AUTHOR=Iwasaki Kanako , Lalani Benjamin , Kahng Jiho , Carapeto Priscila , Sanjines Stephanie , Hela Francesko , Abarca Cristian , Tsuji Tadataka , Darcy Justin , Bartke Andrzej , Tseng Yu-Hua , Kulkarni Rohit N. , Aguayo-Mazzucato Cristina 

TITLE=Decreased IGF1R attenuates senescence and improves function in pancreatic β-cells

JOURNAL=Frontiers in Endocrinology

VOLUME=14

YEAR=2023

URL=https://www.frontiersin.org/journals/endocrinology/articles/10.3389/fendo.2023.1203534

DOI=10.3389/fendo.2023.1203534

ISSN=1664-2392

ABSTRACT=<sec><title>Introduction</title><p>The enhanced β-cell senescence that accompanies insulin resistance and aging contributes to cellular dysfunction and loss of transcriptional identity leading to type 2 diabetes (T2D). While senescence is among the 12 recognized hallmarks of aging, its relation to other hallmarks including altered nutrient sensing (insulin/IGF1 pathway) in β-cells is not fully understood. We previously reported that an increased expression of IGF1R in mouse and human β-cells is a marker of older β-cells; however, its contribution to age-related dysfunction and cellular senescence remains to be determined.</p></sec><sec><title>Methods</title><p>In this study, we explored the direct role of IGF1R in β-cell function and senescence using two independent mouse models with decreased IGF1/IGF1R signaling: a) Ames Dwarf mice (Dwarf <sup>+/+</sup>), which lack growth hormone and therefore have reduced circulating levels of IGF1, and b) inducible β-cell-specific IGF1R knockdown (βIgf1rKD) mice.</p></sec><sec><title>Results</title><p>Compared to Dwarf<sup>+/-</sup> mice, Dwarf<sup>+/+</sup> mice had lower body and pancreas weight, lower circulating IGF1 and insulin levels, and lower IGF1R and p21Cip1 protein expression in β-cells, suggesting the suppression of senescence. Adult βIgf1rKD mice showed improved glucose clearance and glucose-induced insulin secretion, accompanied by decreased p21Cip1 protein expression in β-cells. RNA-Seq of islets isolated from these βIgf1rKD mice revealed the restoration of three signaling pathways known to be downregulated by aging: sulfide oxidation, autophagy, and mTOR signaling. Additionally, deletion of IGF1R in mouse β-cells increased transcription of genes important for maintaining β-cell identity and function, such as <italic>Mafa</italic>, <italic>Nkx6.1</italic>, and <italic>Kcnj11</italic>, while decreasing senescence-related genes, such as <italic>Cdkn2a</italic>, <italic>Il1b</italic>, and <italic>Serpine 1</italic>. Decreased senescence and improved insulin-secretory function of β-cells were also evident when the βIgf1rKD mice were fed a high-fat diet (HFD; 60% kcal from fat, for 5 weeks).</p></sec><sec><title>Discussion</title><p>These results suggest that IGF1R signaling plays a causal role in aging-induced β-cell dysfunction. Our data also demonstrate a relationship between decreased IGF1R signaling and suppressed cellular senescence in pancreatic β-cells. Future studies can further our understanding of the interaction between senescence and aging, developing interventions that restore β-cell function and identity, therefore preventing the progression to T2D.</p></sec>