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HIF-2α regulates Oct-4: effects of hypoxiaon stem cell function, embryonic development, and tumor growth

机译:HIF-2α调节Oct-4:低氧对干细胞功能,胚胎发育和肿瘤生长的影响

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摘要

The division, differentiation, and function of stem cells and multipotent progenitors are influenced by complex signals in the microenvironment, including oxygen availability. Using a genetic “knock-in” strategy, we demonstrate that targeted replacement of the oxygen-regulated transcription factor HIF-1α with HIF-2α results in expanded expression of HIF-2α-specific target genes including Oct-4, a transcription factor essential for maintaining stem cell pluripotency. We show that HIF-2α, but not HIF-1α, binds to the Oct-4 promoter and induces Oct-4 expression and transcriptional activity, thereby contributing to impaired development in homozygous Hif-2α KI/KI embryos, defective hematopoietic stem cell differentiation in embryoid bodies, and large embryonic stem cell (ES)-derived tumors characterized by altered cellular differentiation. Furthermore, loss of HIF-2α severely reduces the number of embryonic primordial germ cells, which require Oct-4 expression for survival and/or maintenance. These results identify Oct-4 as a HIF-2α-specific target gene and indicate that HIF-2α can regulate stem cell function and/or differentiation through activation of Oct-4, which in turn contributes to HIF-2α’s tumor promoting activity.
机译:干细胞和多能祖细胞的分裂,分化和功能受微环境中复杂信号的影响,包括氧气的可用性。使用遗传“敲入”策略,我们证明了用HIF-2α定向取代氧调节的转录因子HIF-1α会导致HIF-2α特异性靶基因(包括必需的转录因子Oct-4)的表达范围扩大用于维持干细胞多能性。我们显示,HIF-2α,而不是HIF-1α,与Oct-4启动子结合并诱导Oct-4表达和转录活性,从而导致纯合Hif-2αKI / KI胚胎发育受损,造血干细胞分化不良。在类胚体中,以及大型胚胎干细胞(ES)衍生的肿瘤,其特征在于细胞分化改变。此外,HIF-2α的丧失严重减少了胚胎原始原始生殖细胞的数量,这些原始原始生殖细胞需要Oct-4表达才能存活和/或维持。这些结果确定了Oct-4是一种HIF-2α特异性靶基因,并表明HIF-2α可以通过激活Oct-4来调节干细胞的功能和/或分化,进而有助于HIF-2α的肿瘤促进活性。

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