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尿道和外生殖器发育过程中对基底膜层粘连蛋白α5的需求。

Requirement for basement membrane laminin α5 during urethral and external genital development.

作者信息

Lin Congxing, Werner Ralf, Ma Liang, Miner Jeffrey H

机构信息

Division of Dermatology, Washington University School of Medicine, St. Louis, MO 63110, USA.

Division of Experimental Paediatric Endocrinology and Diabetes, Department of Paediatric and Adolescent Medicine, University of Luebeck, Luebeck 23538, Germany.

出版信息

Mech Dev. 2016 Aug;141:62-69. doi: 10.1016/j.mod.2016.05.004. Epub 2016 May 18.

Abstract

Hypospadias, a congenital malformation of the penis characteristic of an abnormal urethral orifice, affects 1 in every 125 boys, and its incidence is rising. Herein we test the hypothesis that the basement membrane protein laminin α5 (LAMA5) plays a key role in the development of the mouse genital tubercle, the embryonic anlage of the external genitalia. Using standard histological analyses and electron microscopy, we characterized the morphology of the external genitalia in Lama5 knockout (LAMA5-KO) mouse embryos during both androgen-independent genital tubercle development and androgen-mediated sexual differentiation. We compared regulatory gene expression between control and LAMA5-KO by in situ hybridization. We also examined the epithelial structure of the mutant genital tubercle using immunofluorescence staining and histological analyses of semi-thin sections. We found that Lama5 was expressed in both ectodermal and endodermal epithelia of the cloaca. The LAMA5-KO displayed a profound external genital malformation in which the genital tubercle was underdeveloped with a large ectopic orifice at the proximal end. In older embryos, the urethra failed to form a tubular structure and was left completely exposed. These defects were not associated with a significant alteration in regulatory gene expression, but rather with a defective ectodermal epithelium and an abnormal disintegration of the cloacal membrane. We conclude that LAMA5 is required in the basement membrane to maintain normal architecture of the ventral ectoderm during genital tubercle development, which is essential for the formation of a tubular urethra. Perturbation of LAMA5, and possibly other basement membrane components, may cause hypospadias in humans.

摘要

尿道下裂是一种阴茎先天性畸形,其特征为尿道外口异常,每125名男孩中就有1人受其影响,且发病率呈上升趋势。在此,我们检验了以下假设:基底膜蛋白层粘连蛋白α5(LAMA5)在小鼠生殖结节(外生殖器的胚胎原基)的发育中起关键作用。我们使用标准组织学分析和电子显微镜,对Lama5基因敲除(LAMA5-KO)小鼠胚胎在雄激素非依赖的生殖结节发育阶段以及雄激素介导的性分化阶段的外生殖器形态进行了表征。我们通过原位杂交比较了对照组和LAMA5-KO组之间调控基因的表达。我们还使用免疫荧光染色和半薄切片的组织学分析,检查了突变体生殖结节的上皮结构。我们发现Lama5在泄殖腔的外胚层和内胚层上皮中均有表达。LAMA5-KO小鼠表现出严重的外生殖器畸形,生殖结节发育不全,近端有一个大的异位开口。在较大的胚胎中,尿道未能形成管状结构,而是完全暴露在外。这些缺陷与调控基因表达的显著改变无关,而是与外胚层上皮缺陷和泄殖腔膜异常解体有关。我们得出结论,在生殖结节发育过程中,基底膜需要LAMA5来维持腹侧外胚层的正常结构,这对于管状尿道的形成至关重要。LAMA5以及可能的其他基底膜成分的扰动,可能会导致人类尿道下裂。

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本文引用的文献

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