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成纤维细胞生长因子受体2酪氨酸激酶对于前列腺形态发生以及成年组织稳态中严格雄激素依赖性的获得是必需的。

Fibroblast growth factor receptor 2 tyrosine kinase is required for prostatic morphogenesis and the acquisition of strict androgen dependency for adult tissue homeostasis.

作者信息

Lin Yongshun, Liu Guoqin, Zhang Yongyou, Hu Ya-Ping, Yu Kai, Lin Chunhong, McKeehan Kerstin, Xuan Jim W, Ornitz David M, Shen Michael M, Greenberg Norman, McKeehan Wallace L, Wang Fen

机构信息

Center for Cancer Biology and Nutrition, Institute of Biosciences and Technology, Texas A and M Health Science Center, 2121 W. Holcombe Blvd, Houston, TX 77030-3303, USA.

出版信息

Development. 2007 Feb;134(4):723-34. doi: 10.1242/dev.02765. Epub 2007 Jan 10.

Abstract

The fibroblast growth factor (FGF) family consists of 22 members and regulates a broad spectrum of biological activities by activating diverse isotypes of FGF receptor tyrosine kinases (FGFRs). Among the FGFs, FGF7 and FGF10 have been implicated in the regulation of prostate development and prostate tissue homeostasis by signaling through the FGFR2 isoform. Using conditional gene ablation with the Cre-LoxP system in mice, we demonstrate a tissue-specific requirement for FGFR2 in urogenital epithelial cells--the precursors of prostatic epithelial cells--for prostatic branching morphogenesis and prostatic growth. Most Fgfr2 conditional null (Fgfr2(cn)) embryos developed only two dorsal prostatic (dp) and two lateral prostatic (lp) lobes. This contrasts to wild-type prostate, which has two anterior prostatic (ap), two dp, two lp and two ventral prostatic (vp) lobes. Unlike wild-type prostates, which are composed of well developed epithelial ductal networks, the Fgfr2(cn) prostates, despite retaining a compartmented tissue structure, exhibited a primitive epithelial architecture. Moreover, although Fgfr2(cn) prostates continued to produce secretory proteins in an androgen-dependent manner, they responded poorly to androgen with respect to tissue homeostasis. The results demonstrate that FGFR2 is important for prostate organogenesis and for the prostate to develop into a strictly androgen-dependent organ with respect to tissue homeostasis but not to the secretory function, implying that androgens may regulate tissue homeostasis and tissue function differently. Therefore, Fgfr2(cn) prostates provide a useful animal model for scrutinizing molecular mechanisms by which androgens regulate prostate growth, homeostasis and function, and may yield clues as to how advanced-tumor prostate cells escape strict androgen regulations.

摘要

成纤维细胞生长因子(FGF)家族由22个成员组成,通过激活FGF受体酪氨酸激酶(FGFR)的不同亚型来调节广泛的生物活性。在FGF中,FGF7和FGF10通过FGFR2亚型信号传导参与前列腺发育和前列腺组织稳态的调节。利用小鼠中的Cre-LoxP系统进行条件性基因敲除,我们证明了泌尿生殖上皮细胞(前列腺上皮细胞的前体)中FGFR2对于前列腺分支形态发生和前列腺生长具有组织特异性需求。大多数Fgfr2条件性敲除(Fgfr2(cn))胚胎仅发育出两个背侧前列腺(dp)叶和两个外侧前列腺(lp)叶。这与野生型前列腺形成对比,野生型前列腺有两个前侧前列腺(ap)叶、两个dp叶、两个lp叶和两个腹侧前列腺(vp)叶。与由发育良好的上皮导管网络组成的野生型前列腺不同,Fgfr2(cn)前列腺尽管保留了分区组织结构,但呈现出原始的上皮结构。此外,尽管Fgfr2(cn)前列腺继续以雄激素依赖的方式产生分泌蛋白,但它们在组织稳态方面对雄激素的反应较差。结果表明,FGFR2对于前列腺器官发生以及前列腺在组织稳态方面发育成为严格雄激素依赖的器官很重要,但对于分泌功能并非如此,这意味着雄激素可能以不同方式调节组织稳态和组织功能。因此,Fgfr2(cn)前列腺为研究雄激素调节前列腺生长、稳态和功能的分子机制提供了一个有用的动物模型,并且可能为晚期肿瘤前列腺细胞如何逃避严格的雄激素调节提供线索。

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