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首页> 外文期刊>The journal of clinical investigation >Insulin demand regulates β cell number via the unfolded protein response
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Insulin demand regulates β cell number via the unfolded protein response

机译:胰岛素需求通过未折叠的蛋白质反应调节β细胞数量

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Although stem cell populations mediate regeneration of rapid turnover tissues, such as skin, blood, and gut, a stem cell reservoir has not been identified for some slower turnover tissues, such as the pancreatic islet. Despite lacking identifiable stem cells, murine pancreatic β cell number expands in response to an increase in insulin demand. Lineage tracing shows that new β cells are generated from proliferation of mature, differentiated β cells; however, the mechanism by which these mature cells sense systemic insulin demand and initiate a proliferative response remains unknown. Here, we identified the β cell unfolded protein response (UPR), which senses insulin production, as a regulator of β cell proliferation. Using genetic and physiologic models, we determined that among the population of β cells, those with an active UPR are more likely to proliferate. Moreover, subthreshold endoplasmic reticulum stress (ER stress) drove insulin demand–induced β cell proliferation, through activation of ATF6. We also confirmed that the UPR regulates proliferation of human β cells, suggesting that therapeutic UPR modulation has potential to expand β cell mass in people at risk for diabetes. Together, this work defines a stem cell–independent model of tissue homeostasis, in which differentiated secretory cells use the UPR sensor to adapt organ size to meet demand.
机译:尽管干细胞群体介导了快速周转组织(如皮肤,血液和肠道)的再生,但尚未为某些较慢周转组织(如胰岛)鉴定出干细胞储库。尽管缺乏可识别的干细胞,但鼠类胰岛β细胞数量却随着胰岛素需求的增加而增加。谱系追踪表明,新的β细胞是由成熟的分化的β细胞的增殖产生的。然而,这些成熟细胞感知全身性胰岛素需求并引发增殖反应的机制仍然未知。在这里,我们确定了感测胰岛素产生的β细胞未折叠蛋白应答(UPR)作为β细胞增殖的调节剂。使用遗传和生理模型,我们确定了在β细胞群体中,具有活跃UPR的细胞更可能增殖。此外,亚阈值内质网应激(ER应激)通过激活ATF6驱动了胰岛素需求诱导的β细胞增殖。我们还证实,UPR调节人β细胞的增殖,这表明治疗性UPR调节具有扩大有糖尿病风险的人的β细胞量的潜力。在一起,这项工作定义了一个与干细胞无关的组织动态平衡模型,在该模型中,分化的分泌细胞使用UPR传感器来适应器官大小以满足需求。

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