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人类肾发生过程中CFTR表达的发育调控

Developmental regulation of CFTR expression during human nephrogenesis.

作者信息

Devuyst O, Burrow C R, Schwiebert E M, Guggino W B, Wilson P D

机构信息

Department of Medicine, Johns Hopkins University, Medical School, Baltimore, Maryland 21205, USA.

出版信息

Am J Physiol. 1996 Sep;271(3 Pt 2):F723-35. doi: 10.1152/ajprenal.1996.271.3.F723.

Abstract

Cystic fibrosis transmembrane conductance regulator (CFTR) mRNA and protein are expressed in proximal and distal tubules of the human kidney, but CFTR expression pattern during human nephrogenesis is unknown. We have now studied CFTR expression in fetal kidneys by immunohistochemistry and Western blot analysis, using six antibodies against human CFTR. CFTR was expressed in 12-wk human fetal kidneys, mostly in the apical membrane region of the ureteric bud epithelial cells. By 15 wk, CFTR was also diffusely expressed throughout the cytoplasm of proximal tubules and loops of Henle. No glomerular staining was seen at any state. From 15 to 24 wk of gestation this staining pattern remained constant and also included immunoreactivity of the transitional epithelium. Western blot for CFTR was performed on membrane extracts of human fetal kidneys, using T84 cells as a positive control. A 165-kDa protein corresponding to the predicted size of CFTR was seen at 13 wk and throughout development. We also observed a 75-kDa protein that was distinctly regulated during development. This protein was detected with several antibodies against the first half of CFTR (including the regulatory "R" domain) but not with a COOH-terminal-specific antibody and had the predicted size of a functional splice variant of CFTR identified in the human kidney. These results show the complex regulation of CFTR during nephrogenesis and raise the question of the respective roles of the full-length and the splice variant CFTR proteins in the human kidney.

摘要

囊性纤维化跨膜传导调节因子(CFTR)的mRNA和蛋白在人肾的近端和远端小管中表达,但CFTR在人类肾发生过程中的表达模式尚不清楚。我们现在通过免疫组织化学和蛋白质印迹分析,使用六种抗人CFTR抗体,研究了胎儿肾脏中的CFTR表达。CFTR在12周龄的人胎儿肾脏中表达,主要位于输尿管芽上皮细胞的顶端膜区域。到15周时,CFTR也弥漫性地表达于近端小管和髓袢的整个细胞质中。在任何阶段均未观察到肾小球染色。在妊娠15至24周期间,这种染色模式保持不变,还包括移行上皮的免疫反应性。以T84细胞作为阳性对照,对人胎儿肾脏的膜提取物进行CFTR的蛋白质印迹分析。在13周及整个发育过程中均可见到一条与CFTR预测大小相对应的165 kDa蛋白。我们还观察到一种在发育过程中受到明显调节的75 kDa蛋白。该蛋白可被几种针对CFTR前半部分(包括调节性“R”结构域)的抗体检测到,但不能被COOH末端特异性抗体检测到,其大小与在人肾中鉴定出的CFTR功能性剪接变体的预测大小相符。这些结果显示了肾发生过程中CFTR的复杂调节,并提出了全长和剪接变体CFTR蛋白在人肾中各自作用的问题。

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