Failure to repair endogenous DNA damage in β-cells causes adult-onset diabetes in mice

Age is the greatest risk factor for the development of type 2 diabetes mellitus (T2DM). Age-related decline in organ function is attributed to the accumulation of stochastic damage, including damage to the nuclear genome. Islets of T2DM patients display increased levels of DNA damage. However, wheth...

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Published inAging Biology Vol. 1; no. 1
Main Authors Yousefzadeh, Matthew J, Huerta Guevara, Ana P, Postmus, Andrea C, Flores, Rafael R, Sano, Tokio, Jurdzinski, Angelika, Angelini, Luise, McGowan, Sara J, O'Kelly, Ryan D, Wade, Erin A, Gonzalez-Espada, Lisa V, Henessy-Wack, Danielle, Howard, Shannon, Rozgaja, Tania A, Trussoni, Christy E, LaRusso, Nicholas F, Eggen, Bart J L, Jonker, Johan W, Robbins, Paul D, Niedernhofer, Laura J, Kruit, Janine K
Format Journal Article
LanguageEnglish
Published United States 2023
Subjects
Type 2 diabetes
DNA damage repair
β-cell dysfunction
Pancreatic beta-cells
aging
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Summary:Age is the greatest risk factor for the development of type 2 diabetes mellitus (T2DM). Age-related decline in organ function is attributed to the accumulation of stochastic damage, including damage to the nuclear genome. Islets of T2DM patients display increased levels of DNA damage. However, whether this is a cause or consequence of the disease has not been elucidated. Here, we asked if spontaneous, endogenous DNA damage in β-cells can drive β-cell dysfunction and diabetes, via deletion of , a key DNA repair gene, in β-cells. Mice harboring -deficient β-cells developed adult-onset diabetes as demonstrated by increased random and fasted blood glucose levels, impaired glucose tolerance, and reduced insulin secretion. The inability to repair endogenous DNA damage led to an increase in oxidative DNA damage and apoptosis in β-cells and a significant loss of β-cell mass. Using electron microscopy, we identified β-cells in clear distress that showed an increased cell size, enlarged nuclear size, reduced number of mature insulin granules, and decreased number of mitochondria. Some β-cells were more affected than others consistent with the stochastic nature of spontaneous DNA damage. -deficiency in β-cells also resulted in loss of β-cell function as glucose-stimulated insulin secretion and mitochondrial function were impaired in islets isolated from mice harboring -deficient β-cells. These data reveal that unrepaired endogenous DNA damage is sufficient to drive β-cell dysfunction and provide a mechanism by which age increases the risk of T2DM.