综述:2型糖尿病胰岛巨噬细胞生物学的新观点
Minireview: Emerging Concepts in Islet Macrophage Biology in Type 2 Diabetes.
作者信息
Morris David L
机构信息
Department of Medicine, Indiana University School of Medicine, Indianapolis, Indiana 46202.
出版信息
Mol Endocrinol. 2015 Jul;29(7):946-62. doi: 10.1210/me.2014-1393. Epub 2015 May 22.
Abstract
Chronic systemic inflammation is a hallmark feature of obesity and type 2 diabetes. Both resident and recruited islet macrophages contribute to the proinflammatory milieu of the diabetic islet. However, macrophages also appear to be critical for β-cell formation during development and support β-cell replication in experimental models of pancreas regeneration. In light of these findings, perhaps macrophages in the islet need to be viewed more as a fulcrum where deleterious inflammatory activation is balanced with beneficial tissue repair processes. Undoubtedly, defining the factors that contribute to the ontogeny, heterogeneity, and functionality of macrophages in normal, diseased, and regenerating islets will be necessary to determine whether that fulcrum can be moved to preserve functional β-cell mass in persons with diabetes. The intent of this review is to introduce the reader to emerging concepts of islet macrophage biology that may challenge the perception that macrophage accumulation in islets is merely a pathological feature of type 2 diabetes.
摘要
慢性全身性炎症是肥胖和2型糖尿病的标志性特征。胰岛中的驻留巨噬细胞和募集来的巨噬细胞都促成了糖尿病胰岛的促炎环境。然而,巨噬细胞在发育过程中对β细胞形成似乎也至关重要,并且在胰腺再生的实验模型中支持β细胞复制。鉴于这些发现,或许胰岛中的巨噬细胞需要更多地被视为一个支点,在这个支点上有害的炎症激活与有益的组织修复过程达到平衡。毫无疑问,要确定是否能够移动这个支点以保留糖尿病患者的功能性β细胞量,就有必要明确促成正常、患病和再生胰岛中巨噬细胞的个体发生、异质性和功能的因素。本综述的目的是向读者介绍胰岛巨噬细胞生物学的新兴概念,这些概念可能会挑战胰岛中巨噬细胞聚集仅仅是2型糖尿病病理特征这一认知。
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