The dynamic clustering of insulin receptor underlies its signaling and is disrupted in insulin resistance

Author:

Dall’Agnese Alessandra,Platt Jesse M.,Zheng Ming M.,Friesen MaxORCID,Dall’Agnese Giuseppe,Blaise Alyssa M.ORCID,Spinelli Jessica B.ORCID,Henninger Jonathan E.ORCID,Tevonian Erin N.,Hannett Nancy M.,Lazaris CharalamposORCID,Drescher Hannah K.,Bartsch Lea M.,Kilgore Henry R.ORCID,Jaenisch RudolfORCID,Griffith Linda G.ORCID,Cisse Ibrahim I.ORCID,Jeppesen Jacob F.,Lee Tong I.ORCID,Young Richard A.ORCID

Abstract

AbstractInsulin receptor (IR) signaling is central to normal metabolic control and is dysregulated in metabolic diseases such as type 2 diabetes. We report here that IR is incorporated into dynamic clusters at the plasma membrane, in the cytoplasm and in the nucleus of human hepatocytes and adipocytes. Insulin stimulation promotes further incorporation of IR into these dynamic clusters in insulin-sensitive cells but not in insulin-resistant cells, where both IR accumulation and dynamic behavior are reduced. Treatment of insulin-resistant cells with metformin, a first-line drug used to treat type 2 diabetes, can rescue IR accumulation and the dynamic behavior of these clusters. This rescue is associated with metformin’s role in reducing reactive oxygen species that interfere with normal dynamics. These results indicate that changes in the physico-mechanical features of IR clusters contribute to insulin resistance and have implications for improved therapeutic approaches.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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