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首页> 外文期刊>Nature Communications >Stochastic palmitoylation of accessible cysteines in membrane proteins revealed by native mass spectrometry
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Stochastic palmitoylation of accessible cysteines in membrane proteins revealed by native mass spectrometry

机译:天然质谱揭示膜蛋白中可及的半胱氨酸的随机棕榈酰化

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摘要

Palmitoylation affects membrane partitioning, trafficking and activities of membrane proteins. However, how specificity of palmitoylation and multiple palmitoylations in membrane proteins are determined is not well understood. Here, we profile palmitoylation states of three human claudins, human CD20 and cysteine-engineered prokaryotic KcsA and bacteriorhodopsin by native mass spectrometry. Cysteine scanning of claudin-3, KcsA, and bacteriorhodopsin shows that palmitoylation is independent of a sequence motif. Palmitoylations are observed for cysteines exposed on the protein surface and situated up to 8?? into the inner leaflet of the membrane. Palmitoylation on multiple sites in claudin-3 and CD20 occurs stochastically, giving rise to a distribution of palmitoylated membrane-protein isoforms. Non-native sites in claudin-3 indicate that membrane-protein function imposed evolutionary restraints on native palmitoylation sites. These results suggest a generic, stochastic membrane-protein palmitoylation process that is determined by the accessibility of palmitoyl-acyl transferases to cysteines on membrane-embedded proteins, and not by a preferred substrate-sequence motif.
机译:棕榈酰化影响膜蛋白的膜分配,运输和活性。然而,如何确定膜蛋白中棕榈酰化和多个棕榈酰化的特异性尚不清楚。在这里,我们通过自然质谱分析了三种人类claudins,人类CD20和半胱氨酸工程化的原核生物KcsA和细菌视紫红质的棕榈酰化状态。半胱氨酸对claudin-3,KcsA和细菌视紫红质的扫描显示棕榈酰化与序列基序无关。观察到暴露于蛋白质表面且位于最高达8′′的半胱氨酸的棕榈酰化作用。进入膜的内部小叶。 claudin-3和CD20中多个位点的棕榈酰化是随机发生的,从而导致棕榈酰化膜蛋白同工型的分布。 claudin-3中的非天然位点表明膜蛋白功能对天然棕榈酰化位点施加了进化限制。这些结果表明,一般的,随机的膜蛋白棕榈酰化过程是由棕榈酰酰基转移酶与膜包埋蛋白上的半胱氨酸的可及性决定的,而不是由优选的底物序列基序决定的。

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