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Hoxa13突变小鼠中Bmp7和Fgf8信号缺失导致尿道下裂。

Loss of Bmp7 and Fgf8 signaling in Hoxa13-mutant mice causes hypospadia.

作者信息

Morgan Emily A, Nguyen Susan B, Scott Virginia, Stadler H Scott

机构信息

Shriners Hospital for Children, Portland, OR 97239, USA.

出版信息

Development. 2003 Jul;130(14):3095-109. doi: 10.1242/dev.00530.

Abstract

In humans and mice, mutations in Hoxa13 cause malformation of limb and genitourinary (GU) regions. In males, one of the most common GU malformations associated with loss of Hoxa13 function is hypospadia, a condition defined by the poor growth and closure of the urethra and glans penis. By examining early signaling in the developing mouse genital tubercle, we show that Hoxa13 is essential for normal expression of Fgf8 and Bmp7 in the urethral plate epithelium. In Hoxa13(GFP)-mutant mice, hypospadias occur as a result of the combined loss of Fgf8 and Bmp7 expression in the urethral plate epithelium, as well as the ectopic expression of noggin (Nog) in the flanking mesenchyme. In vitro supplementation with Fgf8 restored proliferation in homozygous mutants to wild-type levels, suggesting that Fgf8 is sufficient to direct early proliferation of the developing genital tubercle. However, the closure defects of the distal urethra and glans can be attributed to a loss of apoptosis in the urethra, which is consistent with reduced Bmp7 expression in this region. Mice mutant for Hoxa13 also exhibit changes in androgen receptor expression, providing a developmental link between Hoxa13-associated hypospadias and those produced by antagonists to androgen signaling. Finally, a novel role for Hoxa13 in the vascularization of the glans penis is also identified.

摘要

在人类和小鼠中,Hoxa13基因的突变会导致肢体和泌尿生殖(GU)区域的畸形。在男性中,与Hoxa13功能丧失相关的最常见的GU畸形之一是尿道下裂,这是一种由尿道和阴茎头生长不良及闭合不全所定义的病症。通过研究发育中的小鼠生殖结节中的早期信号传导,我们发现Hoxa13对于尿道板上皮中Fgf8和Bmp7的正常表达至关重要。在Hoxa13(GFP)突变小鼠中,尿道下裂的发生是由于尿道板上皮中Fgf8和Bmp7表达的联合缺失,以及旁侧间充质中头蛋白(Nog)的异位表达。体外补充Fgf8可将纯合突变体中的增殖恢复到野生型水平,这表明Fgf8足以指导发育中的生殖结节的早期增殖。然而,远端尿道和阴茎头的闭合缺陷可归因于尿道中细胞凋亡的缺失,这与该区域Bmp7表达的降低一致。Hoxa13突变的小鼠在雄激素受体表达上也表现出变化,这为Hoxa13相关的尿道下裂与雄激素信号拮抗剂所产生的尿道下裂之间提供了发育上的联系。最后,还确定了Hoxa13在阴茎头血管形成中的新作用。

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