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人绒毛膜促性腺激素β亚基羧基末端延伸的生物学作用[已校正]

The biological role of the carboxyl-terminal extension of human chorionic gonadotropin [corrected] beta-subunit.

作者信息

Matzuk M M, Hsueh A J, Lapolt P, Tsafriri A, Keene J L, Boime I

机构信息

Department of Pharmacology, Washington University School of Medicine, St. Louis, Missouri 63110.

出版信息

Endocrinology. 1990 Jan;126(1):376-83. doi: 10.1210/endo-126-1-376.

Abstract

hCG is a member of a family of glycoprotein hormones which share a common alpha-subunit, but differ in their hormone-specific beta-subunits. The CG beta-subunit is unique in that it contains a hydrophilic carboxyl-terminal extension with four serine O-linked oligosaccharides. To examine the role of the O-linked oligosaccharides and the carboxyl-terminal extension of hCG beta on receptor binding, steroidogenesis in vitro, and ovulation induction in vivo, site-directed mutagenesis and gene transfer methods were used. Wild-type hCG alpha and hCG beta expression vectors were transfected into an O-glycosylation mutant Chinese hamster ovary cell line to produce intact dimer hCG lacking the beta-subunit O-linked oligosaccharide units. In addition, a mutant hCG beta gene (CG beta delta T) was generated which contained a premature termination signal at codon 115. This gene was cotransfected with the hCG alpha gene into Chinese hamster ovary cells to produce hCG dimer which lacked the carboxyl-terminal amino acids 115-145 of hCG beta (truncated hCG). The O-linked oligosaccharide deficient or truncated hCG derivatives were examined for their ability to bind to the mouse LH/hCG receptor and stimulate cAMP and steroidogenesis in vitro. These studies show that the O-linked oligosaccharides and carboxyl-terminal extension play a minor role in receptor binding and signal transduction. In contrast, comparison of the stimulatory effects of truncated and wild-type hCG in a rat ovulation assay in vivo via either intrabursal or iv injection revealed that the truncated derivative was approximately 3-fold less active than wild-type hCG. These findings indicate that the carboxyl-terminal extension of hCG beta and associated O-linked oligosaccharides are not important for receptor binding or in vitro signal transduction, but are critical for in vivo biological responses.

摘要

人绒毛膜促性腺激素(hCG)是糖蛋白激素家族的一员,该家族成员共享一个共同的α亚基,但激素特异性β亚基不同。绒毛膜促性腺激素β亚基(CGβ)的独特之处在于它包含一个亲水性羧基末端延伸部分,带有四个丝氨酸O-连接寡糖。为了研究hCGβ的O-连接寡糖和羧基末端延伸在受体结合、体外类固醇生成以及体内排卵诱导中的作用,采用了定点诱变和基因转移方法。将野生型hCGα和hCGβ表达载体转染到O-糖基化突变的中国仓鼠卵巢细胞系中,以产生缺乏β亚基O-连接寡糖单元的完整二聚体hCG。此外,还产生了一个突变的hCGβ基因(CGβδT),该基因在第115密码子处含有一个提前终止信号。将该基因与hCGα基因共转染到中国仓鼠卵巢细胞中,以产生缺乏hCGβ羧基末端氨基酸115 - 145的hCG二聚体(截短型hCG)。检测了O-连接寡糖缺陷型或截短型hCG衍生物与小鼠促黄体生成素/人绒毛膜促性腺激素(LH/hCG)受体结合以及体外刺激环磷酸腺苷(cAMP)和类固醇生成的能力。这些研究表明,O-连接寡糖和羧基末端延伸在受体结合和信号转导中起次要作用。相比之下,通过囊内注射或静脉注射在体内大鼠排卵试验中比较截短型和野生型hCG的刺激作用发现,截短型衍生物的活性比野生型hCG低约3倍。这些发现表明,hCGβ的羧基末端延伸和相关的O-连接寡糖对受体结合或体外信号转导并不重要,但对体内生物学反应至关重要。

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