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首页> 外文期刊>Journal of Cell Science >Phosphorylation of the Bruchpilot N-terminus in Drosophila unlocks axonal transport of active zone building blocks
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Phosphorylation of the Bruchpilot N-terminus in Drosophila unlocks axonal transport of active zone building blocks

机译:果蝇中Bruchpilot n-末端的磷酸化解锁了有源区积木的轴突运输

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摘要

Protein scaffolds at presynaptic active zone membranes control information transfer at synapses. For scaffold biogenesis and maintenance, scaffold components must be safely transported along axons. A spectrum of kinases has been suggested to control transport of scaffold components, but direct kinase-substrate relationships and operational principles steering phosphorylation-dependent active zone protein transport are presently unknown. Here, we show that extensive phosphorylation of a 150-residue unstructured region at the N-terminus of the highly elongated Bruchpilot (BRP) active zone protein is crucial for ordered active zone precursor transport in Drosophila. Point mutations that block SRPK79D kinase-mediated phosphorylation of the BRP N-terminus interfered with axonal transport, leading to BRP-positive axonal aggregates that also contain additional active zone scaffold proteins. Axonal aggregates formed only in the presence of non-phosphorylatable BRP isoforms containing the SRPK79D-targeted N-terminal stretch. We assume that specific active zone proteins are pre-assembled in transport packages and are thus co-transported as functional scaffold building blocks. Our results suggest that transient post-translational modification of a discrete unstructured domain of the master scaffold component BRP blocks oligomerization of these building blocks during their long-range transport.
机译:突触前有源区膜在突触突触的蛋白质支架控制信息传递。对于脚手架生物发生和维护,必须安全地沿着轴索安全地运输脚手架部件。已经提出了一种激酶来控制支架组分的传输,但是直接激酶 - 基质关系和转向磷酸化依赖性有源区蛋白转运的操作原理是目前未知的。这里,我们表明,在高度细长的Bruchpilot(BRP)有源区蛋白的N-末端的150-残基非结构化区域的广泛磷酸化对于果蝇中有序的有源区前体转运至关重要。阻断SRPK79D激酶介导的BRP N-末端的激酶介导的点突变干扰了轴突运输,导致BRP阳性轴理聚集体,其还含有另外的有源区支架蛋白。轴突聚集体仅在含有SRPK79D靶向N-末端拉伸的非磷酸化BRP同种型的存在下形成。我们假设特定的有源区蛋白质在运输包装中预先组装,因此作为功能性脚手架构造块共传送。我们的研究结果表明,在其远程运输期间,主支架组分BRP的离散非结构化结构域的分立非结构化结构域的瞬态翻译后修改。

著录项

  • 来源
    《Journal of Cell Science 》 |2019年第6期| 共14页
  • 作者单位

    Free Univ Berlin Inst Chem &

    Biochem Lab Struct Biochem Takustr 6 D-14195 Berlin Germany;

    Free Univ Berlin Inst Biol Lab Genet Takustr 6 D-14195 Berlin Germany;

    Free Univ Berlin Inst Biol Lab Genet Takustr 6 D-14195 Berlin Germany;

    Free Univ Berlin Inst Biol Lab Genet Takustr 6 D-14195 Berlin Germany;

    Free Univ Berlin Inst Chem &

    Biochem Lab Prot Biochem Thielallee 63 D-14195 Berlin Germany;

    Free Univ Berlin Inst Chem &

    Biochem Lab Prot Biochem Thielallee 63 D-14195 Berlin Germany;

    Free Univ Berlin Inst Biol Lab Genet Takustr 6 D-14195 Berlin Germany;

    Free Univ Berlin Inst Biol Lab Genet Takustr 6 D-14195 Berlin Germany;

    Leibniz Forschungsinst Mol Pharmakol Cellular Imaging Robert Roessle Str 10 D-13125 Berlin;

    Karl Franzens Univ Graz Inst Pharmaceut Sci Pharmaceut Chem Univ Pl 1-1 A-8010 Graz Austria;

    Leibniz Inst Analyt Wissensch ISAS eV Bunsen Kirchhoff Str 11 D-44139 Dortmund Germany;

    Leibniz Inst Analyt Wissensch ISAS eV Bunsen Kirchhoff Str 11 D-44139 Dortmund Germany;

    Free Univ Berlin Inst Chem &

    Biochem Lab Prot Biochem Thielallee 63 D-14195 Berlin Germany;

    Free Univ Berlin Inst Biol Lab Genet Takustr 6 D-14195 Berlin Germany;

    Free Univ Berlin Inst Chem &

    Biochem Lab Struct Biochem Takustr 6 D-14195 Berlin Germany;

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

    Active zone; Axonal transport; Bruchpilot; SRPK79D; Synapse; Phosphorylation;

    机译:有源区;轴突运输;Bruchpilot;srpk79d;synapst;磷酸化;

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