一种新的爪蟾骨形态发生蛋白-7 (BMP-7)同源物

Shouwen Wang, Marie Krinks, Logan Kleinwaks, Malcolm Moos
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引用次数: 33

摘要

我们发现了与哺乳动物骨形态发生蛋白(BMP)-7(也称为成骨蛋白-1或OP-1)密切相关的aXenopus基因。它与先前描述的非洲爪蟾同源基因(最初称为XBMP-7)相比,在初级结构和表达模式上与哺乳动物基因相似得多[Nishimatsu, Suzuki, Shoda, Murakami和Ueno (1992) Biochem]。Biophys。[参考文献]。因此,新基因被命名为XBMP-7,先前描述的基因被重新命名为XBMP-7R (M. Moos和N. Ueno,未发表作品)。它分布广泛,主要在原肠胚形成期间的前腹和后腹区,随后在不同阶段在各种结构(眼睛、神经结构、心脏、肾前、后腹区等结构)中突出,与XBMP-4的分布密切相似。但在原肠胚期,其表达开始晚于XBMP-4。胚胎的锂处理集中了XBMP-7在扩大的眼睛和心脏结构中的表达。腹侧过表达XBMP-7可产生大的突出,最终形成血红蛋白特征的着色,α-珠蛋白的显著扩增证实了这一点。背侧过表达抑制背前结构。过表达XBMP-7的动物帽的分子分析显示,诱导了与腹侧和造血组织相关的标记,这与全胚胎过表达的结果一致。XBMP-7对珠蛋白的诱导可以被截断的BMP受体阻断,这表明XBMP-7也与该受体相互作用。我们的数据支持XBMP-7可能在胚胎发生过程中发挥多种作用的概念,并提示可能在血液发生中起作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A novel Xenopus homologue of bone morphogenetic protein-7 (BMP-7)

We identified aXenopus gene closely related to mammalian bone morphogenetic protein (BMP)-7 (also termed osteogenic protein-1 or OP-1). It resembles the mammalian gene in primary structure and expression pattern much more closely than does a previously described Xenopus homologue, originally termed XBMP-7 [Nishimatsu, Suzuki, Shoda, Murakami and Ueno (1992) Biochem. Biophys. Res. Commun. 186, 1487–1495]. The novel gene has therefore been designated XBMP-7 and the gene described earlier has been renamed XBMP-7R (M. Moos and N. Ueno, unpublished work). It has a broad distribution, primarily in the anterior and posterior ventral regions during gastrulation, subsequently becoming prominent at different stages in a wide variety of structures (eyes, neural structures, heart, pronephros, posterior ventral region and other structures), paralleling the distribution of XBMP-4 closely. However, its expression begins later than that of XBMP-4 during gastrulation. Lithium treatment of embryos concentrates the XBMP-7 expression in the expanded eye and heart structures. Ventral overexpression of XBMP-7 produces large protrusions that ultimately develop colouration characteristic of haemoglobin, which is confirmed by markedly expanded expression of α-globin. Dorsal overexpression suppresses dorsal anterior structures. Molecular analysis of animal caps overexpressing XBMP-7 reveals induction of markers associated with ventral and haematopoietic tissue, which is consistent with whole-embryo overexpression results. Globin induction by XBMP-7 can be blocked by a truncated BMP receptor previously shown to interrupt BMP-4 signalling, indicating XBMP-7 also interacts with this receptor. Our data support the concept that XBMP-7 may play a variety of roles during embryogenesis, and suggest a possible role in haematogenesis.

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