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成纤维细胞生长因子信号传导将原始血岛限制于腹侧中胚层。

FGF signaling restricts the primary blood islands to ventral mesoderm.

作者信息

Kumano G, Smith W C

机构信息

Department of Molecular, Cellular and Developmental Biology, University of California at Santa Barbara, Santa Barbara, California 93106, USA.

出版信息

Dev Biol. 2000 Dec 15;228(2):304-14. doi: 10.1006/dbio.2000.9937.

Abstract

According to the three-signal model of mesoderm patterning in Xenopus, all mesoderm, with the exception of the Spemann organizer, is originally specified as ventral type, such as lateral plate and primary blood islands. It is proposed that the blood islands become restricted to the ventralmost mesoderm because they are not exposed to the BMP-inhibiting activity of the Spemann organizer. We present evidence here that, contrary to predictions of this model, the blood islands remain ventrally restricted even in the absence of Spemann organizer signaling. We further observed that inhibition of FGF signaling with a dominant negative receptor resulted in the expansion of the blood island-forming territory with a concomitant loss of somite. The requirement for FGF signaling in specifying somite versus blood island territories was observed as early as midgastrulation. The nonoverlapping expression domains of Xnr-2 and Xbra in the gastrula marginal zone appear to mark presumptive blood island and somite, respectively. Inhibition of FGF signaling with dominant negative receptor leads to an expansion of Xnr-2 expression and to a corresponding reduction in Xbra expression. On the other hand, we found no evidence that manipulation of BMP signaling, either positively or negatively, altered the expression domains of Xnr-2 and Xbra. These results suggest that FGF signaling, rather than BMP-inhibiting activity, is essential for restriction of the ventral blood islands to ventral mesoderm.

摘要

根据非洲爪蟾中胚层模式形成的三信号模型,除了施佩曼组织者外,所有中胚层最初都被指定为腹侧类型,如侧板和原始血岛。有人提出,血岛局限于最腹侧的中胚层,因为它们没有接触到施佩曼组织者的骨形态发生蛋白(BMP)抑制活性。我们在此提供证据表明,与该模型的预测相反,即使在没有施佩曼组织者信号传导的情况下,血岛仍局限于腹侧。我们进一步观察到,用显性负性受体抑制成纤维细胞生长因子(FGF)信号传导会导致血岛形成区域的扩大,同时体节减少。早在原肠胚中期就观察到FGF信号传导在确定体节与血岛区域中的必要性。原肠胚边缘区中Xnr-2和Xbra的非重叠表达域似乎分别标记了推定的血岛和体节。用显性负性受体抑制FGF信号传导会导致Xnr-2表达的扩大和Xbra表达的相应减少。另一方面,我们没有发现证据表明对BMP信号传导进行正向或负向操作会改变Xnr-2和Xbra的表达域。这些结果表明,FGF信号传导而非BMP抑制活性对于将腹侧血岛限制在腹侧中胚层至关重要。

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