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The role of Sox9 in mouse mammary gland development and maintenance of mammary stem and luminal progenitor cells

机译:Sox9在小鼠乳腺发育和维持乳腺干细胞和腔内祖细胞中的作用

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Background Identification and characterization of molecular controls that regulate mammary stem and progenitor cell homeostasis are critical to our understanding of normal mammary gland development and its pathology. Results We demonstrate that conditional knockout of Sox9 in the mouse mammary gland results in impaired postnatal development. In short-term lineage tracing in the postnatal mouse mammary gland using Sox9-CreER driven reporters, Sox9 marked primarily the luminal progenitors and bipotent stem/progenitor cells within the basal mammary epithelial compartment. In contrast, long-term lineage tracing studies demonstrate that Sox9+ precursors gave rise to both luminal and myoepithelial cell lineages. Finally, fate mapping of Sox9 deleted cells demonstrates that Sox9 is essential for luminal, but not myoepithelial, lineage commitment and proliferation. Conclusions These studies identify Sox9 as a key regulator of mammary gland development and stem/progenitor maintenance.
机译:背景调控乳腺干细胞和祖细胞稳态的分子控制的鉴定和表征对于我们对正常乳腺发育及其病理的理解至关重要。结果我们证明在小鼠乳腺中条件性敲除Sox9会导致出生后发育受损。在使用Sox9-CreER驱动的报道分子对产后小鼠乳腺进行短期谱系追踪中,Sox9主要标记了基底乳腺上皮区室中的腔内祖细胞和双能干/祖细胞。相反,长期的谱系追踪研究表明,Sox9 +前体同时产生了腔和肌上皮细胞谱系。最后,Sox9缺失细胞的命运定位表明,Sox9对腔是必不可少的,但对肌上皮,谱系定型和增殖不是必需的。结论这些研究确定Sox9是乳腺发育和干/祖细胞维持的关键调节剂。

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