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生殖细胞中Notch-FGF信号轴的失调会导致小鼠睾丸网的囊性扩张。

Dysregulation of Notch-FGF signaling axis in germ cells results in cystic dilation of the rete testis in mice.

作者信息

Cao Yin, Liu Lingyun, Lin Jing, Sun Penghao, Guo Kaimin, Li Shengqiang, Li Xian, Lan Zi-Jian, Wang Hongliang, Lei Zhenmin

机构信息

Department of Andrology, the First Hospital of Jilin University, Changchun, Jilin, 130021, People's Republic of China.

Department of OB/GYN and Women's Health, MDR Building, University of Louisville School of Medicine, 511 South Floyd Street, Louisville, KY, 40292, USA.

出版信息

J Cell Commun Signal. 2022 Mar;16(1):75-92. doi: 10.1007/s12079-021-00628-0. Epub 2021 Jun 8.

Abstract

Numb (Nb) and Numb-like (Nbl) are functionally redundant adaptor proteins that critically regulate cell fate and morphogenesis in a variety of organs. We selectively deleted Nb and Nbl in testicular germ cells by breeding Nb/Nbl floxed mice with a transgenic mouse line Tex101-Cre. The mutant mice developed unilateral or bilateral cystic dilation in the rete testis (RT). Dye trace indicated partial blockages in the testicular hilum. Morphological and immunohistochemical evaluations revealed that the lining epithelium of the cysts possessed similar characteristics of RT epithelium, suggesting that the cyst originated from dilation of the RT lumen. Spermatogenesis and the efferent ducts were unaffected. In comparisons of isolated germ cells from mutants to control mice, the Notch activity considerably increased and the expression of Notch target gene Hey1 significantly elevated. Further studies identified that germ cell Fgf4 expression negatively correlated the Notch activity and demonstrated that blockade of FGF receptors mediated FGF4 signaling induced enlargement of the RT lumen in vitro. The crucial role of the FGF4 signaling in modulation of RT development was verified by the selective germ cell Fgf4 ablation, which displayed a phenotype similar to that of germ cell Nb/Nbl null mutant males. These findings indicate that aberrant over-activation of the Notch signaling in germ cells due to Nb/Nbl abrogation impairs the RT development, which is through the suppressing germ cell Fgf4 expression. The present study uncovers the presence of a lumicrine signal pathway in which secreted/diffusible protein FGF4 produced by germ cells is essential for normal RT development.

摘要

麻木蛋白(Nb)和类麻木蛋白(Nbl)是功能冗余的衔接蛋白,对多种器官中的细胞命运和形态发生起着关键调节作用。我们通过将Nb/Nbl基因敲除小鼠与转基因小鼠品系Tex101-Cre杂交,选择性地删除睾丸生殖细胞中的Nb和Nbl。突变小鼠的睾丸网(RT)出现单侧或双侧囊性扩张。染料追踪显示睾丸门存在部分阻塞。形态学和免疫组织化学评估表明,囊肿的内衬上皮具有与RT上皮相似的特征,提示囊肿起源于RT管腔的扩张。精子发生和输出小管未受影响。与对照小鼠分离的生殖细胞相比,突变体中的Notch活性显著增加,Notch靶基因Hey1的表达明显升高。进一步研究发现,生殖细胞Fgf4表达与Notch活性呈负相关,并证明阻断FGF受体介导的FGF4信号传导可在体外诱导RT管腔扩大。通过选择性生殖细胞Fgf4基因敲除验证了FGF4信号在调节RT发育中的关键作用,该敲除小鼠表现出与生殖细胞Nb/Nbl基因敲除突变雄性小鼠相似的表型。这些发现表明,由于Nb/Nbl缺失导致生殖细胞中Notch信号异常过度激活会损害RT发育,这是通过抑制生殖细胞Fgf4表达实现的。本研究揭示了一种腔分泌信号通路的存在,其中生殖细胞产生的分泌/可扩散蛋白FGF4对RT的正常发育至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3925/8688682/1e5f6daef457/12079_2021_628_Fig1_HTML.jpg

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