首页> 外文期刊>Journal of receptor and signal transduction research >Study of the interaction among Notch pathway receptors, correlation with stemness, as well as their interaction with CD44, dipeptidyl peptidase-IV, hepatocyte growth factor receptor and the SETMAR transferase, in colon cancer stem cells
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Study of the interaction among Notch pathway receptors, correlation with stemness, as well as their interaction with CD44, dipeptidyl peptidase-IV, hepatocyte growth factor receptor and the SETMAR transferase, in colon cancer stem cells

机译:研究结肠癌干细胞中Notch通路受体之间的相互作用,与干性的关系以及它们与CD44,二肽基肽酶-IV,肝细胞生长因子受体和SETMAR转移酶的相互作用

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Context: The Notch signaling pathway is one of the most important pathways during normal development and implicated in self-renewal of adult stem cells and differentiation of progenitor cells. Abnormal expression of Notch receptors has been associated with many epithelial metaplastic and neoplastic lesions. Objective-materials and methods: In this particular study, it was determined the relative gene expression of Notch receptors after knockdown experiments in colon cancer stem cells (CSCs) and the gene expression changes in stemness transcription factors (Oct4, Sox2, Nanog), as well in dipeptidylpeptidase-4, CD44 antigen, Met proto-oncogene and in Metnase transposase. Results: In control CSCs Notch-2 had the higher expression, followed by Notch-1, Notch-3. Notch-4 demonstrated the lower gene expression among the receptors. The suppression of Notch-1 led to increased expression of Oct4 and Sox2, but in decreased gene expression of cMET, Setmar and CD44. The CD26 expression remained unchanged. The knockdown of Notch-2 led to decreased expression of all transcription factors. Notch-3 down regulation caused increased Oct4 gene expression, but decreased levels for the rest of the genes. Finally, the suppression of Notch-4 had the same effect as in receptor Notch-3. Discussion and conclusion: The above experimental data suggest the possible interaction between the four different receptors of Notch signaling pathway. The expression of CD26, cMET and N-methyltransferase Setmar was also changed. Finally, the stemness phenotype was changed in a different way each time, according to the receptor that was down regulated. All Notch receptors and particularly Notch-2 seem to play an important role in cancer stem cells.
机译:背景:Notch信号通路是正常发育过程中最重要的通路之一,与成人干细胞的自我更新和祖细胞的分化有关。 Notch受体的异常表达与许多上皮化生和赘生性病变有关。目标材料和方法:在这项特殊研究中,确定了敲除实验后在结肠癌干细胞(CSC)中Notch受体的相对基因表达以及干转录因子(Oct4,Sox2,Nanog)的基因表达变化,如下:在二肽基肽酶-4,CD44抗原,Met原癌基因和Metnase转座酶中都很好。结果:在对照CSC中,Notch-2具有较高的表达,其次是Notch-1,Notch-3。 Notch-4证明受体之间的基因表达较低。 Notch-1的抑制导致Oct4和Sox2的表达增加,但导致cMET,Setmar和CD44的基因表达减少。 CD26表达保持不变。 Notch-2的敲低导致所有转录因子的表达降低。 Notch-3下调导致Oct4基因表达增加,但其余基因水平降低。最后,Notch-4的抑制作用与受体Notch-3相同。讨论与结论:以上实验数据表明,Notch信号通路的四个不同受体之间可能存在相互作用。 CD26,cMET和N-甲基转移酶Setmar的表达也发生了变化。最后,根据被下调的受体,茎表型每次都以不同的方式改变。所有的Notch受体,尤其是Notch-2似乎在癌症干细胞中起重要作用。

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