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首页> 外文期刊>Journal of Cell Science >THE ROLE OF THE CORTICAL CYTOSKELETON - F-ACTIN CROSSLINKING PROTEINS PROTECT AGAINST OSMOTIC STRESS, ENSURE CELL SIZE, CELL SHAPE AND MOTILITY, AND CONTRIBUTE TO PHAGOCYTOSIS AND DEVELOPMENT
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THE ROLE OF THE CORTICAL CYTOSKELETON - F-ACTIN CROSSLINKING PROTEINS PROTECT AGAINST OSMOTIC STRESS, ENSURE CELL SIZE, CELL SHAPE AND MOTILITY, AND CONTRIBUTE TO PHAGOCYTOSIS AND DEVELOPMENT

机译:卵磷脂细胞骨架的作用-F-肌动蛋白交联蛋白可防止渗透压,确保细胞大小,细胞形状和运动性,并有助于噬菌体的生长和发育

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We generated Dictyostelium double mutants lacking the two F-actin crosslinking proteins alpha-actinin and gelation factor by inactivating the corresponding genes via homologous recombination, Here we investigated the consequences of these deficiencies both at the single cell level and at the multicellular stage. We found that loss of both proteins severely affected growth of the mutant cells in shaking suspension, and led to a reduction of cell size from 12 mu m in wild-type cells to 9 mu m in mutant cells. Moreover the cells did not exhibit the typical polarized morphology of aggregating Dictyostelium cells but had a more rounded cell shape, and also exhibited an increased sensitivity towards osmotic shock and a reduced rate of phagocytosis. Development was heavily impaired and never resulted in the formation of fruiting bodies. Expression of developmentally regulated genes and the final developmental stages that were reached varied, however, with the substrata on which the cells were deposited. On phosphate buffered agar plates the cells were able to form tight aggregates and mounds and to express prespore and prestalk cell specific genes. Under these conditions the cells could perform chemotactic signalling and cell behavior was normal at the onset of multicellular development as revealed by time-lapse video microscopy. Double mutant cells were motile but speed was reduced by approximately 30% as compared to wild type, These changes were reversed by expressing the gelation factor in the mutant cells. We conclude that the actin assemblies that are formed and/or stabilized by both F-actin crosslinking proteins have a protective function during osmotic stress and are essential for proper cell shape and motility. [References: 71]
机译:我们通过同源重组使相应的基因失活,从而产生了缺少两个F-肌动蛋白交联蛋白α-actinin和胶凝因子的双歧杆菌双突变体。在这里,我们研究了这些缺陷在单细胞水平和多细胞阶段的后果。我们发现这两种蛋白质的损失严重影响了摇晃悬浮液中突变细胞的生长,并导致细胞大小从野生型细胞中的12μm减少到突变细胞中的9μm。此外,这些细胞没有表现出聚集的盘基单胞菌细胞的典型极化形态,但是具有更圆的细胞形状,并且还表现出对渗透性休克的敏感性增加和吞噬率降低。发展受到严重损害,从未导致子实体的形成。然而,发育调节基因的表达和达到的最终发育阶段随细胞沉积​​的基质而变化。在磷酸盐缓冲的琼脂平板上,细胞能够形成紧密的聚集体和土堆,并表达孢子前和茎前细胞特异性基因。在这些条件下,细胞可以执行趋化信号转导,并且在多细胞发育开始时细胞行为是正常的,如延时视频显微镜所揭示。双突变细胞是运动的,但与野生型相比,速度降低了约30%。通过在突变细胞中表达胶凝因子可以逆转这些变化。我们得出的结论是,由两种F-肌动蛋白交联蛋白形成和/或稳定的肌动蛋白装配体在渗透压期间具有保护功能,并且对于适当的细胞形状和运动性至关重要。 [参考:71]

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