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果蝇卷曲信号肽异常长,是信号肽肽酶的底物。

The Drosophila Crumbs signal peptide is unusually long and is a substrate for signal peptide peptidase.

机构信息

Zentrum für Molekulare Biologie der Universität Heidelberg, DKFZ-ZMBH-Allianz, Universität Heidelberg, Im Neuenheimer Feld 282, 69120 Heidelberg, Germany.

出版信息

Eur J Cell Biol. 2010 Jun;89(6):449-61. doi: 10.1016/j.ejcb.2010.02.001. Epub 2010 Mar 1.

DOI:10.1016/j.ejcb.2010.02.001
PMID:20189678
Abstract

N-terminal signal sequences mediate nascent protein targeting to and protein insertion into the membrane of the endoplasmic reticulum. They are typically 15-30 amino acid residues long with a core hydrophobic region flanked by an N-terminal (n-) and a C-terminal region. Following cleavage by signal peptidase, some of the resulting signal peptides are further processed by signal peptide peptidase (SPP) and fragments are liberated into the cytosol. Such fragments can have independent, post-targeting functions affecting diverse cellular processes. We show that Drosophila melanogaster Crumbs, a transmembrane protein controlling cell polarity and morphogenesis, is synthesized with an 83 residues-long signal sequence. To our knowledge, this is currently the longest signal sequence described for an eukaryotic protein. The unusual length is caused by an extended n-region, but the extension does neither affect protein targeting nor signal sequence cleavage. The signal sequence is cleaved off and the resulting signal peptide, SP(Crb), is proteolytically processed by SPP, thus representing the first substrate described for the Drosophila enzyme. We further show that signal peptide fragments can be degraded by the proteasome. Expression of transgenes encoding tagged variants of Crumbs in Drosophila embryos suggests that the signal peptide is short-lived in vivo. Our findings support a model suggesting that besides generating fragments with post-targeting functions, SPP-mediated processing is the first step in the degradation of signal peptides.

摘要

N 端信号序列介导新生蛋白靶向和插入内质网膜。它们通常长 15-30 个氨基酸残基,核心疏水区两侧分别为 N 端(n-)和 C 端区域。在信号肽酶切割后,一些产生的信号肽进一步被信号肽肽酶(SPP)加工,片段被释放到细胞质中。这些片段可以具有独立的、靶向后的功能,影响多种细胞过程。我们表明,控制细胞极性和形态发生的果蝇黑色素瘤 Crumbs 是一种跨膜蛋白,其合成时有一个 83 个残基长的信号序列。据我们所知,这是目前描述的真核蛋白中最长的信号序列。这种不寻常的长度是由于 n 区域的延长,但这种延长既不影响蛋白质靶向,也不影响信号序列的切割。信号序列被切断,产生的信号肽 SP(Crb)被 SPP 蛋白水解加工,因此代表了该果蝇酶的第一个底物。我们进一步表明,信号肽片段可以被蛋白酶体降解。在果蝇胚胎中表达编码 Crumbs 标记变体的转基因表明,信号肽在体内是短寿命的。我们的发现支持这样一种模型,即除了产生具有靶向后功能的片段外,SPP 介导的加工是信号肽降解的第一步。

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The Crumbs_C isoform of shows tissue- and stage-specific expression and prevents light-dependent retinal degeneration.的Crumbs_C亚型表现出组织和阶段特异性表达,并可预防光依赖性视网膜变性。
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Drosophila signal peptidase complex member Spase12 is required for development and cell differentiation.果蝇信号肽酶复合物成员 Spase12 对于发育和细胞分化是必需的。
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