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羧肽酶E是一种激素原分选受体,通过C末端跨膜插入锚定在分泌颗粒上。

Carboxypeptidase E, a prohormone sorting receptor, is anchored to secretory granules via a C-terminal transmembrane insertion.

作者信息

Dhanvantari Savita, Arnaoutova Irina, Snell Chris R, Steinbach Peter J, Hammond Kelli, Caputo Gregory A, London Erwin, Loh Y Peng

机构信息

Section on Cellular Neurobiology, Laboratory of Developmental Neurobiology, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892-4480, USA.

出版信息

Biochemistry. 2002 Jan 8;41(1):52-60. doi: 10.1021/bi015698n.

DOI:10.1021/bi015698n
PMID:11772002
Abstract

Carboxypeptidase E (CPE) is a sorting receptor that directs the prohormone pro-opiomelanocortin (POMC) to the regulated secretory pathway, and is also a prohormone processing enzyme in neuro/endocrine cells. It has been suggested that the 25 C-terminal amino acids are necessary for the binding of CPE to secretory granule membranes, but its orientation in the membrane is not known. In this study, we examined the structure and orientation of the membrane-binding domain at the C-terminus of CPE. In vitro experiments using model membranes demonstrated that the last 22 amino acids of CPE (CP peptide) insert in a shallow orientation into lipid bilayers at low pH. Circular dichroism analysis indicated that the CP peptide adopts a partial alpha-helical configuration at low pH, and helix content increases when it is bound to lipid. Protease protection experiments, immunolabeling, and immunoisolation of intact secretory granules with a C-terminal antibody revealed a cytoplasmic domain in CPE, consistent with a transmembrane orientation of this protein. We conclude that the membrane-binding domain of CPE must adopt an alpha-helical configuration to bind to lipids, and that CPE may require another integral membrane "chaperone" protein to insert through the lipid bilayer in a transmembrane fashion.

摘要

羧肽酶E(CPE)是一种分选受体,可将激素原阿黑皮素原(POMC)导向调节性分泌途径,并且还是神经/内分泌细胞中的一种激素原加工酶。有人提出,CPE的25个C末端氨基酸对于CPE与分泌颗粒膜的结合是必需的,但其在膜中的方向尚不清楚。在本研究中,我们研究了CPE C末端膜结合结构域的结构和方向。使用模型膜的体外实验表明,CPE的最后22个氨基酸(CP肽)在低pH值下以浅方向插入脂质双层。圆二色性分析表明,CP肽在低pH值下采用部分α-螺旋构型,并且在与脂质结合时螺旋含量增加。蛋白酶保护实验、免疫标记以及用C末端抗体对完整分泌颗粒进行免疫分离揭示了CPE中的一个胞质结构域,这与该蛋白的跨膜方向一致。我们得出结论,CPE的膜结合结构域必须采用α-螺旋构型才能与脂质结合,并且CPE可能需要另一种整合膜“伴侣”蛋白以跨膜方式插入脂质双层。

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