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In ], a '''drug-eluting stent''' is a ] (a metal scaffold) placed into diseased ] that slowly releases a drug blocking cell proliferation; this helps to delay or prevent the artery from being re-occluded by ] and clot (]). The stent consists of a expandable metal framework, a drug to prevent ], and a carrier to slowly release the drug. It is placed over a balloon on a ] and guide wire and introduced through a peripheral artery, usually one of the ]. It is threaded back towards the heart; from the ], the appropriate coronary artery is entered. The balloon is inflated, cracking and compressing the plaque and expanding the stent. The balloon and catheter are then withdrawn, leaving the stent in place. The stent releases its drug over the next several months. Patients must take ] therapy afterwards, usually ] for six months and ] indefinitely. Drug-eluting stents have been shown to be superior for many of the conditions that traditional stents (“bare-metal stents”) have been used, and have become quite popular since their ] approval in 2003.<ref name="NEJM review">{{cite journal In ], a '''drug-eluting stent''' is a ] (a metal scaffold) placed into diseased ] that slowly releases a drug blocking cell proliferation; this helps to delay or prevent the artery from being re-occluded by ] and clot (]). The stent consists of a expandable metal framework, a drug to prevent ], and a carrier to slowly release the drug. It is placed over a balloon on a ] and guide wire and introduced through a peripheral artery, usually one of the ]. It is threaded back towards the heart; from the ], the appropriate coronary artery is entered. The balloon is inflated, cracking and compressing the plaque and expanding the stent. The balloon and catheter are then withdrawn, leaving the stent in place. The stent releases its drug over the next several months. Patients must take ] therapy afterwards, usually ] for six months and ] indefinitely.<ref name="G&G"> {{cite book
| last = Michel | first = Thomas | editor = Laurence L. Brunton, John S. Lazo, & Keith L. Parker
| title = Goodman & Gilman’s: The Pharmacologic Basis of Therapeutics | origyear = 1941 | edition = 11th ed. | year = 2006
| publisher = McGraw-Hill | location = New York | pages = 842 | chapter = Treatment of Myocardial Ischemia
}}</ref> Drug-eluting stents have been shown to be superior for many of the conditions that traditional stents (“bare-metal stents”) have been used, and have become quite popular since their ] approval in 2003.<ref name="NEJM review">{{cite journal
| last = Serruys | first = Patrick W. | coauthors = Michael J.B. Kutryk, and Andrew T.L. Ong | date = 2006-02-02 | title = Coronary-Artery Stents | last = Serruys | first = Patrick W. | coauthors = Michael J.B. Kutryk, and Andrew T.L. Ong | date = 2006-02-02 | title = Coronary-Artery Stents
| journal = ] | volume = 354 | issue = 5 | pages = 483–495 | url = http://content.nejm.org/cgi/content/extract/354/5/483 | journal = ] | volume = 354 | issue = 5 | pages = 483–495 | url = http://content.nejm.org/cgi/content/extract/354/5/483

Revision as of 05:15, 22 July 2006

An example of a drug-eluting stent. This is the TAXUS™ Express™ Paclitaxel-Eluting Coronary Stent System, which releases paclitaxel.

In medicine, a drug-eluting stent is a stent (a metal scaffold) placed into diseased coronary arteries that slowly releases a drug blocking cell proliferation; this helps to delay or prevent the artery from being re-occluded by smooth muscle and clot (thrombus). The stent consists of a expandable metal framework, a drug to prevent restenosis, and a carrier to slowly release the drug. It is placed over a balloon on a catheter and guide wire and introduced through a peripheral artery, usually one of the femoral arteries. It is threaded back towards the heart; from the aorta, the appropriate coronary artery is entered. The balloon is inflated, cracking and compressing the plaque and expanding the stent. The balloon and catheter are then withdrawn, leaving the stent in place. The stent releases its drug over the next several months. Patients must take antiplatelet therapy afterwards, usually clopidogrel for six months and aspirin indefinitely. Drug-eluting stents have been shown to be superior for many of the conditions that traditional stents (“bare-metal stents”) have been used, and have become quite popular since their FDA approval in 2003.

References

  1. Michel, Thomas (2006) . "Treatment of Myocardial Ischemia". In Laurence L. Brunton, John S. Lazo, & Keith L. Parker (ed.). Goodman & Gilman’s: The Pharmacologic Basis of Therapeutics (11th ed. ed.). New York: McGraw-Hill. p. 842. {{cite book}}: |edition= has extra text (help)CS1 maint: multiple names: editors list (link)
  2. Serruys, Patrick W. (2006-02-02). "Coronary-Artery Stents". New England Journal of Medicine. 354 (5): 483–495. {{cite journal}}: Unknown parameter |coauthors= ignored (|author= suggested) (help) (extract)
  3. "New Device Approval — Cypher Sirolimus-eluting Coronary Stent". Food and Drug Administration. Retrieved 2006-07-22.

See also