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首页> 外文期刊>Developmental cell >A Lipid Transfer Protein Signaling Axis Exerts Dual Control of Cell-Cycle and Membrane Trafficking Systems
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A Lipid Transfer Protein Signaling Axis Exerts Dual Control of Cell-Cycle and Membrane Trafficking Systems

机译:脂质转移蛋白信号轴施加细胞周期和膜贩运系统的双重控制

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摘要

Kes1/Osh4 is a member of the conserved, but functionally enigmatic, oxysterol binding protein-related protein (ORP) superfamily that inhibits phosphatidylinositol transfer protein (Sec14)-dependent membrane trafficking through the trans-Golgi (TGN)/endosomal network. We now report that Kes1, and select other ORPs, execute cell-cycle control activities as functionally non-redundant inhibitors of the G(1)/S transition when cells confront nutrient-poor environments and promote replicative aging. Kes1-dependent cell-cycle regulation requires the Great-wall/MASTL kinase ortholog Rim15, and is opposed by Sec14 activity in a mechanism independent of Kes1/Sec14 bulk membrane-trafficking functions. Moreover, the data identify Kes1 as a non-histone target for NuA4 through which this lysine acetyltransferase co-modulates membrane-trafficking and cell-cycle activities. We propose the Sec14/Kes1 lipid-exchange protein pair constitutes part of the mechanism for integrating TGN/endosomal lipid signaling with cell-cycle progression and hypothesize that ORPs define a family of stage-specific cell-cycle control factors that execute tumor-suppressor-like functions.
机译:KES1 / OSH4是保守,但功能性神秘的苏西醇结合蛋白质相关蛋白(ORP)超家族的成员,其抑制磷脂酰肌醇转移蛋白(SEC14)依赖性膜流量通过Trans-golgi(TGN)/内体网络。我们现在报告KES1,并选择其他ORPS,当细胞面对营养不良的环境并促进复制老化时,将细胞周期控制活动执行如G(1)/ s转型的功能非冗余抑制剂。 KES1依赖性细胞周期调节需要较大的壁/乳腺激酶ORTHOOG RIM15,并且在独立于KES1 / SEC14散装函数的机制中,通过SEC14活性相反。此外,数据识别KES1作为Nua4的非组蛋白靶,通过该谷氨酸乙酰转移酶共调制膜 - 贩运和细胞循环活性。我们提出SEC14 / KES1脂质交换蛋白对构成与细胞周期进展的TGN /内体脂质信号传导的机制的一部分,并假设ORPS定义了执行肿瘤抑制的阶段特异性细胞周期控制因子的系列喜欢函数。

著录项

  • 来源
    《Developmental cell》 |2018年第3期|共19页
  • 作者单位

    Texas A&

    M Hlth Sci Ctr Dept Mol &

    Cellular Med College Stn TX 77843 USA;

    Curtin Univ Fac Hlth Sci Curtin Hlth Innovat Res Inst Sch Biomed Sci Bentley WA 6102 Australia;

    Univ Ottawa Ottawa Inst Syst Biol Dept Biochem Microbiol &

    Immunol Ottawa ON Canada;

    Texas A&

    M Univ Dept Biochem &

    Biophys College Stn TX 77843 USA;

    Univ Cote Azur CNRS Inst Pharmacol Mol &

    Cellulaire Valbonne France;

    Buck Inst Res Aging 8001 Redwood Blvd Novato CA 94945 USA;

    Dalhousie Univ Atlantic Res Ctr Dept Pediat Halifax NS B3H 4R2 Canada;

    Texas A&

    M Hlth Sci Ctr Dept Mol &

    Cellular Med College Stn TX 77843 USA;

    Univ Ottawa Ottawa Inst Syst Biol Dept Biochem Microbiol &

    Immunol Ottawa ON Canada;

    Buck Inst Res Aging 8001 Redwood Blvd Novato CA 94945 USA;

    Texas A&

    M Univ Dept Chem College Stn TX 77843 USA;

    Univ Ottawa Ottawa Inst Syst Biol Dept Biochem Microbiol &

    Immunol Ottawa ON Canada;

    Texas A&

    M Univ Dept Biochem &

    Biophys College Stn TX 77843 USA;

    Texas A&

    M Hlth Sci Ctr Dept Mol &

    Cellular Med College Stn TX 77843 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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