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首页> 外文期刊>Molecular biology of the cell >The Checkpoint Kinase Hsl1p Is Activated by Elm1p-dependent Phosphorylation
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The Checkpoint Kinase Hsl1p Is Activated by Elm1p-dependent Phosphorylation

机译:检查点激酶Hsl1p被Elm1p依赖性磷酸化激活。

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摘要

Saccharomyces cerevisiae cells growing in the outdoor environment must adapt to sudden changes in temperature and other variables. Many such changes trigger stress responses that delay bud emergence until the cells can adapt. In such circumstances, the morphogenesis checkpoint delays mitosis until a bud has been formed. Mitotic delay is due to the Wee1 family mitotic inhibitor Swe1p, whose degradation is linked to bud emergence by the checkpoint kinase Hsl1p. Hsl1p is concentrated at the mother-bud neck through association with septin filaments, and it was reported that Hsl1p activation involved relief of autoinhibition in response to septin interaction. Here we challenge the previous identification of an autoinhibitory domain and show instead that Hsl1p activation involves the phosphorylation of threonine 273, promoted by the septin-associated kinase Elm1p. We identified elm1 mutants in a screen for defects in Swe1p degradation and show that a phosphomimic T273E mutation in HSL1 bypasses the need for Elm1p in this pathway.
机译:在室外环境中生长的酿酒酵母细胞必须适应温度的突然变化和其他变量。许多此类变化触发了压力响应,从而延迟了芽的萌芽,直到细胞能够适应为止。在这种情况下,形态发生检查点会延迟有丝分裂,直到形成芽为止。有丝分裂延迟归因于Wee1家族有丝分裂抑制剂Swe1p,其降解与检查点激酶Hsl1p的芽萌发有关。 Hsl1p通过与septin细丝结合而集中在母芽颈部,据报道,Hsl1p激活涉及对septin相互作用的自抑制作用的缓解。在这里,我们向自动抑制域的先前鉴定提出挑战,并证明Hsl1p激活涉及由Septin相关激酶Elm1p促进的苏氨酸273的磷酸化。我们在Swe1p降解缺陷的筛选中鉴定了elm1突变体,并显示HSL1中的磷酸化T273E突变绕过了该途径中Elm1p的需要。

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