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Direct reprogramming of epidermal cells toward sweat gland-like cells by defined factors

机译:通过定义因子将表皮细胞的表皮细胞直接重新编程为汗腺样细胞

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Several studies have reported inducing adult cells into sweat gland-like cells; however, slow transition and low efficiency limit the potential for cell-based treatment. Here, we show that overexpression of the transcription factor FoxC1 was sufficient to reprogram epidermal cells to induced functional sweat gland-like cells (iSGCs). The iSGCs expressing secreting-related genes, had a global gene expression profile between fetal SGCs (P5) and adult SGCs (P28). Moreover, iSGCs transplanted into the burn mice model facilitated wound repair and sweat gland regeneration. We further demonstrated that the Foxc1 upregulated BMP5 transcription and BMP5 is responsible for the cell-type transition. Collectively, this study shows that lineage reprogramming of epidermal cells into iSGCs provides an excellent cell source and a promising regenerative strategy for anhidrosis and hypohidrosis.
机译:几项研究报告了将成人细胞诱导为汗腺样细胞;然而,缓慢过渡和低效率限制了基于细胞的治疗潜力。这里,我们表明转录因子FoxC1的过度表达足以重新编程表皮细胞以诱导功能性汗腺状细胞(ISGC)。表达分泌相关基因的ISGCs在胎儿SGCs(P5)和成年SGCs(P28)之间具有全局基因表达谱。此外,移植到燃烧小鼠模型的ISGC促进伤口修复和汗腺再生。我们进一步证明FoxC1上调的BMP5转录和BMP5负责细胞型转变。集体,本研究表明,谱系对ISGC的表皮细胞重新编程提供了优异的细胞来源和对血症和抗皱症的有望的再生策略。

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