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首页> 外文期刊>Nucleic Acids Research >The moonlighting RNA-binding activity of cytosolic serine hydroxymethyltransferase contributes to control compartmentalization of serine metabolism
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The moonlighting RNA-binding activity of cytosolic serine hydroxymethyltransferase contributes to control compartmentalization of serine metabolism

机译:细胞溶质丝氨酸羟甲基转移酶的融合RNA结合活性有助于控制丝氨酸代谢的分区化

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摘要

Enzymes of intermediary metabolism are often reported to have moonlighting functions as RNA-binding proteins and have regulatory roles beyond their primary activities. Human serine hydroxymethyltransferase (SHMT) is essential for the onecarbon metabolism, which sustains growth and proliferation in normal and tumour cells. Here, we characterize the RNA-binding function of cytosolic SHMT (SHMT1) in vitro and using cancer cell models. We show that SHMT1 controls the expression of its mitochondrial counterpart (SHMT2) by binding to the 5'untranslated region of the SHMT2 transcript (UTR2). Importantly, binding to RNA is modulated by metabolites in vitro and the formation of the SHMT1-UTR2 complex inhibits the serine cleavage activity of the SHMT1, without affecting the reverse reaction. Transfection of UTR2 in cancer cells controls SHMT1 activity and reduces cell viability. We propose a novel mechanism of SHMT regulation, which interconnects RNA and metabolites levels to control the cross-talk between cytosolic and mitochondrial compartments of serine metabolism.
机译:通常据报道,中间代谢的酶呈态度为RNA结合蛋白,并且具有超出其主要活动的调节作用。人丝氨酸羟甲基转移酶(SHMT)对于oneCarbon代谢至关重要,其在正常和肿瘤细胞中维持生长和增殖。这里,我们在体外表征细胞溶质Shmt(Shmt1)的RNA结合功能,并使用癌细胞模型。我们表明SHMT1通过结合SHMT2转录物(UTR2)的5'unralstalated区域来控制其线粒体对应物(SHMT2)的表达。重要的是,通过体外代谢物调节与RNA的结合,并且SHMT1-UTR2复合物的形成抑制SHMT1的丝氨酸切割活性,而不会影响反应反应。 UTR2在癌细胞中的转染对照SHMT1活性并降低细胞活力。我们提出了一种新的SHMT调节机制,其互连RNA和代谢物水平来控制丝氨酸代谢的细胞溶质和线粒体间隔之间的串扰。

著录项

  • 来源
    《Nucleic Acids Research》 |2019年第8期|共15页
  • 作者单位

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Catalan Inst Oncol Program Canc Therapeut Resistance ProCURE Metab &

    Canc Grp Girona 17007 Catalonia Spain;

    Sapienza Univ Rome Dept Biol &

    Biotechnol C Darwin I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Barcelona Inst Sci &

    Technol Ctr Genom Regulat CRG Dr Aiguader 88 Barcelona 08003 Spain;

    Sapienza Univ Rome Dept Biol &

    Biotechnol C Darwin I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

    Sapienza Univ Rome Dept Biochem Sci Ple Aldo Moro 5 I-00185 Rome Italy;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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