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抑制素B和抑制素结合蛋白(INhBP)对激活素信号转导的调节作用。

Modulation of activin signal transduction by inhibin B and inhibin-binding protein (INhBP).

作者信息

Chapman S C, Woodruff T K

机构信息

Department of Neurobiology and Physiology, Northwestern University, Evanston, Illinois 60208-2850, USA.

出版信息

Mol Endocrinol. 2001 Apr;15(4):668-79. doi: 10.1210/mend.15.4.0616.

DOI:10.1210/mend.15.4.0616
PMID:11266516
Abstract

An antagonistic relationship between inhibin and activin is essential to the control of pituitary FSH release and to normal gonadal function. Two inhibin ligands, inhibin A and inhibin B, are made by the ovary in females, and each regulate pituitary FSH at different times during the reproductive cycle. Inhibin B, but not inhibin A, is produced by the testes and is therefore responsible for all inhibin-dependent FSH regulation in males. Although the activin signal transduction pathway has been well characterized, little is known about the mechanism of inhibin signaling and its relationship to activin antagonism. A recently cloned inhibin-binding protein, InhBP (p120), associates strongly with the type IB activin receptor (Alk4) in a ligand-responsive manner and interacts to a lesser extent with other activin and bone morphogenetic protein (BMP) type I and activin type II receptors. Activin stimulates the association of InhBP and Alk4, and inhibin B, but not inhibin A, interferes with InhBP-Alk4 complex formation. InhBP is necessary to mediate a specific antagonistic effect of inhibin B on activin-stimulated transcription. Appropriate stoichiometry between InhBP and the activin type I receptor is crucial to InhBP function. These findings suggest that InhBP is an inhibin B-specific receptor that mediates antagonism of activin signal transduction through the modulation of activin heteromeric receptor complex assembly.

摘要

抑制素与激活素之间的拮抗关系对于垂体促卵泡激素(FSH)释放的控制及正常性腺功能至关重要。抑制素的两种配体,即抑制素A和抑制素B,由雌性卵巢产生,且在生殖周期的不同时间调节垂体FSH。抑制素B而非抑制素A由睾丸产生,因此负责男性中所有依赖抑制素的FSH调节。尽管激活素信号转导途径已得到充分表征,但对于抑制素信号传导机制及其与激活素拮抗作用的关系知之甚少。最近克隆的一种抑制素结合蛋白InhBP(p120)以配体反应性方式与IB型激活素受体(Alk4)强烈结合,且与其他激活素及骨形态发生蛋白(BMP)I型和激活素II型受体的相互作用程度较低。激活素刺激InhBP与Alk4的结合,而抑制素B而非抑制素A会干扰InhBP - Alk4复合物的形成。InhBP是介导抑制素B对激活素刺激转录的特异性拮抗作用所必需的。InhBP与激活素I型受体之间适当的化学计量对于InhBP的功能至关重要。这些发现表明,InhBP是一种抑制素B特异性受体,其通过调节激活素异源受体复合物的组装来介导激活素信号转导的拮抗作用。

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