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刚果锥虫主要表面蛋白酶同源物的特性分析

Characterization of major surface protease homologues of Trypanosoma congolense.

作者信息

Marcoux Veronica, Wei Guojian, Tabel Henry, Bull Harold J

机构信息

Department of Microbiology and Immunology, University of Saskatchewan, Saskatoon, SK, Canada S7N 5E5.

出版信息

J Biomed Biotechnol. 2010;2010:418157. doi: 10.1155/2010/418157. Epub 2010 Jan 20.

Abstract

Trypanosomes encode a family of proteins known as Major Surface Metalloproteases (MSPs). We have identified six putative MSPs encoded within the partially sequenced T. congolense genome. Phylogenic analysis indicates that T. congolense MSPs belong to five subfamilies that are conserved among African trypanosome species. Molecular modeling, based on the known structure of Leishmania Major GP63, reveals subfamily-specific structural variations around the putative active site despite conservation of overall structure, suggesting that each MSP subfamily has evolved to recognize distinct substrates. We have cloned and purified a protein encoding the amino-terminal domain of the T. congolense homologue TcoMSP-D (most closely related to Leishmania GP63). We detect TcoMSP-D in the serum of T. congolense-infected mice. Mice immunized with the amino-terminal domain of TcoMSP-D generate a persisting IgG1 antibody response. Surprisingly, a low-dose challenge of immunized mice with T. congolense significantly increases susceptibility to infection, indicating that immunity to TcoMSP-D is a factor affecting virulence.

摘要

锥虫编码一类被称为主要表面金属蛋白酶(MSP)的蛋白质家族。我们在部分测序的刚果锥虫基因组中鉴定出了六种假定的MSP。系统发育分析表明,刚果锥虫MSP属于五个亚家族,这些亚家族在非洲锥虫物种中是保守的。基于利什曼原虫主要GP63的已知结构进行的分子建模显示,尽管整体结构保守,但在假定的活性位点周围存在亚家族特异性的结构变异,这表明每个MSP亚家族已经进化到能够识别不同的底物。我们已经克隆并纯化了一种编码刚果锥虫同源物TcoMSP-D(与利什曼原虫GP63关系最为密切)氨基末端结构域的蛋白质。我们在感染刚果锥虫的小鼠血清中检测到了TcoMSP-D。用TcoMSP-D的氨基末端结构域免疫的小鼠产生了持续的IgG1抗体反应。令人惊讶的是,用刚果锥虫对免疫小鼠进行低剂量攻击会显著增加其感染易感性,这表明对TcoMSP-D的免疫是影响毒力的一个因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/355a/2817373/f2afb1d1fecf/JBB2010-418157.001.jpg

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