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针对来自巴西矛头蝮蛇毒液的金属蛋白酶 BaP1 的单克隆抗体的免疫化学和生物学特性。

Immunochemical and biological characterization of monoclonal antibodies against BaP1, a metalloproteinase from Bothrops asper snake venom.

机构信息

Laboratório de Imunopatologia, Instituto Butantan, Av. Vital Brazil, 1500, Butantã, CEP 05503-900, São Paulo, SP, Brazil.

出版信息

Toxicon. 2010 Nov;56(6):1059-65. doi: 10.1016/j.toxicon.2010.07.014. Epub 2010 Jul 30.

Abstract

BaP1 is a P-I class of Snake Venom Metalloproteinase (SVMP) relevant in the local tissue damage associated with envenomations by Bothrops asper, a medically-important species in Central America and parts of South America. Six monoclonal antibodies (MoAb) against BaP1 (MABaP1) were produced and characterized regarding their isotype, dissociation constant (K(d)), specificity and ability to neutralize BaP1-induced hemorrhagic and proteolytic activity. Two MABaP1 are IgM, three are IgG1 and one is IgG2b. The K(d)s of IgG MoAbs were in the nM range. All IgG MoAbs recognized conformational epitopes of BaP1 and B. asper venom components but failed to recognize venoms from 27 species of Viperidae, Colubridae and Elapidae families. Clone 7 cross-reacted with three P-I SVMPs tested (moojeni protease, insularinase and neuwiedase). BaP1-induced hemorrhage was totally neutralized by clones 3, 6 and 8 but not by clone 7. Inhibition of BaP1 enzymatic activity on a synthetic substrate by MABaP1 was totally achieved by clones 3 and 6, and partially by clone 8, but not by clone 7. In conclusion, these neutralizing MoAbs against BaP1 may become important tools to understand structure-function relationships of BaP1 and the role of P-I class SVMP in snakebite envenomation.

摘要

BaP1 是一种 P-I 类蛇毒金属蛋白酶(SVMP),与中美洲和南美洲部分地区重要的医学物种——矛头蝮属的蛇毒引起的局部组织损伤有关。针对 BaP1 产生了 6 种单克隆抗体(MABaP1),并对其同种型、解离常数(K(d))、特异性和中和 BaP1 诱导的出血和蛋白水解活性的能力进行了表征。两种 MABaP1 是 IgM,三种是 IgG1,一种是 IgG2b。IgG 单克隆抗体的 K(d)在纳摩尔范围内。所有 IgG 单克隆抗体均识别 BaP1 和矛头蝮属毒液成分的构象表位,但未能识别来自 27 种蝰蛇科、游蛇科和眼镜蛇科的毒液。克隆 7 与测试的 3 种 P-I SVMP(moojeni 蛋白酶、insularinase 和 neuwiedase)发生交叉反应。克隆 3、6 和 8 完全中和了 BaP1 诱导的出血,但克隆 7 没有。MABaP1 对合成底物上 BaP1 酶活性的抑制完全由克隆 3 和 6 实现,部分由克隆 8 实现,但克隆 7 没有。总之,这些针对 BaP1 的中和单克隆抗体可能成为了解 BaP1 的结构-功能关系以及 P-I 类 SVMP 在蛇伤中毒中的作用的重要工具。

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