耳塞通过减弱对自我更新因子的反应能力来限制祖细胞的潜能。
Earmuff restricts progenitor cell potential by attenuating the competence to respond to self-renewal factors.
机构信息
Program in Cellular and Molecular Biology, University of Michigan Medical School, Ann Arbor, MI 48109, USA.
出版信息
Development. 2014 Mar;141(5):1036-46. doi: 10.1242/dev.106534.
Despite expressing stem cell self-renewal factors, intermediate progenitor cells possess restricted developmental potential, which allows them to give rise exclusively to differentiated progeny rather than stem cell progeny. Failure to restrict the developmental potential can allow intermediate progenitor cells to revert into aberrant stem cells that might contribute to tumorigenesis. Insight into stable restriction of the developmental potential in intermediate progenitor cells could improve our understanding of the development and growth of tumors, but the mechanisms involved remain largely unknown. Intermediate neural progenitors (INPs), generated by type II neural stem cells (neuroblasts) in fly larval brains, provide an in vivo model for investigating the mechanisms that stably restrict the developmental potential of intermediate progenitor cells. Here, we report that the transcriptional repressor protein Earmuff (Erm) functions temporally after Brain tumor (Brat) and Numb to restrict the developmental potential of uncommitted (immature) INPs. Consistently, endogenous Erm is detected in immature INPs but undetectable in INPs. Erm-dependent restriction of the developmental potential in immature INPs leads to attenuated competence to respond to all known neuroblast self-renewal factors in INPs. We also identified that the BAP chromatin-remodeling complex probably functions cooperatively with Erm to restrict the developmental potential of immature INPs. Together, these data led us to conclude that the Erm-BAP-dependent mechanism stably restricts the developmental potential of immature INPs by attenuating their genomic responses to stem cell self-renewal factors. We propose that restriction of developmental potential by the Erm-BAP-dependent mechanism functionally distinguishes intermediate progenitor cells from stem cells, ensuring the generation of differentiated cells and preventing the formation of progenitor cell-derived tumor-initiating stem cells.
尽管中间祖细胞表达干细胞自我更新因子,但它们具有有限的发育潜力,这使得它们只能产生分化的后代,而不是干细胞后代。如果不能限制发育潜能,中间祖细胞就有可能恢复为异常干细胞,从而促进肿瘤发生。深入了解中间祖细胞发育潜能的稳定限制,可以增进我们对肿瘤发育和生长的理解,但其中涉及的机制在很大程度上仍然未知。果蝇幼虫大脑中的 II 型神经干细胞(神经母细胞)产生的中间神经前体细胞(INP)为研究稳定限制中间祖细胞发育潜能的机制提供了体内模型。在这里,我们报告转录抑制蛋白 Earmuff(Erm)在 Brain tumor(Brat)和 Numb 之后在时间上发挥作用,以限制未分化(未成熟)INP 的发育潜能。一致地,内源性 Erm 在未成熟 INP 中检测到,但在 INP 中未检测到。Erm 依赖性限制未成熟 INP 的发育潜能导致其对 INP 中所有已知神经母细胞自我更新因子的反应能力减弱。我们还发现 BAP 染色质重塑复合物可能与 Erm 协同作用,以限制未成熟 INP 的发育潜能。总之,这些数据使我们得出结论,即 Erm-BAP 依赖性机制通过减弱其对干细胞自我更新因子的基因组反应来稳定限制未成熟 INP 的发育潜能。我们提出,由 Erm-BAP 依赖性机制限制发育潜能在功能上区分了中间祖细胞和干细胞,确保了分化细胞的产生,并防止了祖细胞衍生的肿瘤起始干细胞的形成。
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