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截短的激活素I型受体Alk4亚型是抑制激活素信号传导的显性负性受体。

Truncated activin type I receptor Alk4 isoforms are dominant negative receptors inhibiting activin signaling.

作者信息

Zhou Y, Sun H, Danila D C, Johnson S R, Sigai D P, Zhang X, Klibanski A

机构信息

Neuroendocrine Unit, Massachusetts General Hospital and Harvard Medical School, Boston 02114, USA.

出版信息

Mol Endocrinol. 2000 Dec;14(12):2066-75. doi: 10.1210/mend.14.12.0570.

DOI:10.1210/mend.14.12.0570
PMID:11117535
Abstract

Activin, a member of the transforming growth factor beta (TGFbeta) superfamily of cytokines, inhibits cell proliferation in a variety of cell types. The functions of activin are mediated by type I and type II serine/threonine kinase receptors. The main type I receptor mediating activin signaling in human cells is ActRIB, also called Alk4. We have previously reported that several truncated Alk4 receptor isoforms are exclusively expressed in human pituitary tumors, and that the majority of such tumors did not exhibit activin-induced growth arrest in culture. We therefore studied the function of these truncated receptor isoforms. Transient expression of these truncated receptors inhibited activin-activated transcription from an activin-responsive reporter construct, 3TPLux. When each of these truncated Alk4 receptors was stably transfected into K562 cells, activin-induced expression of an endogenous gene, junB, was blocked, indicating that inhibition of gene expression also occurred at the chromosomal level. Furthermore, activin administration failed to cause growth inhibition and an increase of the G1 population in these cells. Coimmunoprecipitation experiments showed that the truncated Alk4 receptors formed complexes with type II activin receptors, but were not phosphorylated. These data indicate that the truncated activin type I receptors, predominantly expressed in human pituitary adenomas, function as dominant negative receptors to interfere with wild-type receptor function and block the antiproliferative effect of activin. This may contribute to uncontrolled pituitary cell growth and the development of human pituitary tumors.

摘要

激活素是细胞因子转化生长因子β(TGFβ)超家族的成员,可抑制多种细胞类型的细胞增殖。激活素的功能由I型和II型丝氨酸/苏氨酸激酶受体介导。在人类细胞中介导激活素信号传导的主要I型受体是ActRIB,也称为Alk4。我们之前报道过,几种截短的Alk4受体亚型仅在人类垂体肿瘤中表达,并且大多数此类肿瘤在培养中未表现出激活素诱导的生长停滞。因此,我们研究了这些截短的受体亚型的功能。这些截短受体的瞬时表达抑制了来自激活素应答报告构建体3TPLux的激活素激活转录。当将这些截短的Alk4受体中的每一个稳定转染到K562细胞中时,激活素诱导的内源性基因junB的表达被阻断,这表明基因表达的抑制也发生在染色体水平。此外,在这些细胞中给予激活素未能导致生长抑制和G1期细胞群增加。免疫共沉淀实验表明,截短的Alk4受体与II型激活素受体形成复合物,但未被磷酸化。这些数据表明,主要在人类垂体腺瘤中表达的截短的激活素I型受体作为显性负性受体发挥作用,干扰野生型受体功能并阻断激活素的抗增殖作用。这可能导致垂体细胞生长失控和人类垂体肿瘤的发生。

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Truncated activin type I receptor Alk4 isoforms are dominant negative receptors inhibiting activin signaling.截短的激活素I型受体Alk4亚型是抑制激活素信号传导的显性负性受体。
Mol Endocrinol. 2000 Dec;14(12):2066-75. doi: 10.1210/mend.14.12.0570.
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