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摄食相关基因在粘质沙雷氏菌上的食噬作用。

Phagocytosis-associated genes in Acanthamoeba castellanii feeding on Escherichia coli.

机构信息

Department of Biomedical Science, Graduate School, Kyung Hee University, Seoul 02447, Korea.

Department of Medical Zoology, Kyung Hee University School of Medicine, Seoul 02447, Korea.

出版信息

Parasites Hosts Dis. 2023 Nov;61(4):397-404. doi: 10.3347/PHD.23088. Epub 2023 Nov 28.

Abstract

Acanthamoeba species are free-living amoebae those are widely distributed in the environment. They feed on various microorganisms, including bacteria, fungi, and algae. Although majority of the microbes phagocytosed by Acanthamoeba spp. are digested, some pathogenic bacteria thrive within them. Here, we identified the roles of 3 phagocytosis-associated genes (ACA1_077100, ACA1_175060, and AFD36229.1) in A. castellanii. These 3 genes were upregulated after the ingestion of Escherichia coli. However, after the ingestion of Legionella pneumophila, the expression of these 3 genes was not altered after the consumption of L. pneumophila. Furthermore, A. castellanii transfected with small interfering RNS (siRNA) targeting the 3 phagocytosis-associated genes failed to digest phagocytized E. coli. Silencing of ACA1_077100 disabled phagosome formation in the E. coli-ingesting A. castellanii. Alternatively, silencing of ACA1_175060 enabled phagosome formation; however, phagolysosome formation was inhibited. Moreover, suppression of AFD36229.1 expression prevented E. coli digestion and consequently led to the rupturing of A. castellanii. Our results demonstrated that the ACA1_077100, ACA1_175060, and AFD36229.1 genes of Acanthamoeba played crucial roles not only in the formation of phagosome and phagolysosome but also in the digestion of E. coli.

摘要

棘阿米巴属是自由生活的阿米巴,广泛分布于环境中。它们以各种微生物为食,包括细菌、真菌和藻类。虽然棘阿米巴属吞噬的大多数微生物都被消化了,但有些致病性细菌在其中茁壮成长。在这里,我们鉴定了棘阿米巴属中 3 个与吞噬作用相关的基因(ACA1_077100、ACA1_175060 和 AFD36229.1)的作用。这 3 个基因在摄取大肠杆菌后上调。然而,在摄取嗜肺军团菌后,这 3 个基因的表达在消耗嗜肺军团菌后并未改变。此外,用靶向 3 个与吞噬作用相关的基因的小干扰 RNA(siRNA)转染的棘阿米巴属未能消化吞噬的大肠杆菌。沉默与吞噬作用相关的基因 ACA1_077100 会使摄取大肠杆菌的棘阿米巴属无法形成吞噬体。相反,沉默 ACA1_175060 可以形成吞噬体,但抑制了吞噬溶酶体的形成。此外,抑制 AFD36229.1 的表达可阻止大肠杆菌的消化,从而导致棘阿米巴属破裂。我们的结果表明,棘阿米巴属的 ACA1_077100、ACA1_175060 和 AFD36229.1 基因不仅在吞噬体和吞噬溶酶体的形成中起关键作用,而且在大肠杆菌的消化中也起关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e79c/10693966/023f285f5eda/phd-23088f1.jpg

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