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Src family kinases play multiple roles in differentiation of trophoblasts from human term placenta

机译:Src家族激酶在人类足月胎盘滋养细胞分化中发挥多种作用

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摘要

Tyrosine phosphorylation plays a major role in controlling many biological processes in different cell types. Src family kinases (SFKs) are one of the most studied groups of tyrosine kinases and can mediate a variety of signalling pathways. However, little is known about the expression of SFKs in human term placenta and their implication in trophoblast differentiation. Therefore, we examined the expression profile of SFK members over time in culture and their implication in differentiation. In vitro, freshly isolated cytotrophoblast cells, cultured in 10% fetal bovine serum (FBS), spontaneously aggregate and fuse to form multinucleated cells that resemble phenotypically mature syncytiotrophoblasts, that concomitantly produce human chorionic gonadotropin (hCG) and human placental lactogen (hPL). In this study, we showed that trophoblasts expressed all SFK members and some of them are expressed as different splice variants. Moreover, using real-time PCR, this study showed two different expression profiles of SFKs in human trophoblasts during culture. In addition, the protein level and phosphorylation status of Src were evaluated using specific antibodies. Src was rapidly phosphorylated at Tyr-416 and dephosphorylated at Tyr-527 after FBS addition. Surprisingly, inhibition of SFKs by 4-amino-5-(4-chlorophenyl)-7-(t-butyl) pyrazolo[3,4-d] pyrimidine (PP2) or herbimycin A had different effects on trophoblast differentiation. While herbimycin A inhibited morphological and hormonal differentiation, PP2 stimulated hormonal differentiation and inhibited cell adhesion and spreading with no effect on cell fusion. In summary, this study showed that SFKs play different roles in trophoblast differentiation, probably depending on SFK members activated. Thus, this study increases our knowledge and understanding of pathology related to impaired trophoblast differentiation such as pre-eclampsia and trophoblast neoplasm.
机译:酪氨酸磷酸化在控制不同细胞类型中的许多生物过程中起主要作用。 Src家族激酶(SFK)是酪氨酸激酶研究最多的组之一,可以介导多种信号通路。但是,关于人类足月胎盘中SFKs的表达及其在滋养细胞分化中的作用了解甚少。因此,我们检查了SFK成员在文化中随时间的表达情况及其在分化中的意义。在10%胎牛血清(FBS)中培养的体外新鲜分离的细胞滋养层细胞自发聚集并融合,形成类似于表型成熟的合体滋养层细胞的多核细胞,这些细胞同时产生人绒毛膜促性腺激素(hCG)和人胎盘促乳素原(hPL)。在这项研究中,我们表明滋养细胞表达了所有SFK成员,其中一些表达为不同的剪接变体。而且,使用实时PCR,这项研究显示了培养过程中人类滋养细胞中SFK的两种不同表达模式。另外,使用特异性抗体评估了Src的蛋白水平和磷酸化状态。加入FBS后,Src在Tyr-416处迅速磷酸化,并在Tyr-527处去磷酸化。令人惊讶的是,4-氨基-5-(4-氯苯基)-7-(叔丁基)吡唑并[3,4-d]嘧啶(PP2)或除草霉素A对SFKs的抑制作用对滋养层细胞的分化有不同的影响。除草霉素A抑制形态和激素分化,而PP2刺激激素分化并抑制细胞粘附和扩散,而对细胞融合没有影响。总而言之,这项研究表明,SFK在滋养细胞分化中发挥不同的作用,这可能取决于激活的SFK成员。因此,这项研究增加了我们对与滋养细胞分化受损(例如先兆子痫和滋养细胞肿瘤)有关的病理学的认识和了解。

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