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体内胰岛素分泌β细胞的再生。

In vivo regeneration of insulin-producing beta-cells.

机构信息

Lee Gil Ya Cancer and Diabetes Institute, Gachon University of Medicine and Science, Yeonsu-ku, Incheon 406-840, Korea.

出版信息

Adv Exp Med Biol. 2010;654:627-40. doi: 10.1007/978-90-481-3271-3_27.

Abstract

Type 1 and type 2 diabetes mellitus are considered to be caused by defective control of blood glucose resulting from a reduced beta-cell mass. Thus, the restoration of a functional beta-cell mass by replacing the damaged beta-cells or stimulating beta-cell regeneration is a logical approach for the treatment of diabetes. Strategies for increasing the beta-cell mass include stimulating beta-cell replication and differentiation and inhibiting beta-cell death. Treatment with various growth factors such as GLP-1, BTC, HGF, and EGF and forced expression of beta-cell transcription factors such as Pdx-1, NeuroD, and MafA resulted in the regeneration of beta-cells in vivo. Another approach is the administration of stem/progenitor cells, which can differentiate into insulin-producing cells. However, there are no satisfactory methods yet for clinical application. Understanding the mechanisms of the regenerative process of pancreatic beta-cells will pave the way for the development of regenerative medicine for treatment of diabetes.

摘要

1 型和 2 型糖尿病被认为是由于血糖控制缺陷引起的,这是由于β细胞数量减少所致。因此,通过替换受损的β细胞或刺激β细胞再生来恢复功能性β细胞数量是治疗糖尿病的合理方法。增加β细胞数量的策略包括刺激β细胞复制和分化以及抑制β细胞死亡。用各种生长因子(如 GLP-1、BTC、HGF 和 EGF)治疗和强制表达β细胞转录因子(如 Pdx-1、NeuroD 和 MafA)可导致体内β细胞再生。另一种方法是施用干细胞/祖细胞,其可分化为产生胰岛素的细胞。然而,目前尚无令人满意的方法可用于临床应用。了解胰腺β细胞再生过程的机制将为治疗糖尿病的再生医学的发展铺平道路。

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