1 型糖尿病中β细胞内源性双链 RNA 编辑受损的可能病因学作用。
Possible etiological role of impaired endogenous double strand RNA editing in β-cells in type 1 diabetes.
机构信息
Department of Diabetes, Metabolism and Endocrinology, Tohoku University Graduate School of Medicine, Sendai, Miyagi, Japan.
出版信息
J Diabetes Investig. 2024 Sep;15(9):1171-1173. doi: 10.1111/jdi.14224. Epub 2024 Apr 25.
Proposed mechanisms by which disruption of endogenous dsRNA editing in β-cells leads to type 1 diabetes-like phenotypes in βAdarKO mice. Disruption of endogenous dsRNA editing in β-cells initiates IFN responses, thereby inducing pancreatic islet inflammation and β-cell dysfunction. Hyperglycemia induced by β-cell dysfunction further promotes islet inflammation, likely via increased dsRNA resulting from increased β-cell workload, thereby producing a vicious cycle. The mechanism by which impairment of dsRNA editing is integrated with autoimmune-mediated pathogenesis of type 1 diabetes remains to be clarified.
内源性 dsRNA 编辑在 β 细胞中被破坏导致 βAdarKO 小鼠出现 1 型糖尿病样表型的可能机制。β 细胞中内源性 dsRNA 编辑的破坏会引发 IFN 反应,从而导致胰岛炎症和 β 细胞功能障碍。β 细胞功能障碍引起的高血糖进一步促进胰岛炎症,可能是通过增加 β 细胞工作量导致更多 dsRNA 产生,从而产生恶性循环。dsRNA 编辑受损与 1 型糖尿病自身免疫发病机制整合的机制仍有待阐明。
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