Neratinib protects pancreatic beta cells in diabetes

Author:

Ardestani Amin,Li Sijia,Annamalai Karthika,Lupse Blaz,Geravandi Shirin,Dobrowolski Aleksandra,Yu Shan,Zhu Siying,Baguley Tyler D.,Surakattula Murali,Oetjen JaninaORCID,Hauberg-Lotte Lena,Herranz Raquel,Awal Sushil,Altenhofen Delsi,Nguyen-Tran Van,Joseph Sean,Schultz Peter G.,Chatterjee Arnab K.,Rogers Nikki,Tremblay Matthew S.,Shen Weijun,Maedler KathrinORCID

Abstract

Abstract The loss of functional insulin-producing β-cells is a hallmark of diabetes. Mammalian sterile 20-like kinase 1 (MST1) is a key regulator of pancreatic β-cell death and dysfunction; its deficiency restores functional β-cells and normoglycemia. The identification of MST1 inhibitors represents a promising approach for a β-cell-protective diabetes therapy. Here, we identify neratinib, an FDA-approved drug targeting HER2/EGFR dual kinases, as a potent MST1 inhibitor, which improves β-cell survival under multiple diabetogenic conditions in human islets and INS-1E cells. In a pre-clinical study, neratinib attenuates hyperglycemia and improves β-cell function, survival and β-cell mass in type 1 (streptozotocin) and type 2 (obese Leprdb/db) diabetic mouse models. In summary, neratinib is a previously unrecognized inhibitor of MST1 and represents a potential β-cell-protective drug with proof-of-concept in vitro in human islets and in vivo in rodent models of both type 1 and type 2 diabetes.

Funder

JDRF

Publisher

Springer Science and Business Media LLC

Subject

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

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