, and global community, have division regarding whether or not human germline engineering should be practiced or not. It is currently banned in many of the leading, developed countries, and highly regulated in the others due to ethical issues.<ref>{{cite journal |last1=Krause |first1=Kenneth W. |title=Editing the Human Germline: Groundbreaking Science and Mind-Numbing Sentiment |journal=] |
Editing the genes of human embryos raises its own social and ethical concerns. The scientific community, and global community, have division regarding whether or not human germline engineering should be practiced or not. It is currently banned in many of the leading, developed countries, and highly regulated in the others due to ethical issues.<ref>{{cite journal |last1=Krause |first1=Kenneth W. |date=2017 |title=Editing the Human Germline: Groundbreaking Science and Mind-Numbing Sentiment |journal=] |volume=41 |issue=6 |pages=29–31}}</ref> | ||
The ]’s Council on Ethical and Judicial Affairs stated that "genetic interventions to enhance traits should be considered permissible only in severely restricted situations: (1) clear and meaningful benefits to the fetus or child; (2) no trade-off with other characteristics or traits; and (3) equal access to the genetic technology, irrespective of income or other socioeconomic characteristics."<ref>{{cite journal | |
The ]’s Council on Ethical and Judicial Affairs stated that "genetic interventions to enhance traits should be considered permissible only in severely restricted situations: (1) clear and meaningful benefits to the fetus or child; (2) no trade-off with other characteristics or traits; and (3) equal access to the genetic technology, irrespective of income or other socioeconomic characteristics."<ref>{{cite journal |date=July 1994 |title=Ethical issues related to prenatal genetic testing. The Council on Ethical and Judicial Affairs, American Medical Association |journal=Archives of Family Medicine |volume=3 |issue=7 |pages=633–642 |doi=10.1001/archfami.3.7.633 |pmid=7921302}}</ref> | ||
Ethical claims about germline engineering include beliefs that every ] has a right to remain genetically unmodified, that parents hold the right to genetically modify their offspring, and that every child has the right to be born free of preventable diseases.<ref name="Evolution">{{cite journal | |
Ethical claims about germline engineering include beliefs that every ] has a right to remain genetically unmodified, that parents hold the right to genetically modify their offspring, and that every child has the right to be born free of preventable diseases.<ref name="Evolution">{{cite journal |vauthors=Powell R, Buchanan A |date=February 2011 |title=Breaking evolution's chains: the prospect of deliberate genetic modification in humans |journal=The Journal of Medicine and Philosophy |volume=36 |issue=1 |pages=6–27 |doi=10.1093/jmp/jhq057 |pmid=21228084}}</ref><ref name="Baylis, Francoise 2004">{{cite journal |vauthors=Baylis F, Robert JS |year=2004 |title=The inevitability of genetic enhancement technologies |journal=Bioethics |volume=18 |issue=1 |pages=1–26 |doi=10.1111/j.1467-8519.2004.00376.x |pmid=15168695}}</ref><ref>{{cite book |last=Evans |first=John |title=Playing God?: Human Genetic Engineering and the Rationalization of Public Bioethical Debate |publisher=University of Chicago Press |year=2002 |isbn=978-0-226-22262-2 |name-list-style=vanc}}</ref> For parents, genetic engineering could be seen as another child enhancement technique to add to diet, exercise, education, training, cosmetics, and plastic surgery.<ref name="Enhancement"> {{webarchive|url=https://web.archive.org/web/20131203040308/http://ethics.missouri.edu/Gene-Therapy.aspx|date=3 December 2013}} The Center for Health Ethics, University of Missouri School of Medicine. 25 April 2013.</ref><ref name="Roco_Bainbridge_2002">{{cite journal |vauthors=Roco MC, Bainbridge WS |year=2002 |title=Converging Technologies for Improving Human Performance: Integrating From the Nanoscale |journal=Journal of Nanoparticle Research |volume=4 |issue=4 |pages=281–295 |bibcode=2002JNR.....4..281R |doi=10.1023/A:1021152023349 |s2cid=136290217}}</ref> Another theorist claims that moral concerns limit but do not prohibit germline engineering.<ref>{{cite journal |last1=Allhoff |first1=Fritz |date=2005 |title=Germ-Line Genetic Enhancement and Rawlsian Primary Goods |journal=Kennedy Institute of Ethics Journal |volume=15 |issue=1 |pages=39–56 |citeseerx=10.1.1.566.171 |doi=10.1353/ken.2005.0007 |pmid=15881795 |s2cid=14432440}}</ref> | ||
One issue related to human genome editing relates to the impact of the technology on future individuals whose genes are modified without their consent. Clinical ethics accepts the idea that parents are, almost always, the most appropriate surrogate medical decision makers for their children until the children develop their own autonomy and decision-making capacity. This is based on the assumption that, except under rare circumstances, parents have the most to lose or gain from a decision and will ultimately make decisions that reflects the future values and beliefs of their children. According to this assumption, it could be assumed that parents are the most appropriate decision makers for their future children as well. There are anecdotal reports of children and adults who disagree with the medical decisions made by a parent during pregnancy or early childhood, such as when death was a possible outcome. There are also published patient stories by individuals who feel that they would not wish to change or remove their own medical condition if given the choice and individuals who disagree with medical decisions made by their parents during childhood.<ref name=":4">{{cite journal | |
One issue related to human genome editing relates to the impact of the technology on future individuals whose genes are modified without their consent. Clinical ethics accepts the idea that parents are, almost always, the most appropriate surrogate medical decision makers for their children until the children develop their own autonomy and decision-making capacity. This is based on the assumption that, except under rare circumstances, parents have the most to lose or gain from a decision and will ultimately make decisions that reflects the future values and beliefs of their children. According to this assumption, it could be assumed that parents are the most appropriate decision makers for their future children as well. There are anecdotal reports of children and adults who disagree with the medical decisions made by a parent during pregnancy or early childhood, such as when death was a possible outcome. There are also published patient stories by individuals who feel that they would not wish to change or remove their own medical condition if given the choice and individuals who disagree with medical decisions made by their parents during childhood.<ref name=":4">{{cite journal |vauthors=Ishii T |date=August 2014 |title=Potential impact of human mitochondrial replacement on global policy regarding germline gene modification |journal=Reproductive Biomedicine Online |volume=29 |issue=2 |pages=150–5 |doi=10.1016/j.rbmo.2014.04.001 |pmid=24832374 |doi-access=free}}</ref> | ||
Other scientists and philosophers have noted that the issue of the lack of prior consent applies as well to individuals born via traditional sexual reproduction.<ref>{{cite journal |last1=Ranisch |first1=Robert |title=Germline Genome Editing and the Functions of Consent |journal=The American Journal of Bioethics |
Other scientists and philosophers have noted that the issue of the lack of prior consent applies as well to individuals born via traditional sexual reproduction.<ref>{{cite journal |last1=Ranisch |first1=Robert |date=2 December 2017 |title=Germline Genome Editing and the Functions of Consent |journal=The American Journal of Bioethics |volume=17 |issue=12 |pages=27–29 |doi=10.1080/15265161.2017.1388875 |pmid=29148947 |s2cid=10117287}}</ref><ref>{{cite journal |last1=Vassena |first1=R. |last2=Heindryckx |first2=B. |last3=Peco |first3=R. |last4=Pennings |first4=G. |last5=Raya |first5=A. |last6=Sermon |first6=K. |last7=Veiga |first7=A. |date=June 2016 |title=Genome engineering through CRISPR/Cas9 technology in the human germline and pluripotent stem cells |journal=Human Reproduction Update |volume=22 |issue=4 |pages=411–419 |doi=10.1093/humupd/dmw005 |pmid=26932460}}</ref> Philosopher ] further argues that “old-fashioned sexual reproduction is itself an untested genetic experiment”, often compromising a child’s wellbeing and pro-social capacities even if the child grows in a healthy environment. According to Pearce, “the question of comes down to an analysis of risk-reward ratios - and our basic ethical values, themselves shaped by our evolutionary past.”<ref>{{Cite book |last=Pearce |first=David |title=Can Biotechnology Abolish Suffering? |year=2017 |editor-last=Vinding |editor-first=Magnus |chapter=The Reproductive Revolution |asin=B075MV9KS2 |author-link=David Pearce (transhumanist)}}</ref> Bioethicist ] in turn proposes the principle of ], according to which “couples (or single reproducers) should select the child, of the possible children they could have, who is expected to have the best life, or at least as good a life as the others, based on the relevant, available information”.<ref>{{cite journal |last1=Savulescu |first1=Julian |date=October 2001 |title=Procreative Beneficence: Why We Should Select the Best Children |journal=Bioethics |volume=15 |issue=5–6 |pages=413–426 |doi=10.1111/1467-8519.00251 |pmid=12058767}}</ref> Some ethicists argue that the principle of procreative beneficence would justify or even require ] one's children.<ref>{{Cite journal |last=Veit |first=Walter |date=2018 |title=Procreative Beneficence and Genetic Enhancement |url=http://www.kriterion-journal-of-philosophy.org/kriterion/issues/Permanent/Kriterion-veit-01.pdf |journal=KRITERION - Journal of Philosophy |volume=32 |pages=75–92 |doi=10.1515/krt-2018-320105 |s2cid=149244361 |archive-url=https://web.archive.org/web/20211023193825/http://www.kriterion-journal-of-philosophy.org/kriterion/issues/Permanent/Kriterion-veit-01.pdf |archive-date=October 23, 2021}}</ref><ref>{{cite journal |last1=Daws |first1=Steven |date=6 October 2017 |title=Procreative Beneficence in the CRISPR World |journal=Voices in Bioethics |volume=3 |doi=10.7916/vib.v3i.6031}}</ref> | ||
The other ethical concern is the potential for “designer babies”, or the creation of humans with "perfect", or "desirable" traits. There is a debate as to if this is morally acceptable as well. Such debate ranges from the ethical obligation to use safe and efficient technology to prevent disease to seeing some actual benefit in genetic disabilities. | The other ethical concern is the potential for “designer babies”, or the creation of humans with "perfect", or "desirable" traits. There is a debate as to if this is morally acceptable as well. Such debate ranges from the ethical obligation to use safe and efficient technology to prevent disease to seeing some actual benefit in genetic disabilities. | ||
There are concerns that the introduction of desirable traits in a certain part of the population (instead of the entire population) could cause economic inequalities (“positional” good){{Clarify|Aren't there already many positional goods as for example poor people may not always be able to pay treatments in hospitals? Also, doesn't exercising also cause beneficial changes in the DNA which is possed on, again causing a genetic positional good, but without genetic editing|date=October 2020}}.<ref>{{cite news |last1=Johnson |first1=Tess |title=Human genetic enhancement might soon be possible – but where do we draw the line? |url=https://theconversation.com/human-genetic-enhancement-might-soon-be-possible-but-where-do-we-draw-the-line-127406 |
There are concerns that the introduction of desirable traits in a certain part of the population (instead of the entire population) could cause economic inequalities (“positional” good){{Clarify|Aren't there already many positional goods as for example poor people may not always be able to pay treatments in hospitals? Also, doesn't exercising also cause beneficial changes in the DNA which is possed on, again causing a genetic positional good, but without genetic editing|date=October 2020}}.<ref>{{cite news |last1=Johnson |first1=Tess |date=3 December 2019 |title=Human genetic enhancement might soon be possible – but where do we draw the line? |work=The Conversation |url=https://theconversation.com/human-genetic-enhancement-might-soon-be-possible-but-where-do-we-draw-the-line-127406}}</ref> However, this isn't the case if a same desirable trait would be ] (similar to vaccines).{{Cn|date=July 2023}}<!-- What about the introduction of parents of "undesirable traits" into their DNA (i.e. by bad habits as smoking, drinking alcohol, excessive eating, lack of exercise. All of these genetic defects thus produced may be inheritable (see epigenetics). Even the choice of the partner influences the genetic makeup in either a good or bad way -see Mendelian laws- (and since most people don't choose a partner based on their genetic makeup (genetic sequencing), this always results in a choice that is not optimal. All of this too is legally allowed, and seemingly uncontroversial. It's not mentioned here yet--> | ||
Several religious positions have been published with regards to human germline engineering. According to them, many see germline modification as being more moral than the alternative, which would be either discarding of the embryo, or birth of a diseased human. The main conditions when it comes to whether or not it is morally and ethically acceptable lie within the intent of the modification, and the conditions in which the engineering is done. | Several religious positions have been published with regards to human germline engineering. According to them, many see germline modification as being more moral than the alternative, which would be either discarding of the embryo, or birth of a diseased human. The main conditions when it comes to whether or not it is morally and ethically acceptable lie within the intent of the modification, and the conditions in which the engineering is done. | ||
The process of modifying the human genome has raised ethical questions. One of the issues is “off target effects”, large genomes may contain identical or homologous DNA sequences, and the enzyme complex CRISPR/Cas9 may unintentionally cleave these DNA sequences causing mutations that may lead to cell death. The mutations can cause important genes to be turned on or off, such as genetic anti-cancer mechanisms, that could speed up disease exasperation.<ref name=":4" /><ref name=":5">{{Cite book|url=https://books.google.com/books?id=E3qsPJb44Q8C&pg=PR7 |title=Design and Destiny: Jewish and Christian Perspectives on Human Germline Modification |
The process of modifying the human genome has raised ethical questions. One of the issues is “off target effects”, large genomes may contain identical or homologous DNA sequences, and the enzyme complex CRISPR/Cas9 may unintentionally cleave these DNA sequences causing mutations that may lead to cell death. The mutations can cause important genes to be turned on or off, such as genetic anti-cancer mechanisms, that could speed up disease exasperation.<ref name=":4" /><ref name=":5">{{Cite book |last=Cole-Turner |first=Ronald |url=https://books.google.com/books?id=E3qsPJb44Q8C&pg=PR7 |title=Design and Destiny: Jewish and Christian Perspectives on Human Germline Modification |date=2008 |publisher=MIT Press |isbn=9780262533010}}</ref><ref name=":6" /><ref name=":7">{{cite journal |last1=Wivel |first1=Nelson A. |last2=Walters |first2=LeRoy |date=22 October 1993 |title=Germ-Line Gene Modification and Disease Prevention: Some Medical and Ethical Perspectives |journal=Science |volume=262 |issue=5133 |pages=533–538 |doi=10.1126/science.8211180 |pmid=8211180 |id={{Gale|A14296431}} {{ProQuest|213545041}}}}</ref><ref name=":8">{{cite journal |last1=Darnovsky |first1=Marcy |date=July 2013 |title=A slippery slope to human germline modification |journal=Nature |volume=499 |issue=7457 |pages=127 |doi=10.1038/499127a |pmid=23846625 |s2cid=4430248 |id={{ProQuest|1415758114}}}}</ref><ref>{{Cite journal |last1=Alanis-Lobato |first1=Gregorio |last2=Zohren |first2=Jasmin |last3=McCarthy |first3=Afshan |last4=Fogarty |first4=Norah M. E. |last5=Kubikova |first5=Nada |last6=Hardman |first6=Emily |last7=Greco |first7=Maria |last8=Wells |first8=Dagan |last9=Turner |first9=James M. A. |last10=Niakan |first10=Kathy K. |date=June 2021 |title=Frequent loss of heterozygosity in CRISPR-Cas9–edited early human embryos |journal=Proceedings of the National Academy of Sciences |language=en |volume=118 |issue=22 |pages=e2004832117 |doi=10.1073/pnas.2004832117 |issn=0027-8424 |pmc=8179174 |pmid=34050011 |doi-access=free}}</ref> | ||
Other ethical concerns are: unintentionally editing the human germline forever, not knowing how one change to a human germline will affect the expression of the remainder of the genes. A scientist recently made an analogy to increase understanding in regard to mapping and manipulating the human genome / germline in relation to a stage play: it is if we have very precise character descriptions (the mapped genome), and yet we (the scientific community) have no idea yet how the characters interact with each other. In other words, if one makes one change to the human germline, what other cascade of changes might we be making?<ref name="Newson & Wrigley 2016">{{cite journal |last1=Newson |first1=Ainsley |last2=Wrigley |first2=Anthony |title=Being human: The ethics, law, and scientific progress of genome editing |journal=AQ - Australian Quarterly |
Other ethical concerns are: unintentionally editing the human germline forever, not knowing how one change to a human germline will affect the expression of the remainder of the genes. A scientist recently made an analogy to increase understanding in regard to mapping and manipulating the human genome / germline in relation to a stage play: it is if we have very precise character descriptions (the mapped genome), and yet we (the scientific community) have no idea yet how the characters interact with each other. In other words, if one makes one change to the human germline, what other cascade of changes might we be making?<ref name="Newson & Wrigley 2016">{{cite journal |last1=Newson |first1=Ainsley |last2=Wrigley |first2=Anthony |date=2016 |title=Being human: The ethics, law, and scientific progress of genome editing |url=https://search.informit.org/doi/abs/10.3316/agispt.20190516010395 |journal=AQ - Australian Quarterly |volume=87 |issue=1 |pages=3–8 |id={{Gale|A441491350}} {{ProQuest|2046113711}}}}</ref><ref>{{cite web |title=Sickle Cell Anemia: Stem Cell Therapy – Donald Kohn |url=https://www.youtube.com/watch?v=3vbrC6mAS5A |access-date=20 February 2020 |website=YouTube |publisher=California Institute for Regenerative Medicine}}</ref> | ||
Another ethical concern pertains to potential unequal distribution of benefits, even in the case of genome editing being inexpensive. For example, corporations may be able to take unfair advantage of patent law or other ways of restricting access to genome editing and thereby may increase the inequalities. There are already disputes in the courts where CRISPR-Cas9 patents and access issues are being negotiated.<ref name="Newson & Wrigley 2016"/> | Another ethical concern pertains to potential unequal distribution of benefits, even in the case of genome editing being inexpensive. For example, corporations may be able to take unfair advantage of patent law or other ways of restricting access to genome editing and thereby may increase the inequalities. There are already disputes in the courts where CRISPR-Cas9 patents and access issues are being negotiated.<ref name="Newson & Wrigley 2016" /> | ||
There remains debate on if the permissibility of human germline engineering for reproduction is dependent on the use, being either a therapeutic or non-therapeutic application. In a survey by the UK's Royal Society, 76% of participants in the UK supported therapeutic human germline engineering to prevent or correct disease, however for non-therapeutic edits such as enhancing intelligence or altering eye or hair color in embryos, there was only 40% and 31% support, respectively.<ref name=":10" /> There was a similar result in a study at the ], Colombia, where students as well as professors generally agreed that therapeutic genome editing is acceptable, while non-therapeutic genome editing is not.<ref name=":11" /> | There remains debate on if the permissibility of human germline engineering for reproduction is dependent on the use, being either a therapeutic or non-therapeutic application. In a survey by the UK's Royal Society, 76% of participants in the UK supported therapeutic human germline engineering to prevent or correct disease, however for non-therapeutic edits such as enhancing intelligence or altering eye or hair color in embryos, there was only 40% and 31% support, respectively.<ref name=":10" /> There was a similar result in a study at the ], Colombia, where students as well as professors generally agreed that therapeutic genome editing is acceptable, while non-therapeutic genome editing is not.<ref name=":11" /> | ||
There is also debate on if there can be a defined distinction between therapeutic and non-therapeutic germline editing. An example would be if two embryos are predicted to grow up to be very short in height. Boy 1 will be short because of a mutation in his Human Growth Hormone gene, while boy 2 will be short because his parents are very short. Editing the embryo of boy 1 to make him of average height would be a therapeutic germline edit, while editing the embryo of boy 2 to be of average height would be a non-therapeutic germline edit. In both cases with no editing of the boys' genomes they would both grow up to be very short, which would decrease their wellbeing in life. Likewise editing both of the boys' genomes would allow them to grow up to be of average height. In this scenario, editing for the same phenotype for being of average height falls under both therapeutic and non-therapeutic germline engineering.<ref>{{Cite journal |last1=Greene |first1=Marsha |last2=Master |first2=Zubin |date=2018-09-01 |title=Ethical Issues of Using CRISPR Technologies for Research on Military Enhancement |url=https://doi.org/10.1007/s11673-018-9865-6 |journal=Journal of Bioethical Inquiry |language=en |volume=15 |issue=3 |pages=327–335 |doi=10.1007/s11673-018-9865-6 |pmid=29968018 |s2cid=49640190 |
There is also debate on if there can be a defined distinction between therapeutic and non-therapeutic germline editing. An example would be if two embryos are predicted to grow up to be very short in height. Boy 1 will be short because of a mutation in his Human Growth Hormone gene, while boy 2 will be short because his parents are very short. Editing the embryo of boy 1 to make him of average height would be a therapeutic germline edit, while editing the embryo of boy 2 to be of average height would be a non-therapeutic germline edit. In both cases with no editing of the boys' genomes they would both grow up to be very short, which would decrease their wellbeing in life. Likewise editing both of the boys' genomes would allow them to grow up to be of average height. In this scenario, editing for the same phenotype for being of average height falls under both therapeutic and non-therapeutic germline engineering.<ref>{{Cite journal |last1=Greene |first1=Marsha |last2=Master |first2=Zubin |date=2018-09-01 |title=Ethical Issues of Using CRISPR Technologies for Research on Military Enhancement |url=https://doi.org/10.1007/s11673-018-9865-6 |journal=Journal of Bioethical Inquiry |language=en |volume=15 |issue=3 |pages=327–335 |doi=10.1007/s11673-018-9865-6 |issn=1872-4353 |pmid=29968018 |s2cid=49640190}}</ref> | ||
⚫ | == Current global policy == | ||
== He Jiankui controversy and research == | |||
⚫ | There is distinction in some country policies, including but not limited to official regulation and legislation, between human germline engineering for reproductive use and for laboratory research. As of October 2020, there are 96 countries that have policies involving the use of germline engineering in human cells.<ref name=":3">{{Cite journal |last1=Baylis |first1=Françoise |last2=Darnovsky |first2=Marcy |last3=Hasson |first3=Katie |last4=Krahn |first4=Timothy M. |date=2020-10-01 |title=Human Germline and Heritable Genome Editing: The Global Policy Landscape |url=https://www.liebertpub.com/doi/10.1089/crispr.2020.0082 |journal=The CRISPR Journal |language=en |volume=3 |issue=5 |pages=365–377 |doi=10.1089/crispr.2020.0082 |pmid=33095042 |s2cid=225053656 |issn=2573-1599}}</ref> | ||
⚫ | === Reproductive use === | ||
⚫ | {{Main|He Jiankui affair}} | ||
⚫ | Reproductive use of human germline engineering involves implanting the edited embryo to be born. 70 countries currently explicitly prohibit the use of human germline engineering for use in reproduction, while 5 countries prohibit it for reproduction with exceptions. No countries permit the use of human germline engineering for reproduction.<ref name=":3" /> | ||
⚫ | Countries that explicitly prohibit any use of human germline engineering for reproduction are: ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], the ], the ], ], and the ]<ref name=":3" /> | ||
⚫ | On 25 November 2018, two days before the Second International Summit on Human Genome Editing in Hong Kong, ], a Chinese researcher of the Southern University of Science and Technology, released a video on YouTube announcing that he and his colleagues have “created” the world’s first genetically altered babies, Lulu and Nana. | ||
⚫ | Countries that explicitly prohibit (with exceptions) the use of human germline engineering for reproduction are: ], ], ], ], and the ]<ref name=":3" /> | ||
⚫ | He explained the details of his experiment in his address at the Hong Kong conference. He and his team had recruited eight couples through an HIV volunteer group named Baihualin (BHL) China League (one couple later withdrew from the research). All the male participants are HIV-positive, and all female participants are HIV-negative. The participants’ sperm was “washed off” to get rid of HIV and then injected into eggs collected from the female participants. By using clustered regularly interspaced short palindromic repeat (CRISPR)-Cas9, a gene editing technique, they disabled a gene called ] in the embryos, aiming to close the protein doorway that allows HIV to enter a cell and make the subjects immune to the HIV virus. The process led to at least one successful pregnancy and the birth of the twin baby girls, ].<ref name=Statuproar>{{cite news |last1=Begley |first1=Sharon |title=Amid uproar, Chinese scientist defends creating gene-edited babies|url=https://www.statnews.com/2018/11/28/chinese-scientist-defends-creating-gene-edited-babies/ |
||
⚫ | A major concern has been that He Jiankui’s attempts to cripple CCR5, the gene for a protein on immune cells that HIV uses to infect the cells, also made “off-target” changes elsewhere in the girls’ genomes. Those changes could cause cancer or other problems. He contends that the babies have no such off-target mutations, although some scientists are skeptical of the evidence offered so far.<ref>{{Cite web|url=https://www.statnews.com/2018/11/28/chinese-scientist-defends-creating-gene-edited-babies/ |
||
=== Laboratory research === | |||
⚫ | People inherit two copies of CCR5, one from each parent. He chose the gene as a target because he knew that about 1% of Northern European populations are born with both copies missing 32 base pairs, resulting in a truncated protein that doesn't reach the cell surface. These people, known as CCR5Δ32 ], appear healthy and are highly resistant to HIV infection. | ||
⚫ | Laboratory research use involves human germline engineering restricted to '']'' use, where edited cells will not be implanted to be born. 19 countries currently explicitly prohibit any use of human germline engineering for '']'' use, while 4 prohibit it with exceptions, and 11 permit it.<ref name=":3" /> | ||
⚫ | In the embryos, He's team designed CRISPR to cut CCR5 at the base pair at one end of the natural deletion. The error-prone cell-repair mechanism, which CRISPR depends on to finish knocking out genes, then deleted 15 base pairs in one of Lulu’s copies of the gene, but none in the other. With one normal CCR5, she is expected to have no protection from HIV. Nana, according to the data He presented in a slide at an international genome-editing summit held in November 2018 in Hong Kong, China, had bases added to one CCR5 copy and deleted from the other, which likely would cripple both genes and provide HIV resistance. | ||
⚫ | Countries that explicitly prohibit any use of germline engineering for '']'' use are: ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], ], and the ]<ref name=":3" /> | ||
⚫ | He added the genes for the CRISPR machinery almost immediately after each embryo was created through in vitro fertilization, but several researchers who closely studied the slide caution that it may have done its editing after Nana’s embryo was already past the one-cell stage. That means she could be a genetic “mosaic” who has some unaffected cells with normal CCR5—and ultimately might have no protection from HIV. | ||
⚫ | Countries that explicitly prohibit (with exceptions) the use of germline engineering for '']'' use are: ], ], ], and ]<ref name=":3" /> | ||
⚫ | Aside from the primary HIV concerns, the gene edits may have inadvertently altered cognitive function. Researchers showed in 2016 that knocking out one or both CCR5s in mice enhances their memory and cognition. A subsequent study that crippled CCR5 in mice found that, compared with control animals, the mutants recovered from strokes more quickly and had improved motor and cognitive functions following traumatic brain injury. The later study, in the 21 February issue of Cell, also included an analysis of 68 stroke patients who had one copy of CCR5 with the HIV resistance mutation; it concluded they had improved recovery, too. | ||
⚫ | Countries that explicitly permit the use of germline engineering for '']'' use are: ], ], ], ], ], ], ], ], ], the ], and the ]<ref name=":3" /><!-- Global maps would be good to show global policies --> | ||
⚫ | On the night of 26 November, 122 Chinese scientists issued a statement strongly condemning He’s action as unethical. They stated that while CRISPR-Cas is not a new technology, it involves serious off-target risks and associated ethical considerations, and so should not be used to produce gene-altered babies. They described He’s experiment as “crazy” and “a huge blow to the global reputation and development of Chinese science”. The Scientific Ethics Committee of the Academic Divisions of the ] posted a statement declaring their opposition to any clinical use of genome editing on human embryos, noting that “the theory is not reliable, the technology is deficient, the risks are uncontrollable, and ethics and regulations prohibit the action”.<ref name="PC-20150418"/> The Chinese Academy of Engineering released a statement on 28 November, calling on scientists to improve self-discipline and self-regulation, and to abide by corresponding ethical principles, laws, and regulations. Finally, the Chinese Academy of Medical Sciences published a correspondence in The Lancet, stating that they are “opposed to any clinical operation of human embryo genome editing for reproductive purposes." | ||
⚫ | == Major studies of influence == | ||
⚫ | * The first known publication of research into human germline editing was by a group of Chinese scientists in April 2015 in the Journal "Protein and Cell".<ref name="PC-20150418" /> The scientists used tripronuclear (3PN) zygotes, zygotes fertilized by two sperm and therefore non-viable, to investigate ]-mediated gene editing in human cells, something that had never been attempted before. The scientists found that while ] could effectively cleave the ], the efficiency of homologous recombination directed repair of '']'' was highly inefficient and did not do so in a majority of the trials. Problems arose such as off target cleavage and the competitive recombination of the endogenous delta-globin with the '']'' led to unexpected mutation. The results of the study indicated that repair of '']'' in the embryos occurred preferentially through alternative pathways. In the end only 4 of the 54 zygotes carried the intended genetic information, and even then the successfully edited embryos were mosaics containing the preferential genetic code and the mutation. The conclusion of the scientists was that further effort was needed in to improve the precision and efficiency of ] gene editing. | ||
⚫ | * In March 2017 a group of Chinese scientists claimed to have edited three normal viable human embryos out of six total in the experiment.<ref>{{cite journal | |
||
⚫ | * In August 2017 a group of scientists from Oregon published an article in ''Nature'' journal detailing the successful use of ] to edit out a mutation responsible for congenital heart disease.<ref>{{cite journal | vauthors |
||
⚫ | * In June 2018 a group of scientists published and article in "Nature" journal indicating a potential link for edited cells having increased potential turn cancerous.<ref>{{cite journal | |
||
⚫ | * In November 2018 a group of Chinese scientists published research in the journal "Molecular Therapy" detailing their use of ] technology to correct a single mistaken amino acid successfully in 16 out of 18 attempts in a human embryo.<ref>{{cite journal | |
||
== See also == | == See also == |
Revision as of 06:45, 2 August 2023
Process of editing the human genomeThis article may require copy editing for grammar, style, cohesion, tone, or spelling. You can assist by editing it. (July 2023) (Learn how and when to remove this message) |
Human germline engineering is the process by which the genome of an individual is edited in such a way that the change is heritable. This is achieved by altering the genes of the germ cells, which then mature into genetically modified eggs and sperm. For safety, ethical, and social reasons, there is broad agreement among the scientific community and the public that germline editing for reproduction is a red line that should not be crossed at this point in time. There are differing public sentiments, however, on whether it may be performed in the future depending on whether the intent would be therapeutic or non-therapeutic.
Using germline editing for reproduction is prohibited by law in more than 70 countries and by a binding international treaty of the Council of Europe. However, in November 2015, a group of Chinese scientists used the gene-editing technique CRISPR/Cas9 to edit single-celled, non-viable embryos to see the effectiveness of this technique. This attempt was rather unsuccessful; only a small fraction of the embryos successfully incorporated the new genetic material and many of the embryos contained a large number of random mutations. The non-viable embryos that were used contained an extra set of chromosomes, which may have been problematic. In 2016, another similar study was performed in China which also used non-viable embryos with extra sets of chromosomes. This study showed very similar results to the first; there were successful integrations of the desired gene, yet the majority of the attempts failed, or produced undesirable mutations.
In an experiment in August 2017, the correction of the heterozygous MYBPC3 mutation associated with hypertrophic cardiomyopathy in human embryos was attempted with precise CRISPR–Cas9 targeting. 52% of human embryos were successfully edited to retain only the wild type normal copy of MYBPC3 gene, the rest of the embryos were mosaic, where some cells in the zygote contained the normal gene copy and some contained the mutation.
In November 2018, researcher He Jiankui claimed that he had created the first human genetically edited babies, known by their pseudonyms, Lulu and Nana. In May 2019, lawyers in China reported, in light of the purported creation by He Jiankui of the first gene-edited humans, the drafting of regulations that anyone manipulating the human genome by gene-editing techniques, like CRISPR, would be held responsible for any related adverse consequences.
Techniques
CRISPR-cas9
Main articles: CRISPR and Cas9In general, CRISPR-Cas9 is the most effective gene-editing technique to date. The CRISPR-Cas9 system consists of an enzyme called Cas9 and a special piece of guide RNA (gRNA). Cas9 acts as a pair of ‘molecular scissors’ that can cut the DNA at a specific location in the genome so that DNA can be added or removed. The guide RNA is a piece of RNA with complementary bases to those at the target location, so that it will only bind there and no other regions of the genome. The Cas9 follows the guide RNA to the same location in the DNA sequence and makes a cut across both strands of the DNA. At this stage the cell recognizes that the DNA is damaged and tries to repair it. Scientists can use the DNA repair machinery to introduce changes to one or more genes in the genome of a cell of interest.
Although the CRISPR/Cas9 can be used in humans, it is more commonly used by scientists in other animal models or cell culture systems, including in experiments to learn more about genes that could be involved in human diseases. Clinical trials are being conducted on somatic cells, but CRISPR could make it possible to modify the DNA of spermatogonial stem cells. This could be used to eliminate certain diseases in humans, or at least significantly decrease a disease's frequency until it eventually disappears over generations. Cancer survivors theoretically would be able to have their genes modified by the CRISPR/cas9 so that certain diseases or mutations will not be passed down to their offspring. This could possibly eliminate cancer predispositions in humans. Researchers hope that they can use the system in the future to treat currently incurable diseases by altering the genome altogether.
PGD
A genetically modified human contains a genetic makeup that has been selected or altered, often to include a particular gene or to remove genes associated with disease. This process usually involves analyzing human embryos to identify genes associated with disease, and selecting embryos that have the desired genetic makeup - a process known as PGD, or Preimplantation Genetic Diagnosis. IVF, or in vitro fertilization, is ofted used to obtain embryos for evaluation of the genome – alternatively, oocytes can be screened prior to fertilization. The technique was first used in 1989.
PGD is used primarily to select embryos for implantation in the case of possible genetic defects, allowing identification of mutated or disease-related alleles and selection against them. It is especially useful in embryos from parents where one or both carry a heritable disease. PGD can also be used to select for embryos of a certain sex, most commonly when a disease is more strongly associated with one sex than the other (as is the case for X-linked disorders which are more common in males, such as hemophilia). Infants born with traits selected following PGD are sometimes considered to be designer babies.
One application of PGD is the selection of ‘savior siblings’, children who are born to provide a transplant (of an organ or group of cells) to a sibling with a usually life-threatening disease. Savior siblings are conceived through IVF and then screened using PGD to analyze genetic similarity to the child needing a transplant, in order to reduce the risk of rejection.
Detailed description
Embryos for PGD are obtained from IVF procedures in which the oocyte is artificially fertilized by sperm. Oocytes from the woman are harvested following controlled ovarian hyper stimulation (COH), which involves fertility treatments to induce production of multiple oocytes. After harvesting the oocytes, they are fertilized in vitro, either during incubation with multiple sperm cells in culture, or via intracytoplasmic sperm injection(ICSI), where sperm is directly injected into the oocyte. Such tests include amniocentesis, ultrasounds, and other preimplantation genetic diagnostic tests. These tests are quite common, and reliable, as we talk about them today; however, in the past when they were first introduced, they too were scrutinized. The resulting embryos are usually cultured for 3–6 days, allowing them to reach the blastomere or blastocyst stage.Once embryos reach the desired stage of development, cells are biopsied and genetically screened. The screening procedure varies based on the nature of the disorder being investigated. Polymerase chain reaction (PCR) is a process in which DNA sequences are amplified to produce many more copies of the same segment, allowing screening of large samples and identification of specific genes. The process is often used when screening for monogenic disorders, such as cystic fibrosis.
Another screening technique, fluorescent in situ hybridization (FISH) uses fluorescent probes which specifically bind to highly complementary sequences on chromosomes, which can then be identified using fluorescence microscopy. FISH is often used when screening for chromosomal abnormalities such as aneuploidy, making it a useful tool when screening for disorders such as Down syndrome.
Following screening, embryos with the desired trait (or lacking an undesired trait such as a mutation) are transferred into the mother's uterus, then allowed to develop naturally.
Conceivable uses
Human germline engineering could be used to heritably cure genetic disorders and other diseases, and to give specific traits to human babies. For example, The Berlin Patient has a genetic mutation in the CCR5 gene (which codes for a protein on the surface of white blood cells, targeted by the HIV virus) that deactivates the expression of CCR5, conferring innate resistance to HIV. HIV/AIDS carries a large disease burden and is incurable (see Epidemiology of HIV/AIDS). One proposal is to genetically modify human embryos to give the CCR5 Δ32 allele to people.
Another use would be to cure genetic disorders. In the first study published regarding human germline engineering, the researchers attempted to edit the HBB gene which codes for the human β-globin protein. Mutations in the HBB gene result in the disorder β-thalassaemia, which can be fatal. Perfect editing of the genome in patients who have these HBB mutations would result in copies of the gene which do not possess any mutations, effectively curing the disease. If the germline could be edited, this normal copy of the HBB genes could be passed on to future generations.
Designer babies
The non-therapeutic use of human germline engineering would be eugenic modifications to humans which would result in what are known as "designer babies". The concept of a "designer baby" is that its entire genetic composition could be selected for. In an extreme case, people would be able to effectively create the offspring that they want, with a genotype of their choosing. Not only does human germline engineering allow for the selection of specific traits, but it also allows for enhancement of these traits. Using human germline editing for selection and enhancement is currently very heavily scrutinized, and the main driving force behind the movement of trying to ban human germline engineering.
In a 2019 animal study with Liang Guang Small Spotted pigs, increased muscle mass was achieved with precise editing of the myostatin signal peptide. Myostatin is a negative regulator of muscle growth, so through mutating the signal peptide regions of the gene, muscle growth could be promoted in the experimental pigs. The Myostatin genes in 955 pig embryos were mutated at several locations with CRISPR and implanted into five surrogates, resulting in 16 piglets. It was found that only specific mutations to the myostatin signal peptide resulted in increased muscle mass in the piglets mainly due to an increase in muscle fibers. A similar animal study created a knockout in the myostatin gene in mice, which also increased their muscle mass. This showed that muscle mass could be increased with germline editing, which is likely applicable to humans because humans also have the myostatin gene to regulate muscle growth. Human germline engineering may then result in intentionally increased muscle mass, with applications such as gene doping.
Research and use
State of research
Human germline engineering is a widely debated topic, and in more than 40 countries, it is formally outlawed. While there is no current legislation explicitly prohibiting germline engineering in the United States, the Consolidated Appropriation Act of 2016 bans the use of US FDA funds to engage in research regarding human germline modification. In April 2015, a research team published an experiment in which they used CRISPR to edit a gene that is associated with blood disease in non-living human embryos. This experiment was unsuccessful, but gene editing tools are used in labs.
Scientists using the CRISPR/cas9 system to modify genetic materials have run into issues when it comes to mammalian alterations due to the complex diploid cells. Studies have been done in microorganisms regarding loss of function genetic screening and some studies have been done using mice as a subject. Because RNA processes differ between bacteria and mammalian cells, scientists have had difficulties coding for mRNA's translated data without the interference of RNA. Studies have been done using the cas9 nuclease that uses a single guide RNA to allow for larger knockout regions in mice, and this was successful. Altering the genetic sequence of mammals is also widely debated, and this creates a difficult FDA regulation standard for such studies.
He Jiankui controversy and research
Main article: He Jiankui affairOn 25 November 2018, two days before the Second International Summit on Human Genome Editing in Hong Kong, He Jiankui, a Chinese researcher of the Southern University of Science and Technology, released a video on YouTube announcing that he and his colleagues have “created” the world’s first genetically altered babies, Lulu and Nana.
He explained the details of his experiment in his address at the Hong Kong conference. He and his team had recruited eight couples through an HIV volunteer group named Baihualin (BHL) China League (one couple later withdrew from the research). All the male participants are HIV-positive, and all female participants are HIV-negative. The participants’ sperm was “washed off” to get rid of HIV and then injected into eggs collected from the female participants. By using clustered regularly interspaced short palindromic repeat (CRISPR)-Cas9, a gene editing technique, they disabled a gene called CCR5 in the embryos, aiming to close the protein doorway that allows HIV to enter a cell and make the subjects immune to the HIV virus. The process led to at least one successful pregnancy and the birth of the twin baby girls, Lulu and Nana. Researcher Alcino J. Silva has discovered an impact the CCR5 gene has on the memory function the brain. A major concern has been that He Jiankui’s attempts to cripple CCR5, the gene for a protein on immune cells that HIV uses to infect the cells, also made “off-target” changes elsewhere in the girls’ genomes. Those changes could cause cancer or other problems. He contends that the babies have no such off-target mutations, although some scientists are skeptical of the evidence offered so far.
People inherit two copies of CCR5, one from each parent. He chose the gene as a target because he knew that about 1% of Northern European populations are born with both copies missing 32 base pairs, resulting in a truncated protein that doesn't reach the cell surface. These people, known as CCR5Δ32 homozygotes, appear healthy and are highly resistant to HIV infection. In the embryos, He's team designed CRISPR to cut CCR5 at the base pair at one end of the natural deletion. The error-prone cell-repair mechanism, which CRISPR depends on to finish knocking out genes, then deleted 15 base pairs in one of Lulu’s copies of the gene, but none in the other. With one normal CCR5, she is expected to have no protection from HIV. Nana, according to the data He presented in a slide at an international genome-editing summit held in November 2018 in Hong Kong, China, had bases added to one CCR5 copy and deleted from the other, which likely would cripple both genes and provide HIV resistance.
He added the genes for the CRISPR machinery almost immediately after each embryo was created through in vitro fertilization, but several researchers who closely studied the slide caution that it may have done its editing after Nana’s embryo was already past the one-cell stage. That means she could be a genetic “mosaic” who has some unaffected cells with normal CCR5—and ultimately might have no protection from HIV.
Aside from the primary HIV concerns, the gene edits may have inadvertently altered cognitive function. Researchers showed in 2016 that knocking out one or both CCR5s in mice enhances their memory and cognition. A subsequent study that crippled CCR5 in mice found that, compared with control animals, the mutants recovered from strokes more quickly and had improved motor and cognitive functions following traumatic brain injury. The later study, in the 21 February issue of Cell, also included an analysis of 68 stroke patients who had one copy of CCR5 with the HIV resistance mutation; it concluded they had improved recovery, too.
On the night of 26 November, 122 Chinese scientists issued a statement strongly condemning He’s action as unethical. They stated that while CRISPR-Cas is not a new technology, it involves serious off-target risks and associated ethical considerations, and so should not be used to produce gene-altered babies. They described He’s experiment as “crazy” and “a huge blow to the global reputation and development of Chinese science”. The Scientific Ethics Committee of the Academic Divisions of the Chinese Academy of Sciences posted a statement declaring their opposition to any clinical use of genome editing on human embryos, noting that “the theory is not reliable, the technology is deficient, the risks are uncontrollable, and ethics and regulations prohibit the action”. The Chinese Academy of Engineering released a statement on 28 November, calling on scientists to improve self-discipline and self-regulation, and to abide by corresponding ethical principles, laws, and regulations. Finally, the Chinese Academy of Medical Sciences published a correspondence in The Lancet, stating that they are “opposed to any clinical operation of human embryo genome editing for reproductive purposes."
Major studies of influence
- The first known publication of research into human germline editing was by a group of Chinese scientists in April 2015 in the Journal "Protein and Cell". The scientists used tripronuclear (3PN) zygotes, zygotes fertilized by two sperm and therefore non-viable, to investigate CRISPR/Cas9-mediated gene editing in human cells, something that had never been attempted before. The scientists found that while CRISPR/Cas9 could effectively cleave the β-globin gene (HBB), the efficiency of homologous recombination directed repair of HBB was highly inefficient and did not do so in a majority of the trials. Problems arose such as off target cleavage and the competitive recombination of the endogenous delta-globin with the HBB led to unexpected mutation. The results of the study indicated that repair of HBB in the embryos occurred preferentially through alternative pathways. In the end only 4 of the 54 zygotes carried the intended genetic information, and even then the successfully edited embryos were mosaics containing the preferential genetic code and the mutation. The conclusion of the scientists was that further effort was needed in to improve the precision and efficiency of CRISPR/Cas9 gene editing.
- In March 2017 a group of Chinese scientists claimed to have edited three normal viable human embryos out of six total in the experiment. The study showed that CRISPR/Cas9 is could effectively be used as a gene-editing tool in human 2PN zygotes, which could lead potentially pregnancy viable if implanted. The scientists used injection of Cas9 protein complexed with the relevant sgRNAs and homology donors into human embryos. The scientists found homologous recombination-mediated alteration in HBB and G6PD. The scientists also noted the limitations of their study and called for further research.
- In August 2017 a group of scientists from Oregon published an article in Nature journal detailing the successful use of CRISPR to edit out a mutation responsible for congenital heart disease. The study looked at heterozygous MYBPC3 mutation in human embryos. The study claimed precise CRISPR/Cas9 and homology-directed repair response with high accuracy and precision. Double-strand breaks at the mutant paternal allele were repaired using the homologous wild-type gene. By modifying the cell cycle stage at which the DSB was induced, they were able to avoid mosaicism, which had been seen in earlier similar studies, in cleaving embryos and achieve a large percentage of homozygous embryos carrying the wild-type MYBPC3 gene without evidence of unintended mutations. The scientists concluded that the technique may be used for the correction of mutations in human embryos. The claims of this study were however pushed back on by critics who argued the evidence was overall unpersuasive.
- In June 2018 a group of scientists published and article in "Nature" journal indicating a potential link for edited cells having increased potential turn cancerous. The scientists reported that genome editing by CRISPR/Cas9 induced DNA damage response and the cell cycle stopped. The study was conducted in human retinal pigment epithelial cells, and the use of CRISPR led to a selection against cells with a functional p53 pathway. The conclusion of the study would suggest that p53 inhibition might increase efficiency of human germline editing and that p53 function would need to be watched when developing CRISPR/Cas9 based therapy.
- In November 2018 a group of Chinese scientists published research in the journal "Molecular Therapy" detailing their use of CRISPR/Cas9 technology to correct a single mistaken amino acid successfully in 16 out of 18 attempts in a human embryo. The unusual level of precision was achieved by the use of a base editor (BE) system which was constructed by fusing the deaminase to the dCas9 protein. The BE system efficiently edits the targeted C to T or G to A without the use of a donor and without DBS formation. The study focused on the FBN1 mutation that is causative for Marfan syndrome. The study provides proof positive for the corrective value of gene therapy for the FBN1 mutation in both somatic cells and germline cells. The study is noted for its relative precision which is a departure from past results of CRISPR/Cas9 studies.
Lack of clear international regulation
The lack of clear international regulation has led to researchers across the globe attempting to create an international framework of ethical guidelines. Current framework lacks the requisite treaties among nations to create a mechanism for international enforcement. At the first International Summit on Human Gene Editing in December 2015 the collaboration of scientists issued the first international guidelines on genetic research. These guidelines allow for the pre-clinical research into the editing of genetic sequences in human cells granted the embryos are not used to implant pregnancy. Genetic alteration of somatic cells for therapeutic proposes was also considered an ethically acceptable field of research in part due to the lack of ability of somatic cells to transfer genetic material to subsequent generations. However citing the lack of social consensus, and the risk of inaccurate gene editing the conference called for restraint on any germline modifications on implanted embryos intended for pregnancy.
With the international outcry in response to the first recorded case of human germ line edited embryos being implanted by researcher He Jiankui, scientists have continued discussion on the best possible mechanism for enforcement of an international framework. On March 13, 2019 researchers Eric Lander, Françoise Baylis, Feng Zhang, Emmanuelle Charpentier, Paul Bergfrom along with others across the globe published a call for a framework that does not foreclose any outcome but includes a voluntary pledge by nations along with a coordinating body to monitor the application of pledged nations in a moratorium on human germline editing with an attempt to reach social consensus before moving forward into further research. The World Health Organization announced on December 18, 2018 plans to convene an intentional committee on clinical germline editing.
Ethical and moral debates
The neutrality of this section is disputed. Relevant discussion may be found on the talk page. Please do not remove this message until conditions to do so are met. (October 2020) (Learn how and when to remove this message) |
As it stands, there is controversy surrounding human germline engineering. As early in the history of biotechnology as 1990, there have been scientists opposed to attempts to modify the human germline using these new tools, and such concerns have continued as technology progressed. With the advent of new techniques like CRISPR, in March 2015 a group of scientists urged a worldwide moratorium on clinical use of gene editing technologies to edit the human genome in a way that can be inherited. In April 2015, researchers reported results of basic research to edit the DNA of non-viable human embryos using CRISPR, creating controversy. A committee of the American National Academy of Sciences and National Academy of Medicine gave support to human genome editing in 2017 once answers have been found to safety and efficiency problems "but only for serious conditions under stringent oversight."
Editing the genes of human embryos raises its own social and ethical concerns. The scientific community, and global community, have division regarding whether or not human germline engineering should be practiced or not. It is currently banned in many of the leading, developed countries, and highly regulated in the others due to ethical issues.
The American Medical Association’s Council on Ethical and Judicial Affairs stated that "genetic interventions to enhance traits should be considered permissible only in severely restricted situations: (1) clear and meaningful benefits to the fetus or child; (2) no trade-off with other characteristics or traits; and (3) equal access to the genetic technology, irrespective of income or other socioeconomic characteristics."
Ethical claims about germline engineering include beliefs that every fetus has a right to remain genetically unmodified, that parents hold the right to genetically modify their offspring, and that every child has the right to be born free of preventable diseases. For parents, genetic engineering could be seen as another child enhancement technique to add to diet, exercise, education, training, cosmetics, and plastic surgery. Another theorist claims that moral concerns limit but do not prohibit germline engineering.
One issue related to human genome editing relates to the impact of the technology on future individuals whose genes are modified without their consent. Clinical ethics accepts the idea that parents are, almost always, the most appropriate surrogate medical decision makers for their children until the children develop their own autonomy and decision-making capacity. This is based on the assumption that, except under rare circumstances, parents have the most to lose or gain from a decision and will ultimately make decisions that reflects the future values and beliefs of their children. According to this assumption, it could be assumed that parents are the most appropriate decision makers for their future children as well. There are anecdotal reports of children and adults who disagree with the medical decisions made by a parent during pregnancy or early childhood, such as when death was a possible outcome. There are also published patient stories by individuals who feel that they would not wish to change or remove their own medical condition if given the choice and individuals who disagree with medical decisions made by their parents during childhood.
Other scientists and philosophers have noted that the issue of the lack of prior consent applies as well to individuals born via traditional sexual reproduction. Philosopher David Pearce further argues that “old-fashioned sexual reproduction is itself an untested genetic experiment”, often compromising a child’s wellbeing and pro-social capacities even if the child grows in a healthy environment. According to Pearce, “the question of comes down to an analysis of risk-reward ratios - and our basic ethical values, themselves shaped by our evolutionary past.” Bioethicist Julian Savulescu in turn proposes the principle of procreative beneficence, according to which “couples (or single reproducers) should select the child, of the possible children they could have, who is expected to have the best life, or at least as good a life as the others, based on the relevant, available information”. Some ethicists argue that the principle of procreative beneficence would justify or even require genetically enhancing one's children.
The other ethical concern is the potential for “designer babies”, or the creation of humans with "perfect", or "desirable" traits. There is a debate as to if this is morally acceptable as well. Such debate ranges from the ethical obligation to use safe and efficient technology to prevent disease to seeing some actual benefit in genetic disabilities. There are concerns that the introduction of desirable traits in a certain part of the population (instead of the entire population) could cause economic inequalities (“positional” good). However, this isn't the case if a same desirable trait would be introduced over the entire population (similar to vaccines).
Several religious positions have been published with regards to human germline engineering. According to them, many see germline modification as being more moral than the alternative, which would be either discarding of the embryo, or birth of a diseased human. The main conditions when it comes to whether or not it is morally and ethically acceptable lie within the intent of the modification, and the conditions in which the engineering is done.
The process of modifying the human genome has raised ethical questions. One of the issues is “off target effects”, large genomes may contain identical or homologous DNA sequences, and the enzyme complex CRISPR/Cas9 may unintentionally cleave these DNA sequences causing mutations that may lead to cell death. The mutations can cause important genes to be turned on or off, such as genetic anti-cancer mechanisms, that could speed up disease exasperation.
Other ethical concerns are: unintentionally editing the human germline forever, not knowing how one change to a human germline will affect the expression of the remainder of the genes. A scientist recently made an analogy to increase understanding in regard to mapping and manipulating the human genome / germline in relation to a stage play: it is if we have very precise character descriptions (the mapped genome), and yet we (the scientific community) have no idea yet how the characters interact with each other. In other words, if one makes one change to the human germline, what other cascade of changes might we be making?
Another ethical concern pertains to potential unequal distribution of benefits, even in the case of genome editing being inexpensive. For example, corporations may be able to take unfair advantage of patent law or other ways of restricting access to genome editing and thereby may increase the inequalities. There are already disputes in the courts where CRISPR-Cas9 patents and access issues are being negotiated.
There remains debate on if the permissibility of human germline engineering for reproduction is dependent on the use, being either a therapeutic or non-therapeutic application. In a survey by the UK's Royal Society, 76% of participants in the UK supported therapeutic human germline engineering to prevent or correct disease, however for non-therapeutic edits such as enhancing intelligence or altering eye or hair color in embryos, there was only 40% and 31% support, respectively. There was a similar result in a study at the University of Bogota, Colombia, where students as well as professors generally agreed that therapeutic genome editing is acceptable, while non-therapeutic genome editing is not.
There is also debate on if there can be a defined distinction between therapeutic and non-therapeutic germline editing. An example would be if two embryos are predicted to grow up to be very short in height. Boy 1 will be short because of a mutation in his Human Growth Hormone gene, while boy 2 will be short because his parents are very short. Editing the embryo of boy 1 to make him of average height would be a therapeutic germline edit, while editing the embryo of boy 2 to be of average height would be a non-therapeutic germline edit. In both cases with no editing of the boys' genomes they would both grow up to be very short, which would decrease their wellbeing in life. Likewise editing both of the boys' genomes would allow them to grow up to be of average height. In this scenario, editing for the same phenotype for being of average height falls under both therapeutic and non-therapeutic germline engineering.
Current global policy
There is distinction in some country policies, including but not limited to official regulation and legislation, between human germline engineering for reproductive use and for laboratory research. As of October 2020, there are 96 countries that have policies involving the use of germline engineering in human cells.
Reproductive use
Reproductive use of human germline engineering involves implanting the edited embryo to be born. 70 countries currently explicitly prohibit the use of human germline engineering for use in reproduction, while 5 countries prohibit it for reproduction with exceptions. No countries permit the use of human germline engineering for reproduction.
Countries that explicitly prohibit any use of human germline engineering for reproduction are: Albania, Argentina, Australia, Austria, Bahrain, Belarus, Benin, Bosnia and Herzegovina, Brazil, Bulgaria, Burundi, Canada, Chile, China, Congo, Costa Rica, Croatia, Cyprus, Czech Republic, Denmark, Estonia, Finland, France, Georgia, Germany, Greece, Hungary, Iceland, India, Iran, Ireland, Israel, Japan, Kenya, Latvia, Lebanon, Lithuania, Malaysia, Malta, Mexico, Moldova, Montenegro, Netherlands, New Zealand, Nigeria, North Macedonia, Norway, Oman, Pakistan, Poland, Portugal, Qatar, Romania, Russia, San Marino, Saudi Arabia, Serbia, Slovakia, Slovenia, South Korea, Spain, Sweden, Switzerland, Thailand, Tunisia, Turkey, the United Kingdom, the United States, Uruguay, and the Vatican
Countries that explicitly prohibit (with exceptions) the use of human germline engineering for reproduction are: Belgium, Colombia, Italy, Panama, and the United Arab Emirates
Laboratory research
Laboratory research use involves human germline engineering restricted to in vitro use, where edited cells will not be implanted to be born. 19 countries currently explicitly prohibit any use of human germline engineering for in vitro use, while 4 prohibit it with exceptions, and 11 permit it.
Countries that explicitly prohibit any use of germline engineering for in vitro use are: Albania, Austria, Bahrain, Belarus, Brazil, Canada, Costa Rica, Croatia, Germany, Greece, Lebanon, Malaysia, Malta, Pakistan, Saudi Arabia, Sweden, Switzerland, Uruguay, and the Vatican
Countries that explicitly prohibit (with exceptions) the use of germline engineering for in vitro use are: Colombia, Finland, Italy, and Panama
Countries that explicitly permit the use of germline engineering for in vitro use are: Burundi, China, Congo, India, Iran, Ireland, Japan, Norway, Thailand, the United Kingdom, and the United States
See also
- Human genetic engineering
- Gene therapy
- Germinal choice technology
- Human genetic enhancement
- CRISPR
- Designer Baby
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Further reading
- Enriquez, Juan; Gullans, Steve (2015). Evolving Ourselves: How Unnatural Selection is Changing Life on Earth. One World Publications. ISBN 978-1780748412.
- Metzl, Jamie (2020). Hacking Darwin: Genetic Engineering and the Future of Humanity. Naperville, IL: Sourcebooks.
- "Special Issue: Human Germline Editing". Bioethics. 34 (1). 2020.
- Venter, Craig (2014). Life at the Speed of Light: From the Double Helix to the Dawn of Digital Life. United Kingdom: Penguin Books. ISBN 978-0143125907.