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首页> 外文期刊>Biological chemistry >Genetic interactions with mutations affecting septin assembly reveal ESCRT functions in budding yeast cytokinesis.
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Genetic interactions with mutations affecting septin assembly reveal ESCRT functions in budding yeast cytokinesis.

机译:具有影响Septin装配的突变的遗传相互作用揭示了ESCRT在发芽酵母胞质分裂中的功能。

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摘要

Membrane trafficking via targeted exocytosis to the Saccharomyces cerevisiae bud neck provides new membrane and membrane-associated factors that are critical for cytokinesis. It remains unknown whether yeast plasma membrane abscission, the final step of cytokinesis, occurs spontaneously following extensive vesicle fusion, as in plant cells, or requires dedicated membrane fission machinery, as in cultured mammalian cells. Components of the endosomal sorting complexes required for transport (ESCRT) pathway, or close relatives thereof, appear to participate in cytokinetic abscission in various cell types, but roles in cell division had not been documented in budding yeast, where ESCRTs were first characterized. By contrast, the septin family of filament-forming cytoskeletal proteins were first identified by their requirement for yeast cell division. We show here that mutations in ESCRT-encoding genes exacerbate the cytokinesis defects of cla4Delta or elm1Delta mutants, in which septin assembly is perturbed at an early stage in cell division, and alleviate phenotypes of cells carrying temperature-sensitive alleles of a septin-encoding gene, CDC10. Elevated chitin synthase II (Chs2) levels coupled with aberrant morphogenesis and chitin deposition in elm1Delta cells carrying ESCRT mutations suggest that ESCRTs normally enhance the efficiency of cell division by promoting timely endocytic turnover of key cytokinetic enzymes.
机译:通过靶向胞吐作用将膜运输到酿酒酵母芽颈提供了新的膜和膜相关因子,这对于胞质分裂至关重要。酵母胞膜脱落是胞质分裂的最后一步,是在广泛的囊泡融合后自发发生的,如在植物细胞中,还是需要专用的膜裂变机制,如在培养的哺乳动物细胞中,还是未知的。运输(ESCRT)途径所需的内体分选复合物的成分或其近亲,似乎参与了各种细胞类型的细胞动力学脱落,但是尚未在萌芽的酵母中记录到细胞分裂的作用。相反,首先通过它们对酵母细胞分裂的需求来鉴定丝状蛋白形成的细胞骨架蛋白的septin家族。我们在这里显示,ESCRT编码基因中的突变加剧了cla4Delta或elm1Delta突变体的胞质分裂缺陷,其中septin装配在细胞分裂的早期受到干扰,并减轻了携带septin编码基因的温度敏感等位基因的细胞的表型。 ,CDC10。带有ESCRT突变的elm1Delta细胞中几丁质合酶II(Chs2)水平升高,加上异常的形态发生和几丁质沉积,表明ESCRT通常通过促进关键细胞动力学酶的内吞周转来正常增强细胞分裂效率。

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