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c-ret的表达促进了小鼠肾内髓集合管细胞(mIMCD-3细胞)的形态发生和细胞存活。

Expression of c-ret promotes morphogenesis and cell survival in mIMCD-3 cells.

作者信息

O'Rourke D A, Sakurai H, Spokes K, Kjelsberg C, Takahashi M, Nigam S, Cantley L

机构信息

Division of Nephrology, Beth Israel Deaconess Medical Center, Boston, Massachusetts 02215, USA.

出版信息

Am J Physiol. 1999 Apr;276(4):F581-8. doi: 10.1152/ajprenal.1999.276.4.F581.

Abstract

c-Ret, a protein tyrosine kinase receptor, and its ligand glial-derived neurotropic factor (GDNF) are critical for early regulation of ureteric bud development and nephrogenesis. To address whether c-ret directly initiates epithelial cell morphogenesis, the c-ret receptor was expressed in murine inner medullary collecting duct cells (mIMCD-3, a cell line of ureteric bud origin, which has no detectable endogenous c-ret expression). Stable expression of wild-type c-ret was found to yield a constitutively tyrosine-phosphorylated receptor, with no change after the addition of GDNF. Examination of mRNA from these cells demonstrated the message for endogenous GDNF, suggesting that c-ret was potentially being constitutively activated by an autocrine mechanism. When mIMCD-3 cells stably expressing the phosphorylated c-ret receptor were cultured in a type I collagen matrix, they exhibited little GDNF-independent or -dependent branching process formation at early time points compared with the known morphogen hepatocyte growth factor (HGF) (48 h; control, 0.33 +/- 0.33; GDNF, 1.0 +/- 0.58, P = nonsignificant; and HGF, 6.33 +/- 0.33 processes/20 cell clusters, P < 0.001), whereas extended culture (7 days) under serum-free conditions revealed a marked increase in cell survival and the spontaneous development of rudimentary branching process formation. Extended culture (7 days) of c-ret-expressing clones in type I collagen with the epithelial morphogens HGF and/or epidermal growth factor (EGF) resulted in the development of complex three-dimensional spiny cysts, whereas parental mIMCD-3 cells died under these conditions. We conclude that activated c-ret appears to mediate epithelial morphogenesis by prolonging cell survival and, in conjunction with activation of the morphogenic receptors c-met and the EGF receptor, initiates the events required for very early branching morphogenesis.

摘要

c-Ret是一种蛋白酪氨酸激酶受体,其配体胶质细胞源性神经营养因子(GDNF)对于输尿管芽发育和肾发生的早期调节至关重要。为了探究c-ret是否直接启动上皮细胞形态发生,c-ret受体在小鼠内髓集合管细胞(mIMCD-3,一种输尿管芽起源的细胞系,其未检测到内源性c-ret表达)中表达。发现野生型c-ret的稳定表达产生一种组成型酪氨酸磷酸化受体,添加GDNF后无变化。对这些细胞的mRNA检测显示了内源性GDNF的信息,表明c-ret可能通过自分泌机制被组成型激活。当在I型胶原基质中培养稳定表达磷酸化c-ret受体的mIMCD-3细胞时,与已知形态发生素肝细胞生长因子(HGF)相比,在早期时间点它们几乎没有形成不依赖或依赖GDNF的分支过程(48小时;对照组,0.33±0.33;GDNF,1.0±0.58,P无显著性差异;HGF,6.33±0.33个分支/20个细胞簇,P<0.001),而在无血清条件下延长培养(7天)显示细胞存活率显著增加,并且自发形成基本的分支过程。在I型胶原中用上皮形态发生素HGF和/或表皮生长因子(EGF)对表达c-ret的克隆进行延长培养(7天)导致形成复杂的三维棘状囊肿,而亲本mIMCD-3细胞在这些条件下死亡。我们得出结论,激活的c-ret似乎通过延长细胞存活来介导上皮形态发生,并与形态发生受体c-met和EGF受体的激活一起,启动非常早期分支形态发生所需的事件。

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