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首页> 外文期刊>Journal of Cell Science >Interaction between secretogranin III and carboxypeptidase E facilitates prohormone sorting within secretory granules.
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Interaction between secretogranin III and carboxypeptidase E facilitates prohormone sorting within secretory granules.

机译:促分泌素颗粒III和羧肽酶E之间的相互作用促进了促分泌素在分泌颗粒中的分选。

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摘要

Secretogranin III (SgIII) and carboxypeptidase E (CPE) bind specifically to cholesterol-rich secretory granule (SG) membranes. We previously showed that SgIII binds chromogranin A (CgA) and targets CgA to the SGs in endocrine cells. We investigated the binding of SgIII and CPE because they frequently localize close to the periphery of SGs, and they bind each other in mouse corticotrope-derived AtT-20 cells. In Cpe(fat) mouse corticotropes, which have defective CPE, proopiomelanocortin (POMC)-derived adrenocorticotrophin hormone (ACTH)-containing peptides were distributed over the entire surface of the SGs, and displayed a regulated secretion by secretagogues. The Cpe(fat) pituitary exhibited elevated levels of SgIII and CgA, which suggests that they compensate for a sorting function of CPE for POMC and its intermediates to ACTH. Indeed, both SgIII and CgA were able to bind POMC-derived intermediates. In a competitive pull-down assay, excessive SgIII led to a decrease in CPE-bound POMC-derived intermediate molecules, and SgIII pulled-down by anti-ACTH antibody increased proportionately. We suggest that SgIII and CPE form the separate functional sorting complex by anchoring to cholesterol-rich SG membranes, and POMC-derived peptides are transferred from CPE to SgIII, and subsequently to CgA.
机译:Secretogranin III(SgIII)和羧肽酶E(CPE)与富含胆固醇的分泌颗粒(SG)膜特异性结合。我们先前显示SgIII结合嗜铬粒蛋白A(CgA),并将CgA靶向内分泌细胞中的SGs。我们调查了SgIII和CPE的结合,因为它们经常位于SGs的外围附近,并且在小鼠皮质激素衍生的AtT-20细胞中彼此结合。在具有CPE缺陷的Cpe(fat)小鼠促肾上腺皮质激素中,含有促黑素皮质激素(POMC)的促肾上腺皮质激素(ACTH)肽段分布在SGs的整个表面上,并通过促分泌剂显示出调节的分泌。 Cpe(fat)垂体的SgIII和CgA含量升高,表明它们补偿了CPE对POMC及其中间产物至ACTH的分选功能。实际上,SgIII和CgA都能够结合POMC衍生的中间体。在竞争性下拉测定中,过量的SgIII导致CPE结合的POMC衍生的中间分子减少,而被抗ACTH抗体下拉的SgIII则成比例增加。我们建议SgIII和CPE通过锚定到富含胆固醇的SG膜上形成单独的功能分类复合物,并且POMC衍生的肽从CPE转移到SgIII,然后转移到CgA。

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