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SCL在非洲爪蟾胚胎中指定造血中胚层。

SCL specifies hematopoietic mesoderm in Xenopus embryos.

作者信息

Mead P E, Kelley C M, Hahn P S, Piedad O, Zon L I

机构信息

Division of Hematology/Oncology, Howard Hughes Medical Institute, Children's Hospital and Dana-Farber Cancer Institute, Boston, MA, USA.

出版信息

Development. 1998 Jul;125(14):2611-20. doi: 10.1242/dev.125.14.2611.

Abstract

Targeted gene disruption experiments in the mouse have demonstrated an absolute requirement for several transcription factors for the development of hematopoietic progenitors during embryogenesis. Disruption of the basic helix-loop-helix gene SCL (stem cell leukemia) causes a block early in the hematopoietic program with defects in all hematopoietic lineages. To understand how SCL participates in the organogenesis of blood, we have isolated cDNAs encoding Xenopus SCL and characterized the function of SCL during embryogenesis. We demonstrate that SCL is expressed in ventral mesoderm early in embryogenesis. SCL expression is induced by BMP-4, and a dominant negative BMP-4 receptor inhibits SCL expression in the ventral region of the embryo. Expression of SCL in either bFGF-treated animal pole explants or dorsal marginal zone explants leads to the expression of globin protein. Furthermore, over-expression of SCL does not alter normal dorsal-ventral patterning in the embryo, indicating that SCL acts to specify mesoderm to a hematopoietic fate after inductive and patterning events have occurred. We propose that SCL is both necessary and sufficient to specify hematopoietic mesoderm, and that it has a similar role in specifying hematopoietic cell fate as MyoD has in specifying muscle cell fate.

摘要

在小鼠中进行的靶向基因破坏实验表明,胚胎发育过程中造血祖细胞的发育绝对需要几种转录因子。破坏基本的螺旋-环-螺旋基因SCL(干细胞白血病)会导致造血程序早期出现阻滞,所有造血谱系均有缺陷。为了了解SCL如何参与血液的器官发生,我们分离了编码非洲爪蟾SCL的cDNA,并对胚胎发育过程中SCL的功能进行了表征。我们证明SCL在胚胎发育早期的腹侧中胚层中表达。SCL的表达由BMP-4诱导,而显性负性BMP-4受体抑制胚胎腹侧区域的SCL表达。在经bFGF处理的动物极外植体或背侧边缘区外植体中表达SCL会导致珠蛋白的表达。此外,SCL的过表达不会改变胚胎正常的背腹模式,这表明在诱导和模式形成事件发生后,SCL的作用是将中胚层指定为造血命运。我们提出,SCL对于指定造血中胚层既是必要的也是充分的,并且它在指定造血细胞命运方面具有与MyoD在指定肌肉细胞命运方面类似的作用。

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