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首页> 外文期刊>Cancer science. >Efficient immortalization of primary human cells by p16INK4a-specific short hairpin RNA or Bmi-1, combined with introduction of hTERT.
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Efficient immortalization of primary human cells by p16INK4a-specific short hairpin RNA or Bmi-1, combined with introduction of hTERT.

机译:p16INK4a特异性短发夹RNA或Bmi-1与hTERT的引入共同有效地使人类原代细胞永生化。

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摘要

Activation of telomerase is sufficient for immortalization of some types of human cells but additional factors may also be essential. It has been proposed that stress imposed by inadequate culture conditions induces senescence due to accumulation of p16(INK4a). Here, we present evidence that many human cell types undergo senescence by activation of the p16(INK4a)/Rb pathway, and that introduction of Bmi-1 can inhibit p16(INK4a) expression and extend the life span of human epithelial cells derived from skin, mammary gland and lung. Introduction of p16(INK4a)-specific short hairpin RNA, as well as Bmi-1, suppressed p16(INK4a) expression in human mammary epithelial cells without promoter methylation, and extended their life span. Subsequent introduction of hTERT, the telomerase catalytic subunit, into cells with low p16(INK4a) levels resulted in efficient immortalization of three cell types without crisis or growth arrest. The majority of the human mammary epithelial cells thus immortalized showed almost normal ploidy as judged by G-banding and spectral karyotyping analysis. Our data suggest that inhibition of p16(INK4a) and introduction of hTERT can immortalize many human cell types with little chromosomal instability.
机译:端粒酶的激活足以使某些类型的人类细胞永生化,但其他因素也可能是必不可少的。已经提出,由于p16(INK4a)的积累,由不适当的培养条件引起的应激诱导衰老。在这里,我们提供的证据表明,许多人类细胞类型都通过激活p16(INK4a)/ Rb途径而经历衰老,而Bmi-1的引入可以抑制p16(INK4a)的表达并延长源自皮肤的人类上皮细胞的寿命,乳腺和肺。 p16(INK4a)特异性短发夹RNA以及Bmi-1的引入抑制了p16(INK4a)在人乳腺上皮细胞中的表达而没有启动子甲基化,并延长了它们的寿命。随后将端粒酶催化亚基hTERT引入低p16(INK4a)水平的细胞中,导致三种细胞类型的永生化永无危机或生长停滞。如通过G带和光谱核型分析所判断的,如此永生化的大多数人类乳腺上皮细胞显示出几乎正常的倍性。我们的数据表明,对p16(INK4a)的抑制和hTERT的引入可以使许多人类细胞永生化,而染色体的不稳定性很小。

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