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首页> 外文期刊>Molecular biology of the cell >A cleavable propeptide influences Toxoplasma infection by facilitating the trafficking and secretion of the TgMIC2-M2AP invasion complex
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A cleavable propeptide influences Toxoplasma infection by facilitating the trafficking and secretion of the TgMIC2-M2AP invasion complex

机译:可裂解的前肽通过促进TgMIC2-M2AP入侵复合物的运输和分泌影响弓形虫感染。

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摘要

Propeptides regulate protein function and trafficking in many eukaryotic systems and have emerged as important features of regulated secretory proteins in parasites of the phylum Apicomplexa. Regulated protein secretion from micronemes and host cell invasion are inextricably linked and essential processes for the apicomplexan parasite Toxoplasma gondii. TgM2AP is a propeptide-containing microneme protein found in a heterohexameric complex with the microneme protein TgMIC2, a protein that has a demonstrated fundamental role in gliding motility and invasion. TgM2AP function is also central to these processes, because disruption of TgM2AP (m2apKO) results in secretory retention of TgMIC2, leading to reduced TgMIC2 secretion from the micronemes and impaired invasion. Because the TgM2AP propeptide is predicted to be processed in an intracellular site near where TgMIC2 is retained in m2apKO parasites, we hypothesized that the propeptide and its proteolytic removal influence trafficking and secretion of the complex. We found that proTgM2AP traffics through endosomal compartments and that deletion of the propeptide leads to defective trafficking of the complex within or near this site, resulting in aberrant processing and decreased secretion of TgMIC2, impaired invasion, and reduced virulence in vivo, mirroring the phenotypes observed in m2apKO parasites. In contrast, mutation of several cleavage site residues resulted in normal localization, but it affected the stability and secretion of the complex from the micronemes. Therefore, the propeptide and its cleavage site influence distinct aspects of TgMIC2-M2AP function, with both impacting the outcome of infection.
机译:前肽在许多真核系统中调节蛋白质的功能和运输,并且已被作为蜂巢复合体的寄生物中调节的分泌蛋白的重要特征。微小的neme和宿主细胞入侵的调节的蛋白质分泌是密不可分的联系,是apicomplexan寄生虫弓形虫的必不可少的过程。 TgM2AP是与微血红素蛋白TgMIC2异六聚体复合物中发现的含前肽的微血红素蛋白,该蛋白质在滑行运动和侵袭中具有基本作用。 TgM2AP功能在这些过程中也很重要,因为TgM2AP(m2apKO)的破坏会导致TgMIC2的分泌保持,从而导致微克星的TgMIC2分泌减少和侵袭受损。由于预计TgM2AP前肽会在mgapKO寄生虫中保留TgMIC2的细胞内位点附近加工,因此我们假设前肽及其蛋白水解作用会影响复合物的运输和分泌。我们发现proTgM2AP通过内体区室运输,并且前肽的缺失导致该位点内或附近的复合物的缺陷运输,从而导致异常加工和TgMIC2的分泌减少,侵袭受损并降低了体内的毒力,反映了观察到的表型在m2apKO寄生虫中。相反,几个切割位点残基的突变导致正常定位,但是它影响了复合物的稳定性和微团簇的分泌。因此,前肽及其切割位点影响TgMIC2-M2AP功能的不同方面,都影响感染的结果。

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