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疟原虫表面相关蛋白(PbSR)在大配子母细胞中合成,并参与疟原虫晶体的形成。

PbSR is synthesized in macrogametocytes and involved in formation of the malaria crystalloids.

作者信息

Carter Victoria, Shimizu Shoichi, Arai Meiji, Dessens Johannes T

机构信息

Department of Infectious and Tropical Diseases, London School of Hygiene and Tropical Medicine, Keppel Street, London WC1E 7HT, UK.

出版信息

Mol Microbiol. 2008 Jun;68(6):1560-9. doi: 10.1111/j.1365-2958.2008.06254.x. Epub 2008 Apr 29.

Abstract

Crystalloids are transient organelles that form in developing malaria ookinetes and disappear after ookinete-to-oocyst transition. Their origins and functions remain poorly understood. The Plasmodium berghei scavenger receptor-like protein PbSR is essential for mosquito-to-host transmission of the parasite: PbSR knockout parasites produce normal numbers of oocysts that fail to form sporozoites, pointing to a role for PbSR in the oocyst during sporogony. Here, using fluorescent protein tagging and targeted gene disruption, we show that PbSR is synthesized in macrogametocytes, gets targeted to the crystalloids of developing ookinetes and is involved in crystalloid formation. While oocyst sporulation rates of PbSR knockout parasites are highly reduced in parasite-infected mosquitoes, sporulation rates in vitro are not adversely affected, supporting the view that mosquito factors could be involved in the PbSR loss-of-function phenotype. These findings are the first to identify a parasite protein involved with the crystalloid organelle, and suggest a novel protein-trafficking mechanism to deliver PbSR to the oocysts.

摘要

晶体是在疟原虫动合子发育过程中形成的短暂细胞器,在动合子向卵囊转变后消失。它们的起源和功能仍知之甚少。伯氏疟原虫清道夫受体样蛋白PbSR对寄生虫从蚊子到宿主的传播至关重要:PbSR基因敲除的寄生虫产生正常数量的卵囊,但无法形成子孢子,这表明PbSR在孢子生殖过程中对卵囊起作用。在这里,我们使用荧光蛋白标记和靶向基因破坏技术,表明PbSR在大配子母细胞中合成,靶向发育中动合子的晶体,并参与晶体形成。虽然在感染寄生虫的蚊子中,PbSR基因敲除寄生虫的卵囊孢子化率大幅降低,但体外孢子化率并未受到不利影响,这支持了蚊子因素可能参与PbSR功能丧失表型的观点。这些发现首次鉴定出一种与晶体细胞器相关的寄生虫蛋白,并提出了一种将PbSR输送到卵囊的新型蛋白质运输机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f6e7/2615194/c8f439f33653/mmi0068-1560-f1.jpg

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