Inhibition of IKK 3 and TBK1 Improves Glucose Control in a Subset of Patients with Type 2 Diabetes
Date
2017Author
Neidert, Adam H.
Chenevert, Thomas L.
Hench, Rita
Korytnaya, Evgenia
Saltiel, Alan R.
Oral, Elif A.
Reilly, Shannon M.
Gomez, Andrew V.
Meral, Rasimcan
Butz, Laura
Ajluni, Nevin
Evans, Ronald M.
Downes, Michael
Ahmadian, Maryam
Liddle, Christopher
Yu, Ruth
Jain, Mohit
Lehmann, Kim
Zhao, Peng
Poirier, BreAnne
Horowitz, Jeffrey F.
Rus, Diana
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Show full item recordAbstract
Numerous studies indicate an inflammatory link between obesity and type 2 diabetes. The inflammatory kinases IKK 3 and TBK1 are elevated in obesity; their inhibition in obese mice reduces weight, insulin resistance, fatty liver and inflammation. Here we studied amlexanox, an inhibitor of IKK 3 and TBK1, in a proof-of-concept randomized, double-blind, placebo-controlled study of 42 obese patients with type 2 diabetes and nonalcoholic fatty liver disease. Treatment of patients with amlexanox produced a statistically significant reduction in Hemoglobin A1c and fructosamine. Interestingly, a subset of drug responders also exhibited improvements in insulin sensitivity and hepatic steatosis. This subgroup was characterized by a distinct inflammatory gene expression signature from biopsied subcutaneous fat at baseline. They also exhibited a unique pattern of gene expression changes in response to amlexanox, consistent with increased energy expenditure. Together, these data suggest that dual-specificity inhibitors of IKK 3 and TBK1 may be effective therapies for metabolic disease in an identifiable subset of patients.
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