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Sorting nexin 31 binds multiple β integrin cytoplasmic domains and regulates β1 integrin surface levels and stability

机译:分选nexin 31结合多个β整合素胞质域并调节β1整合素表面水平和稳定性

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摘要

Trafficking of α5β1 integrin to lysosomes and its subsequent degradation is influenced by ligand occupancy and the binding of SNX17 via its protein 4.1, ezrin, radixin, moesin (FERM) domain to the membrane-distal NPxY motif in the cytoplasmic domain of β1 integrin in early endosomes. Two other sorting nexin (SNX) family members, namely SNX27 and SNX31, share with SNX17 next to their obligate phox domain a FERM domain, which may enable them to bind β integrin tails. Here we report that, in addition to SNX17, SNX31 but not SNX27 binds several β integrin tails in early endosomes in a PI3 (phosphatidylinositide 3)-kinase-dependent manner. Similarly like SNX17, binding of SNX31 with β1 integrin tails in early endosomes occurs between the FERM domain and the membrane-distal NPxY motif in the β1 integrin cytoplasmic domain. Furthermore, expression of SNX31 rescues β1 integrin surface levels and stability in SNX17-depleted cells. In contrast to SNX17, expression of SNX31 is restricted and found highly expressed in bladder and melanoma tissue. Altogether, these results demonstrate that SNX31 is an endosomal regulator of β integrins with a restricted expression pattern.
机译:α5β1整联蛋白向溶酶体的运输及其随后的降解受配体占据和SNX17经由其蛋白4.1,ezrin,radixin,moesin(FERM)结构域与早期β1整联蛋白胞质结构域中的膜远端NPxY基序的结合的影响内体。 SNX27和SNX31这两个其他排序nexin(SNX)家族成员在其专用phox域旁边与SNX17共享一个FERM域,这可能使它们能够结合β整联蛋白尾巴。在这里我们报告,除了SNX17,SNX31但不是SNX27以PI3(磷脂酰肌醇3)-激酶依赖性方式结合早期内体中的多个β整联蛋白尾巴。与SNX17类似,SNX31与早期内体中β1整合素尾部的结合发生在FERM域和β1整合素胞质域中的膜远端NPxY基序之间。此外,SNX31的表达可挽救SNX17缺失细胞中的β1整合素表面水平和稳定性。与SNX17相反,SNX31的表达受到限制,并在膀胱和黑色素瘤组织中高度表达。总而言之,这些结果表明SNX31是β整联蛋白的内体调节剂,其表达模式受到限制。

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