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肌球蛋白2在无变形虫谱系之外的快速爬行物种中驱动肌动蛋白收缩。

Myosin 2 drives actin contractility in fast-crawling species outside of the amorphean lineage.

作者信息

Guest Sarah L, Velle Katrina B, Jacques Samantha M, Park Yvette, Man Jarrett, Titus Margaret A, Fritz-Laylin Lillian K

机构信息

University of Massachusetts Amherst, Department of Biology, Amherst MA 01003.

University of Massachusetts Dartmouth, Biology Department, Dartmouth MA 02747.

出版信息

bioRxiv. 2025 May 19:2025.05.16.654244. doi: 10.1101/2025.05.16.654244.

Abstract

Myosin 2-dependent actin contractility drives essential cell functions including fast crawling motility in animal cells, amoebae, and other species from the Amorphea lineage. Whether and how species outside this single eukaryotic group can generate contractile actin networks has been largely unexplored. We demonstrate that , an amoeba from the Heterolobosea-an evolutionarily distant eukaryotic lineage that includes the fastest known crawling eukaryotes-expresses three distinct Myosin 2 homologs. Using biochemical assays and immunofluorescence, we show that these Myosin 2 proteins bind cellular actin networks and that these networks generate ATP-dependent contractility. By identifying additional Myosin 2 homologs in dozens of additional heterolobosean amoebae (but not obligate flagellates), we find a widespread correlation within this group between crawling behavior and contractile actin networks. This correlation includes the amoeba , which we demonstrate can crawl at speeds exceeding 180 μm/min and has contractile actin networks and Myosin 2 homologs. These findings show that Myosin 2-driven contractility exists beyond Amorphea and is associated with diverse, fast-crawling cell types. Expanding the taxonomic breadth of actin network contractility impacts our basic understanding of cell motility, evolutionary biology, and of the fundamental biology of human pathogens that rely on fast cell migration.

摘要

肌球蛋白2依赖的肌动蛋白收缩性驱动着重要的细胞功能,包括动物细胞、变形虫以及变形虫总门中其他物种的快速爬行运动。在这个单一真核生物类群之外的物种是否以及如何产生收缩性肌动蛋白网络,在很大程度上尚未得到探索。我们证明,一种来自异叶足虫纲的变形虫——这是一个在进化上距离较远的真核生物谱系,其中包括已知爬行速度最快的真核生物——表达三种不同的肌球蛋白2同源物。通过生化分析和免疫荧光,我们表明这些肌球蛋白2蛋白与细胞肌动蛋白网络结合,并且这些网络产生ATP依赖的收缩性。通过在另外几十种异叶足虫纲变形虫(但不是专性鞭毛虫)中鉴定出额外的肌球蛋白2同源物,我们发现在这个类群中,爬行行为与收缩性肌动蛋白网络之间存在广泛的相关性。这种相关性包括这种变形虫,我们证明它可以以超过180μm/分钟的速度爬行,并且具有收缩性肌动蛋白网络和肌球蛋白2同源物。这些发现表明,肌球蛋白2驱动的收缩性存在于变形虫总门之外,并且与多种快速爬行的细胞类型相关。扩展肌动蛋白网络收缩性的分类学广度会影响我们对细胞运动、进化生物学以及依赖快速细胞迁移的人类病原体基础生物学的基本理解。

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