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基于顶端的疟原虫邻近标记法鉴定出一种在蚊子感染过程中具有双重功能的膜蛋白。

APEX-based proximity labeling in Plasmodium identifies a membrane protein with dual functions during mosquito infection.

作者信息

Kehrer Jessica, Pietsch Emma, Ricken Dominik, Strauss Léanne, Heinze Julia M, Gilberger Tim, Frischknecht Friedrich

机构信息

Center for Infectious Diseases, Integrative Parasitology, Heidelberg University Medical School, Heidelberg, Germany.

German Center for Infection Research, DZIF, partner site Heidelberg, Heidelberg, Germany.

出版信息

PLoS Pathog. 2024 Dec 18;20(12):e1012788. doi: 10.1371/journal.ppat.1012788. eCollection 2024 Dec.

Abstract

Transmission of the malaria parasite Plasmodium to mosquitoes necessitates gamete egress from red blood cells to allow zygote formation and ookinete motility to enable penetration of the midgut epithelium. Both processes are dependent on the secretion of proteins from distinct sets of specialized vesicles. Inhibiting some of these proteins has shown potential for blocking parasite transmission to the mosquito. To identify new transmission blocking vaccine candidates, we aimed to define the microneme content from ookinetes of the rodent model organism Plasmodium berghei using APEX2-mediated rapid proximity-dependent biotinylation. Besides known proteins of ookinete micronemes, this identified over 50 novel candidates and sharpened the list of a previous survey based on subcellular fractionation. Functional analysis of a first candidate uncovered a dual role for this membrane protein in male gametogenesis and ookinete midgut traversal. Mutation of a putative trafficking motif in the C-terminus affected ookinete to oocyst transition but not gamete formation. This suggests the existence of distinct functional and transport requirements for Plasmodium proteins in different parasite stages.

摘要

疟原虫向蚊子的传播需要配子从红细胞中逸出,以形成合子并使动合子具有运动能力,从而穿透中肠上皮。这两个过程都依赖于来自不同组特殊囊泡的蛋白质分泌。抑制其中一些蛋白质已显示出阻断寄生虫向蚊子传播的潜力。为了鉴定新的传播阻断疫苗候选物,我们旨在利用APEX2介导的快速邻近依赖性生物素化来确定啮齿动物模型生物伯氏疟原虫动合子的微线体成分。除了动合子微线体的已知蛋白质外,这还鉴定出了50多种新的候选物,并完善了先前基于亚细胞分级分离的调查清单。对第一个候选物的功能分析揭示了这种膜蛋白在雄配子发生和动合子穿越中肠过程中的双重作用。C末端一个假定的运输基序的突变影响了动合子向卵囊的转变,但不影响配子的形成。这表明疟原虫蛋白质在不同寄生虫阶段存在不同的功能和运输需求。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1084/11695019/d4fa67e9cdea/ppat.1012788.g001.jpg

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