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Peroxisomal membrane proteins contain common Pex19p-binding sites that are an integral part of their targeting signals

机译:过氧化物酶体膜蛋白含有常见的Pex19p结合位点,这是其靶向信号的组成部分

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Targeting of peroxisomal membrane proteins (PMPs) is a multistep process that requires not only recognition of PMPs in the cytosol but also their insertion into the peroxisomal membrane. As a consequence, targeting signals of PMPs (mPTS) are rather complex. A candidate protein for the PMP recognition event is Pex19p, which interacts with most PMPs. However, the respective Pex19p-binding sites are ill-defined and it is currently disputed whether these sites are contained within mPTS. By using synthetic peptide scans and yeast two-hybrid analyses, we determined and characterized Pex19p-binding sites in Pex11p and Pex13p, two PMPs from Saccharomyces cerevisiae. The sites turned out to be composed of a short helical motif with a minimal length of 11 amino acids. With the acquired data, it proved possible to predict and experimentally verify Pex19p-binding sites in several other PMPs by applying a pattern search and a prediction matrix. A peroxisomally targeted Pex13p fragment became mislocalized to the endoplasmic reticulum in the absence of its Pex19p-binding site. By adding the heterologous binding site of Pex11p, peroxisomal targeting of the Pex13p fragment was restored. We conclude that Pex19p-binding sites are well-defined entities that represent an essential part of the mPTS.
机译:靶向过氧化物酶体膜蛋白(PMP)是一个多步骤过程,不仅需要识别胞质溶胶中的PMP,还需要将其插入过氧化物酶体膜中。结果,PMP(mPTS)的目标信号相当复杂。 PMP识别事件的候选蛋白是Pex19p,它与大多数PMP相互作用。但是,各自的Pex19p结合位点定义不清,目前争论这些位点是否包含在mPTS中。通过使用合成肽扫描和酵母双杂交分析,我们确定和表征了来自酿酒酵母的两个PMP Pex11p和Pex13p中的Pex19p结合位点。这些位点由短螺旋基序组成,最小长度为11个氨基酸。利用所获取的数据,通过应用模式搜索和预测矩阵,可以预测和实验验证其他几个PMP中的Pex19p结合位点。在没有Pex19p结合位点的情况下,过氧化物酶体靶向的Pex13p片段错误定位到内质网。通过添加Pex11p的异源结合位点,恢复了Pex13p片段的过氧化物酶体靶向。我们得出结论,Pex19p结合位点是定义明确的实体,代表mPTS的重要组成部分。

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