ω-芋螺毒素GVIA的非肽模拟物的合成与生物学评价

Synthesis and biological evaluation of nonpeptide mimetics of omega-conotoxin GVIA.

作者信息

Baell Jonathan B, Duggan Peter J, Forsyth Stewart A, Lewis Richard J, Lok Y Phei, Schroeder Christina I

机构信息

Biomolecular Research Institute, 343 Royal Parade, Parkville, Victoria 3052, Australia.

出版信息

Bioorg Med Chem. 2004 Aug 1;12(15):4025-37. doi: 10.1016/j.bmc.2004.05.040.

DOI:10.1016/j.bmc.2004.05.040

PMID:15246080

Abstract

A benzothiazole-derived compound (4a) designed to mimic the C(alpha)-C(beta) bond vectors and terminal functionalities of Lys2, Tyr13 and Arg17 in omega-conotoxin GVIA was synthesised, together with analogues (4b-d), which had each side-chain mimic systematically truncated or eliminated. The affinity of these compounds for rat brain N-type and P/Q-type voltage gated calcium channels (VGCCs) was determined. In terms of N-type channel affinity and selectivity, two of these compounds (4a and 4d) were found to be highly promising, first generation mimetics of omega-conotoxin. The fully functionalised mimetic (4a) showed low microM binding affinity to N-type VGCCs (IC(50)=1.9 microM) and greater than 20-fold selectivity for this channel sub-type over P/Q-type VGCCs, whereas the mimetic in which the guanidine-type side chain was truncated back to an amine (4d, IC(50)= 4.1 microM) showed a greater than 25-fold selectivity for the N-type channel.

摘要

合成了一种旨在模拟ω-芋螺毒素GVIA中Lys2、Tyr13和Arg17的C(α)-C(β)键向量和末端官能团的苯并噻唑衍生化合物(4a)，以及类似物(4b-d)，其中每个侧链模拟物都被系统地截短或消除。测定了这些化合物对大鼠脑N型和P/Q型电压门控钙通道(VGCCs)的亲和力。就N型通道亲和力和选择性而言，发现其中两种化合物(4a和4d)是非常有前景的第一代ω-芋螺毒素模拟物。完全功能化的模拟物(4a)对N型VGCCs表现出低微摩尔结合亲和力(IC(50)=1.9μM)，并且对该通道亚型的选择性比对P/Q型VGCCs高20倍以上，而胍型侧链被截短为胺的模拟物(4d，IC(50)=4.1μM)对N型通道的选择性大于25倍。

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ω-芋螺毒素GVIA的非肽模拟物的合成与生物学评价

Synthesis and biological evaluation of nonpeptide mimetics of omega-conotoxin GVIA.

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