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布氏锥虫天然半胱氨酸肽酶抑制剂ICP在分化和毒力中的作用。

Role of the Trypanosoma brucei natural cysteine peptidase inhibitor ICP in differentiation and virulence.

作者信息

Santos Camila C, Coombs Graham H, Lima Ana Paula C A, Mottram Jeremy C

机构信息

Instituto de Biofisica Carlos Chagas Filho, Universidade Federal do Rio de Janeiro, Bloco G, C.C.S., Cidade Universitaria, Rio de Janeiro, RJ, 21949-900, Brazil.

出版信息

Mol Microbiol. 2007 Nov;66(4):991-1002. doi: 10.1111/j.1365-2958.2007.05970.x. Epub 2007 Oct 17.

Abstract

ICP is a chagasin-family natural tight binding inhibitor of Clan CA, family C1 cysteine peptidases (CPs). We investigated the role of ICP in Trypanosoma brucei by generating bloodstream form ICP-deficient mutants (Deltaicp). A threefold increase in CP activity was detected in lysates of Deltaicp, which was restored to the levels in wild type parasites by re-expression of the gene in the null mutant. Deltaicp displayed slower growth in culture and increased resistance to a trypanocidal synthetic CP inhibitor. More efficient exchange of the variant surface glycoprotein (VSG) to procyclin during differentiation from bloodstream to procyclic form was observed in Deltaicp, a phenotype that was reversed in the presence of synthetic CP inhibitors. Furthermore, we showed that degradation of anti-VSG IgG is abolished when parasites are pretreated with synthetic CP inhibitors, and that parasites lacking ICP degrade IgG more efficiently than wild type. In addition, Deltaicp reached higher parasitemia than wild type parasites in infected mice, suggesting that ICP modulates parasite infectivity. Taken together, these data suggest that CPs of T. brucei bloodstream form play a role in surface coat exchange during differentiation, in the degradation of internalized IgG and in parasite infectivity, and that their function is regulated by ICP.

摘要

ICP是半胱氨酸蛋白酶(CPs)家族C1、CA族的一种来自查加辛家族的天然紧密结合抑制剂。我们通过构建血流形式的ICP缺陷型突变体(Deltaicp)来研究ICP在布氏锥虫中的作用。在Deltaicp的裂解物中检测到CP活性增加了三倍,通过在无该基因的突变体中重新表达该基因,其活性恢复到野生型寄生虫的水平。Deltaicp在培养物中生长较慢,并且对一种杀锥虫的合成CP抑制剂的抗性增加。在从血流形式向原循环形式分化过程中,Deltaicp中观察到变体表面糖蛋白(VSG)向原环蛋白的交换更有效,在存在合成CP抑制剂的情况下这种表型会逆转。此外,我们发现当用合成CP抑制剂预处理寄生虫时,抗VSG IgG的降解被消除,并且缺乏ICP的寄生虫比野生型更有效地降解IgG。另外,Deltaicp在感染小鼠中达到的寄生虫血症水平高于野生型寄生虫,这表明ICP调节寄生虫的感染性。综上所述,这些数据表明布氏锥虫血流形式的CPs在分化过程中的表面被膜交换、内化IgG的降解以及寄生虫感染性方面发挥作用,并且它们的功能受ICP调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1431/2680270/363b34fa399f/mmi0066-0991-f1.jpg

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