小岛
胰岛素
胰岛素抵抗
内科学
内分泌学
炎症
免疫系统
分泌物
2型糖尿病
糖尿病
生物
2型糖尿病
树突状细胞
医学
免疫学
作者
Claire E. Macdougall,Elizabeth G. Wood,Antonia Solomou,Valeria Scagliotti,Makoto M. Taketo,Carles Gaston‐Massuet,Federica M. Marelli‐Berg,Marika Charalambous,M. Paula Longhi
出处
期刊:Diabetes
[American Diabetes Association]
日期:2019-05-02
卷期号:68 (7): 1473-1484
被引量:14
摘要
β-Cell failure is central to the development of type 2 diabetes mellitus (T2DM). Dysregulation of metabolic and inflammatory processes during obesity contributes to the loss of islet function and impaired β-cell insulin secretion. Modulating the immune system, therefore, has the potential to ameliorate diseases. We report that inducing sustained expression of β-catenin in conventional dendritic cells (cDCs) provides a novel mechanism to enhance β-cell insulin secretion. Intriguingly, cDCs with constitutively activated β-catenin induced islet expansion by increasing β-cell proliferation in a model of diet-induced obesity. We further found that inflammation in these islets was reduced. Combined, these effects improved β-cell insulin secretion, suggesting a unique compensatory mechanism driven by cDCs to generate a greater insulin reserve in response to obesity-induced insulin resistance. Our findings highlight the potential of immune modulation to improve β-cell mass and function in T2DM.
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