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配体介导入胞作用和鸟苷酸环化酶/利钠肽受体的细胞内隔离:GDAY 基序的作用。

Ligand-mediated endocytosis and intracellular sequestration of guanylyl cyclase/natriuretic peptide receptors: role of GDAY motif.

机构信息

Department of Physiology, Tulane University School of Medicine, SL-39 1430 Tulane Ave, New Orleans, LA 70112, USA.

出版信息

Mol Cell Biochem. 2010 Jan;334(1-2):81-98. doi: 10.1007/s11010-009-0332-x. Epub 2009 Nov 26.

Abstract

The guanylyl cyclase/natriuretic peptide receptor-A (GC-A/NPRA), also referred to as GC-A, is a single polypeptide molecule having a critical function in blood pressure regulation and cardiovascular homeostasis. GC-A/NPRA, which resides in the plasma membrane, consists of an extracellular ligand-binding domain, a single transmembrane domain, and an intracellular cytoplasmic region containing a protein kinase-like homology domain (KHD) and a guanylyl cyclase (GC) catalytic domain. After binding with atrial and brain natriuretic peptides (ANP and BNP), GC-A/NPRA is internalized and sequestered into intracellular compartments. Therefore, GC-A/NPRA is a dynamic cellular macromolecule that traverses different subcellular compartments through its lifetime. This review describes the roles of short-signal sequences in the internalization, trafficking, and intracellular redistribution of GC-A/NPRA from cell surface to cell interior. Evidence indicates that, after internalization, the ligand-receptor complexes dissociate inside the cell and a population of GC-A/NPRA recycles back to the plasma membrane. Subsequently, the disassociated ligands are degraded in the lysosomes. However, a small percentage of the ligand escapes the lysosomal degradative pathway, and is released intact into culture medium. Using pharmacologic and molecular perturbants, emphasis has been placed on the cellular regulation and processing of ligand-bound GC-A/NPRA in terms of receptor trafficking and down-regulation in intact cells. The discussion is concluded by examining the functions of short-signal sequence motifs in the cellular life-cycle of GC-A/NPRA, including endocytosis, trafficking, metabolic processing, inactivation, and/or down-regulation in model cell systems.

摘要

鸟苷酸环化酶/利钠肽受体-A(GC-A/NPRA),也称为 GC-A,是一种在血压调节和心血管稳态中具有关键功能的单一多肽分子。GC-A/NPRA 位于质膜中,由一个细胞外配体结合域、一个单一的跨膜域和一个包含蛋白激酶样同源域(KHD)和鸟苷酸环化酶(GC)催化域的细胞内细胞质区域组成。与心房利钠肽(ANP)和脑利钠肽(BNP)结合后,GC-A/NPRA 被内化并隔离到细胞内隔室中。因此,GC-A/NPRA 是一种动态的细胞大分子,通过其生命周期在不同的亚细胞隔室中穿梭。本综述描述了短信号序列在 GC-A/NPRA 从细胞表面内化、运输和细胞内再分布到细胞内部的作用。有证据表明,内化后,配体-受体复合物在细胞内解离,一部分 GC-A/NPRA 循环回到质膜。随后,解离的配体在溶酶体中被降解。然而,一小部分配体逃脱了溶酶体降解途径,并完整地释放到培养基中。使用药理学和分子扰动剂,重点研究了配体结合的 GC-A/NPRA 在完整细胞中受体运输和下调方面的细胞调节和加工。通过检查短信号序列基序在 GC-A/NPRA 的细胞生命周期中的功能,包括内吞作用、运输、代谢加工、失活和/或下调,讨论在模型细胞系统中结束。

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