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干扰IIA型和IIB型激活素受体对非洲爪蟾发育的不同影响。

Differential effects on Xenopus development of interference with type IIA and type IIB activin receptors.

作者信息

New H V, Kavka A I, Smith J C, Green J B

机构信息

Division of Developmental Biology, National Institute for Medical Research, Ridgeway, London, UK.

出版信息

Mech Dev. 1997 Jan;61(1-2):175-86. doi: 10.1016/s0925-4773(96)00639-9.

Abstract

One candidate for a mesoderm-inducing factor in early amphibian development is activin, a member of the TGF beta family. Overexpression of a truncated form of an activin receptor Type IIB abolishes activin responsiveness and mesoderm formation in vivo. The Xenopus Type IIA activin receptor XSTK9 differs from the Type IIB receptor by 43 and 25% in extracellular and intracellular domains respectively, suggesting the possibility of different functions in vivo. In this paper, we compare the Type IIA receptor with the Type IIB to test such a possibility. Simple overexpression of the wild-type receptors reveals minimal differences, but experiments with dominant negative mutants of each receptor show qualitatively distinct effects. We show that while truncated (kinase domain-deleted) Type IIB receptors cause axial defects as previously described, truncated type IIA receptors cause formation of secondary axes, similar to those seen by overexpression of truncated receptors for BMP-4, another TGF beta family member. Furthermore, in animal cap assays, truncated type IIB receptors inhibit induction of all mesodermal markers tested, while truncated type IIA receptors suppress induction only of ventral markers; the anterior/dorsal marker goosecoid is virtually unaffected. The suppression of ventral development by the type IIA truncated receptor suggests either that the truncated Type IIA receptor interferes with ventral BMP pathways, or that activin signaling through the Type IIA receptor is necessary for ventral patterning.

摘要

在两栖动物早期发育中,一种中胚层诱导因子的候选物质是激活素,它是转化生长因子β(TGFβ)家族的成员之一。在体内,截短形式的IIB型激活素受体的过表达会消除激活素反应性和中胚层形成。非洲爪蟾的IIA型激活素受体XSTK9在细胞外和细胞内结构域分别与IIB型受体有43%和25%的差异,这表明其在体内可能具有不同的功能。在本文中,我们比较了IIA型受体和IIB型受体以检验这种可能性。野生型受体的简单过表达显示出极小的差异,但对每个受体的显性负性突变体进行的实验显示出质的不同影响。我们发现,虽然截短的(缺失激酶结构域的)IIB型受体如前所述会导致轴向缺陷,但截短的IIA型受体却会导致副轴形成,这与另一个TGFβ家族成员BMP-4的截短受体过表达时所观察到的情况相似。此外,在动物帽实验中,截短的IIB型受体抑制了所有测试的中胚层标记物的诱导,而截短的IIA型受体仅抑制腹侧标记物的诱导;前/背侧标记物鹅膏蕈氨酸几乎不受影响。IIA型截短受体对腹侧发育的抑制表明,要么截短的IIA型受体干扰了腹侧BMP信号通路,要么通过IIA型受体的激活素信号传导对于腹侧模式形成是必需的。

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