首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Critical and Distinct Roles of p16 and Telomerase in Regulating the Proliferative Life Span of Normal Human Prostate Epithelial Progenitor Cells
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Critical and Distinct Roles of p16 and Telomerase in Regulating the Proliferative Life Span of Normal Human Prostate Epithelial Progenitor Cells

机译:p16和端粒酶在调节细胞凋亡中的关键作用和独特作用 正常人前列腺上皮祖细胞的增殖寿命 细胞

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摘要

Normal human prostate (NHP) epithelial cells undergo senescence in vitro and in vivo, but the underlying molecular mechanisms remain obscure. Here we show that the senescence of primary NHP cells, which are immunophenotyped as intermediate basal-like cells expressing progenitor cell markers CD44, α2β1, p63, hTERT, and CK5/CK18, involves loss of telomerase expression, up-regulation of p16, and activation of p53. Using genetically defined manipulations of these three signaling pathways, we show that p16 is the primary determinant of the NHP cell proliferative capacity and that hTERT is required for unlimited proliferative life span. Hence, suppression of p16 significantly extends NHP cell life span, but both p16 inhibition and hTERT are required to immortalize NHP cells. Importantly, immortalized NHP cells retain expression of most progenitor markers, demonstrate gene expression profiles characteristic of proliferating progenitor cells, and possess multilineage differentiation potential generating functional prostatic glands. Our studies shed important light on the molecular mechanisms regulating the proliferative life span of NHP progenitor cells.
机译:正常人前列腺(NHP)上皮细胞在体外和体内都会衰老,但其潜在的分子机制仍然不清楚。在这里,我们表明原发性NHP细胞的衰老被免疫表型表达为表达祖细胞标记CD44,α2β1,p63,hTERT和CK5 / CK18的中间基底样细胞,涉及端粒酶表达的丧失,p16的上调和p53的激活。使用这三个信号通路的遗传定义的操作,我们表明p16是NHP细胞增殖能力的主要决定因素,而hTERT是无限增殖寿命所必需的。因此,p16的抑制显着延长了NHP细胞的寿命,但是p16抑制和hTERT都需要永生化NHP细胞。重要的是,永生化的NHP细胞保留了大多数祖细胞标记物的表达,展示了增殖祖细胞特征的基因表达谱,并具有产生多系分化潜能的功能性前列腺。我们的研究为调节NHP祖细胞增殖寿命的分子机制提供了重要启示。

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