A NEW CONOTOXIN AFFECTING SODIUM CURRENT INACTIVATION INTERACTS WITH THE DELTA-CONOTOXIN RECEPTOR-SITE

被引：57

作者：

FAINZILBER, M

LODDER, JC

KITS, KS

KOFMAN, O

VINNITSKY, I

VANRIETSCHOTEN, J

ZLOTKIN, E

GORDON, D

机构：

[1] HEBREW UNIV JERUSALEM,SILBERMAN INST LIFE SCI,DEPT CELL & ANIM BIOL,IL-91904 JERUSALEM,ISRAEL

[2] BEN GURION UNIV NEGEV,BEER SHEVA MENTAL HLTH CTR,IL-84105 BEER SHEVA,ISRAEL

[3] BEN GURION UNIV NEGEV,DEPT BEHAV SCI,IL-84105 BEER SHEVA,ISRAEL

[4] UNIV AIX MARSEILLE 2,FAC MED,DEPT BIOCHEM,F-13916 MARSEILLE 20,FRANCE

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 1995年 / 270卷 / 03期

关键词：

D O I：

10.1074/jbc.270.3.1123

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

We describe a new peptide conotoxin affecting sodium current inactivation, that competes on binding with S-conotoxin TxVIA (delta TxVIA). The amino acid sequence of the new toxin, designated conotoxin NgVIA (NgVIA), is SKCFSOGTFCGIKOGLCCSVRCFSLFCISFE (where O is trans-4-hydroxyproline). The primary structure of NgVIA has an identical cysteine framework and similar hydrophobicity as delta TxVIA but differs in its net charge. NgVIA competes with delta TxVIA on binding to rat brain synaptosomes and molluscan central nervous system and strongly inhibits sodium current inactivation in snail neurons, as does delta TxVIA. In contrast to delta TxVIA, NgVIA is a potent paralytic toxin in vertebrate systems, its binding appears to be voltage-dependent, and it synergically increases veratridine-induced sodium influx to rat brain synaptosomes. delta TxVIA acts as a partial antagonist to NgVIA in rat brain in vivo. NgVIA appears to act via a receptor site distinct from that of delta TxVIA but similar to that of Conus striatus toxin. This new toxin provides a lead for structure function relationship studies in the delta-conotoxins and will enable analysis of the functional significance of this complex of receptor sites in gating mechanisms of sodium channels.

引用

页码：1123 / 1129

页数：7

共 32 条

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