肺干细胞自我更新依赖于 BMI1 依赖性控制印迹基因座的表达。
Lung stem cell self-renewal relies on BMI1-dependent control of expression at imprinted loci.
机构信息
Stem Cell Program, Children's Hospital Boston, Boston, MA 02115 USA.
出版信息
Cell Stem Cell. 2011 Sep 2;9(3):272-81. doi: 10.1016/j.stem.2011.07.007.
Abstract
BMI1 is required for the self-renewal of stem cells in many tissues including the lung epithelial stem cells, Bronchioalveolar Stem Cells (BASCs). Imprinted genes, which exhibit expression from only the maternally or paternally inherited allele, are known to regulate developmental processes, but what their role is in adult cells remains a fundamental question. Many imprinted genes were derepressed in Bmi1 knockout mice, and knockdown of Cdkn1c (p57) and other imprinted genes partially rescued the self-renewal defect of Bmi1 mutant lung cells. Expression of p57 and other imprinted genes was required for lung cell self-renewal in culture and correlated with repair of lung epithelial cell injury in vivo. Our data suggest that BMI1-dependent regulation of expressed alleles at imprinted loci, distinct from imprinting per se, is required for control of lung stem cells. We anticipate that the regulation and function of imprinted genes is crucial for self-renewal in diverse adult tissue-specific stem cells.
摘要
BMI1 是许多组织中干细胞自我更新所必需的,包括肺上皮干细胞、支气管肺泡干细胞(BASCs)。印迹基因仅从母本或父本遗传等位基因表达,已知其调控发育过程,但它们在成体细胞中的作用仍是一个基本问题。在 Bmi1 敲除小鼠中,许多印迹基因被去抑制,Cdkn1c(p57)和其他印迹基因的敲低部分挽救了 Bmi1 突变肺细胞的自我更新缺陷。p57 和其他印迹基因的表达是肺细胞在培养中自我更新所必需的,并与体内肺上皮细胞损伤的修复相关。我们的数据表明,BMI1 依赖于印迹基因座上表达等位基因的调节,与印迹本身不同,这对于控制肺干细胞是必需的。我们预计,印迹基因的调节和功能对于不同的成体组织特异性干细胞的自我更新至关重要。
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