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首页> 外文期刊>Cell death & disease. >Neurogenin 3+ cells contribute to β-cell neogenesis and proliferation in injured adult mouse pancreas
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Neurogenin 3+ cells contribute to β-cell neogenesis and proliferation in injured adult mouse pancreas

机译:Neurogenin 3 + 细胞促进成年小鼠胰腺胰腺β细胞的新生和增殖

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摘要

We previously showed that injury by partial duct ligation (PDL) in adult mouse pancreas activates Neurogenin 3 (Ngn3)+ progenitor cells that can differentiate to β cells ex vivo . Here we evaluate the role of Ngn3+ cells in β cell expansion in situ . PDL not only induced doubling of the β cell volume but also increased the total number of islets. β cells proliferated without extended delay (the so-called ‘refractory’ period), their proliferation potential was highest in small islets, and 86% of the β cell expansion was attributable to proliferation of pre-existing β cells. At sufficiently high Ngn3 expression level, upto 14% of all β cells and 40% of small islet β cells derived from non- β cells. Moreover, β cell proliferation was blunted by a selective ablation of Ngn3+ cells but not by conditional knockout of Ngn3 in pre-existing β cells supporting a key role for Ngn3+ insulin? cells in β cell proliferation and expansion. We conclude that Ngn3+ cell-dependent proliferation of pre-existing and newly-formed β cells as well as reprogramming of non- β cells contribute to in vivo β cell expansion in the injured pancreas of adult mice.
机译:我们先前发现成年小鼠胰腺受到部分导管结扎(PDL)的损伤会激活Neurogenin 3(Ngn3) + 祖细胞,该细胞可以离体分化为β细胞。在这里,我们评估了Ngn3 + 细胞在β细胞原位扩增中的作用。 PDL不仅诱导β细胞体积增加一倍,而且增加了胰岛的总数。 β细胞的增殖没有延长的延迟(所谓的“不应期”),其增殖潜力在小胰岛最高,β细胞的86%的增殖归因于先前存在的β细胞的增殖。在足够高的Ngn3表达水平下,多达14%的所有β细胞和40%的小胰岛β细胞衍生自非β细胞。此外,β细胞的增殖受Ngn3 + 细胞的选择性消融的影响而减弱,但不因Ngn3的条件性敲除而减弱,而已有的β细胞支持Ngn3 + 胰岛素的关键作用?细胞中β细胞的增殖和扩增。我们得出结论,既存的和新形成的β细胞的Ngn3 + 细胞依赖性增殖以及非β细胞的重新编程都有助于成年小鼠胰腺损伤中体内β细胞的扩增。

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