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顶复门寄生虫的分裂和对宿主环境的适应依赖于质体脂质代谢的可塑性和宿主细胞器的重塑。

Division and Adaptation to Host Environment of Apicomplexan Parasites Depend on Apicoplast Lipid Metabolic Plasticity and Host Organelle Remodeling.

机构信息

ApicoLipid Team, Institute for Advanced Biosciences, CNRS UMR5309, Université Grenoble Alpes, INSERM U1209, Grenoble, France.

Dynamique des interactions Membranaires normales et pathologiques, UMR5235, Université Montpellier II, Montpellier, France.

出版信息

Cell Rep. 2020 Mar 17;30(11):3778-3792.e9. doi: 10.1016/j.celrep.2020.02.072.

Abstract

Apicomplexan parasites are unicellular eukaryotic pathogens that must obtain and combine lipids from both host cell scavenging and de novo synthesis to maintain parasite propagation and survival within their human host. Major questions on the role and regulation of each lipid source upon fluctuating host nutritional conditions remain unanswered. Characterization of an apicoplast acyltransferase, TgATS2, shows that the apicoplast provides (lyso)phosphatidic acid, required for the recruitment of a critical dynamin (TgDrpC) during parasite cytokinesis. Disruption of TgATS2 also leads parasites to shift metabolic lipid acquisition from de novo synthesis toward host scavenging. We show that both lipid scavenging and de novo synthesis pathways in wild-type parasites exhibit major metabolic and cellular plasticity upon sensing host lipid-deprived environments through concomitant (1) upregulation of de novo fatty acid synthesis capacities in the apicoplast and (2) parasite-driven host remodeling to generate multi-membrane-bound structures from host organelles that are imported toward the parasite.

摘要

顶复门寄生虫是单细胞真核病原体,它们必须从宿主细胞的吞噬作用和从头合成中获取和结合脂质,以维持寄生虫在其人类宿主内的繁殖和生存。关于在宿主营养条件波动时每种脂质来源的作用和调节的主要问题仍未得到解答。对一个质体酰基转移酶 TgATS2 的特征描述表明,质体提供了(溶血)磷脂酸,这对于寄生虫胞质分裂过程中关键的动力蛋白(TgDrpC)的募集是必需的。TgATS2 的缺失也导致寄生虫将代谢脂质的获取从从头合成转向宿主吞噬作用。我们表明,在感知宿主缺乏脂质的环境时,野生型寄生虫中的脂质吞噬作用和从头合成途径都表现出显著的代谢和细胞可塑性,这是通过(1)在质体中上调从头脂肪酸合成能力和(2)寄生虫驱动的宿主重塑来实现的,这种重塑可以从宿主细胞器中产生多膜结合结构,并将这些结构导入寄生虫。

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