Sea anemone neurotoxin: Difference between revisions

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	This family also includes the ] and ]s BDS-I ({{Uniprot\|P11494}}) and BDS-II ({{Uniprot\|P59084}}) expressed by '']''. BDS-I is organised into a triple-stranded antiparallel beta-sheet, with an additional small antiparallel beta-sheet at the N-terminus<ref name="PUB00016458">{{cite journal \|author=Clore GM, Driscoll PC, Gronenborn AM, Beress L \|title=Determination of the three-dimensional solution structure of the antihypertensive and antiviral protein BDS-I from the sea anemone Anemonia sulcata: a study using nuclear magnetic resonance and hybrid distance geometry-dynamical simulated annealing \|journal=Biochemistry \|volume=28 \|issue=5 \|pages=2188–2198 \|year=1989 \|pmid=2566326 \|doi=10.1021/bi00431a033}}</ref>. Both peptides are known to specifically block the Kv3.4 potassium channel, and thus bring about a decrease in blood pressure<ref name="PUB00016411">{{cite journal \|author=Lazdunski M, Schweitz H, Diochot S, Beress L \|title=Sea anemone peptides with a specific blocking activity against the fast inactivating potassium channel Kv3.4 \|journal=J. Biol. Chem. \|volume=273 \|issue=12 \|pages=6744–6749 \|year=1998 \|pmid=9506974 \|doi=10.1074/jbc.273.12.6744}}</ref>. Moreover, they inhibit the cytopathic effects of mouse hepatitis virus strain MHV-A59 on mouse liver cells, by an unknown mechanism<ref name="PUB00016458" />.		This family also includes the ] and ]s BDS-I ({{Uniprot\|P11494}}) and BDS-II ({{Uniprot\|P59084}}) expressed by '']''. BDS-I is organised into a triple-stranded antiparallel beta-sheet, with an additional small antiparallel beta-sheet at the N-terminus<ref name="PUB00016458">{{cite journal \|author=Clore GM, Driscoll PC, Gronenborn AM, Beress L \|title=Determination of the three-dimensional solution structure of the antihypertensive and antiviral protein BDS-I from the sea anemone Anemonia sulcata: a study using nuclear magnetic resonance and hybrid distance geometry-dynamical simulated annealing \|journal=Biochemistry \|volume=28 \|issue=5 \|pages=2188–2198 \|year=1989 \|pmid=2566326 \|doi=10.1021/bi00431a033}}</ref>. Both peptides are known to specifically block the Kv3.4 potassium channel, and thus bring about a decrease in blood pressure<ref name="PUB00016411">{{cite journal \|author=Lazdunski M, Schweitz H, Diochot S, Beress L \|title=Sea anemone peptides with a specific blocking activity against the fast inactivating potassium channel Kv3.4 \|journal=J. Biol. Chem. \|volume=273 \|issue=12 \|pages=6744–6749 \|year=1998 \|pmid=9506974 \|doi=10.1074/jbc.273.12.6744}}</ref>. Moreover, they inhibit the cytopathic effects of mouse hepatitis virus strain MHV-A59 on mouse liver cells, by an unknown mechanism<ref name="PUB00016458" />.

	{\|-valign=top		{\|
			\|-valign=top
	\|{{Pfam_box		\|{{Pfam_box
	\| Symbol = Toxin_4		\| Symbol = Toxin_4
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	\| caption = Structure of the antihypertensive and antiviral protein BDS-I from the sea anemone ''Anemonia sulcata''.<ref>PubMed Id: 2566326</ref>		\| caption = Structure of the antihypertensive and antiviral protein BDS-I from the sea anemone ''Anemonia sulcata''.<ref>PubMed Id: 2566326</ref>
	\| Pfam= PF07936		\| Pfam= PF07936
			\| Pfam_clan = CL0075
	\| InterPro= IPR012414		\| InterPro= IPR012414
	\| SMART=		\| SMART=

Revision as of 09:34, 12 August 2010

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Sea anemone neurotoxin is the name given to neurotoxins produced by sea anemones with related structure and function. A number of proteins belonging to this family, including calitoxin and anthopleurin. The neurotoxins bind specifically to the sodium channel, thereby delaying its inactivation during signal transduction, resulting in strong stimulation of mammalian cardiac muscle contraction. Calitoxin 1 has been found in neuromuscular preparations of crustaceans, where it increases transmitter release, causing firing of the axons. Three disulfide bonds are present in this protein.

This family also includes the antihypertensive and antiviral proteins BDS-I (P11494) and BDS-II (P59084) expressed by Anemonia sulcata. BDS-I is organised into a triple-stranded antiparallel beta-sheet, with an additional small antiparallel beta-sheet at the N-terminus. Both peptides are known to specifically block the Kv3.4 potassium channel, and thus bring about a decrease in blood pressure. Moreover, they inhibit the cytopathic effects of mouse hepatitis virus strain MHV-A59 on mouse liver cells, by an unknown mechanism.

Protein family

Anenome neurotoxin

Structure of the neurotoxin ATX Ia from Anemonia sulcata.

Identifiers

Symbol

Toxin_4

Pfam clan

1atx / SCOPe / SUPFAM

OPM superfamily

OPM protein

1apf

Available protein structures:
Pfam	structures / ECOD
PDB	RCSB PDB; PDBe; PDBj
PDBsum	structure summary
PDB	1apf :3-47 1ahl :3-47 1atx :3-44 2sh1 :2-44 1shi :2-44 1sh1 :2-44

Protein family

Antihypertensive protein BDS-I/II

Structure of the antihypertensive and antiviral protein BDS-I from the sea anemone Anemonia sulcata.

Identifiers

Symbol

BDS_I_II

Pfam clan

2bds / SCOPe / SUPFAM

OPM superfamily

OPM protein

1bds

Available protein structures:
Pfam	structures / ECOD
PDB	RCSB PDB; PDBe; PDBj
PDBsum	structure summary
PDB	2bds :1-43 1bds :1-43 1wqkA:1-41 1wxnA:1-41

References

Norton TR (1981). "Cardiotonic polypeptides from Anthopleura xanthogrammica (Brandt) and A. elegantissima (Brandt)". Fed. Proc. 40 (1): -. PMID 6108877.
Yasunobu KT, Norton TR, Reimer NS, Yasunobu CL (1985). "Amino acid sequence of the Anthopleura xanthogrammica heart stimulant, anthopleurin-B". J. Biol. Chem. 260 (15): -. PMID 4019448.{{cite journal}}: CS1 maint: multiple names: authors list (link)
Scanlon MJ, Pallaghy PK, Norton RS, Monks SA (1995). "Solution structure of the cardiostimulant polypeptide anthopleurin-B and comparison with anthopleurin-A". Structure. 3 (8): -. PMID 7582896.{{cite journal}}: CS1 maint: multiple names: authors list (link)
^ Clore GM, Driscoll PC, Gronenborn AM, Beress L (1989). "Determination of the three-dimensional solution structure of the antihypertensive and antiviral protein BDS-I from the sea anemone Anemonia sulcata: a study using nuclear magnetic resonance and hybrid distance geometry-dynamical simulated annealing". Biochemistry. 28 (5): 2188–2198. doi:10.1021/bi00431a033. PMID 2566326.{{cite journal}}: CS1 maint: multiple names: authors list (link)
Lazdunski M, Schweitz H, Diochot S, Beress L (1998). "Sea anemone peptides with a specific blocking activity against the fast inactivating potassium channel Kv3.4". J. Biol. Chem. 273 (12): 6744–6749. doi:10.1074/jbc.273.12.6744. PMID 9506974.{{cite journal}}: CS1 maint: multiple names: authors list (link) CS1 maint: unflagged free DOI (link)
Widmer H, Billeter M, Wüthrich K (1989). "Three-dimensional structure of the neurotoxin ATX Ia from Anemonia sulcata in aqueous solution determined by nuclear magnetic resonance spectroscopy". Proteins. 6 (4): 357–71. doi:10.1002/prot.340060403. PMID 2576133.{{cite journal}}: CS1 maint: multiple names: authors list (link)
PubMed Id: 2566326

This article incorporates text from the public domain Pfam and InterPro: IPR000693

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