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艾滋病病毒1型辅助受体APJ的内源性配体apelin-13肽的结构与功能研究

Structural and functional study of the apelin-13 peptide, an endogenous ligand of the HIV-1 coreceptor, APJ.

作者信息

Fan Xuejun, Zhou Naiming, Zhang Xiaoling, Mukhtar Muhammad, Lu Zhixian, Fang Jianhua, DuBois Garrett C, Pomerantz Roger J

机构信息

Kimmel Cancer Center, Thomas Jefferson University, Philadelphia, Pennsylvania 19107, USA.

出版信息

Biochemistry. 2003 Sep 2;42(34):10163-8. doi: 10.1021/bi030049s.

Abstract

The APJ receptor is widely expressed in the human central nervous system (CNS). Apelin was recently identified as the endogenous peptidic ligand for human APJ. Studies with animal models suggested that APJ and apelin play an important role in the hypothalamic regulation of water intake and the endocrine axis, in the regulation of blood pressure, and in cardiac contractility. Apelin has been found to block the activity of APJ as a human immunodeficiency virus type I (HIV-1) coreceptor. In this study, we combined chemical synthetic approaches with alanine substitution to evaluate the structural requirements for interactions with the APJ receptor. We demonstrated that apelin peptides in aqueous solution adopt a random conformation, and the positive charge and hydrophobic residues of apelin-13 play important roles in interactions with the APJ receptor. We have observed an important correlation between receptor binding affinity and cell-cell fusion inhibitory activity. The elucidation of structural requirements of apelin-13 in its interaction with the APJ receptor is critical for further investigation of apelin-APJ functions in vivo and in the design of small molecular inhibitors for potential treatment of HIV-1 infection in the CNS.

摘要

APJ受体在人类中枢神经系统(CNS)中广泛表达。Apelin最近被确定为人类APJ的内源性肽配体。动物模型研究表明,APJ和apelin在下丘脑对水摄入和内分泌轴的调节、血压调节以及心脏收缩性方面发挥重要作用。已发现Apelin作为I型人类免疫缺陷病毒(HIV-1)共受体可阻断APJ的活性。在本研究中,我们将化学合成方法与丙氨酸取代相结合,以评估与APJ受体相互作用的结构要求。我们证明,水溶液中的apelin肽呈随机构象,apelin-13的正电荷和疏水残基在与APJ受体的相互作用中起重要作用。我们观察到受体结合亲和力与细胞-细胞融合抑制活性之间存在重要相关性。阐明apelin-13与APJ受体相互作用的结构要求对于进一步研究apelin-APJ在体内的功能以及设计用于潜在治疗CNS中HIV-1感染的小分子抑制剂至关重要。

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