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In vivo conversion of adult alpha-cells into beta-like cells: a new research avenue in the context of type 1 diabetes.

机译:成人α细胞在体内转化为β样细胞:在1型糖尿病背景下的新研究途径。

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摘要

Type 1 diabetes is caused by the loss of insulin-producing beta-cells as a result of an autoimmune condition. Despite current therapeutic approaches aimed at restoring the insulin supply, complications caused by variations in glycaemia may still arise with age. There is therefore mounting interest in the establishment of alternative therapies. Most current approaches consist in designing rational protocols for in vitro or in vivo cell differentiation/reprogramming from a number of cell sources, including stem, progenitor or differentiated cells. Towards this ultimate goal, it is clear that we need to gain further insight into the interplay between signalling events and transcriptional networks that act in concert throughout pancreatic morphogenesis. This short review will therefore focus on the main events underlying pancreatic development with particular emphasis on the genetic determinants implicated, as well as on the relatively new concept of endocrine cell reprogramming, that is the conversion of pancreatic alpha-cells into cells displaying a beta-cell phenotype.
机译:1型糖尿病是由自身免疫性疾病导致的胰岛素生产性β细胞损失引起的。尽管目前有旨在恢复胰岛素供应的治疗方法,但随着年龄的增长,仍可能出现由血糖变化引起的并发症。因此,人们对建立替代疗法越来越感兴趣。当前大多数方法包括设计合理的方案,以从许多细胞来源,包括干细胞,祖细胞或分化细胞中进行体外或体内细胞分化/重编程。为了实现这一最终目标,很显然,我们需要进一步了解信号事件与整个胰腺形态发生过程中共同起作用的转录网络之间的相互作用。因此,本篇短评将重点关注胰腺发育的主要事件,特别着重于涉及的遗传决定因素,以及相对较新的内分泌细胞重编程概念,即将胰腺α细胞转化为显示β-细胞的细胞。细胞表型。

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