Selective Inhibition of FOXO1 Activator/Repressor Balance Modulates Hepatic Glucose Handling

Fanny Langlet; Rebecca A. Haeusler; Daniel Lindén; Elke Ericson; Tyrrell Norris; Anders Johansson; Joshua R. Cook; Kumiko Aizawa; Ling Wang; Christoph Buettner; Domenico Accili

doi:10.1016/j.cell.2017.09.045

Selective Inhibition of FOXO1 Activator/Repressor Balance Modulates Hepatic Glucose Handling

Fanny Langlet, Rebecca A. Haeusler, Daniel Lindén, Elke Ericson, Tyrrell Norris, Anders Johansson, Joshua R. Cook, Kumiko Aizawa, Ling Wang, Christoph Buettner, Domenico Accili

Research output: Contribution to journal › Article › peer-review

161 Scopus citations

Abstract

Insulin resistance is a hallmark of diabetes and an unmet clinical need. Insulin inhibits hepatic glucose production and promotes lipogenesis by suppressing FOXO1-dependent activation of G6pase and inhibition of glucokinase, respectively. The tight coupling of these events poses a dual conundrum: mechanistically, as the FOXO1 corepressor of glucokinase is unknown, and clinically, as inhibition of glucose production is predicted to increase lipogenesis. Here, we report that SIN3A is the insulin-sensitive FOXO1 corepressor of glucokinase. Genetic ablation of SIN3A abolishes nutrient regulation of glucokinase without affecting other FOXO1 target genes and lowers glycemia without concurrent steatosis. To extend this work, we executed a small-molecule screen and discovered selective inhibitors of FOXO-dependent glucose production devoid of lipogenic activity in hepatocytes. In addition to identifying a novel mode of insulin action, these data raise the possibility of developing selective modulators of unliganded transcription factors to dial out adverse effects of insulin sensitizers. The transcriptional output of FOXO1 can be selectively modulated in a way that might reduce adverse effects of insulin sensitizers.

Original language	English
Pages (from-to)	824-835.e18
Journal	Cell
Volume	171
Issue number	4
DOIs	https://doi.org/10.1016/j.cell.2017.09.045
State	Published - 2 Nov 2017

Keywords

diabetes
drug therapy
hepatic glucose production
hepatosteatosis
insulin resistance
insulin sensitizers
lipogenesis
selective modulators
small molecule inhibitor
transcription repressor

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10.1016/j.cell.2017.09.045

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title = "Selective Inhibition of FOXO1 Activator/Repressor Balance Modulates Hepatic Glucose Handling",

abstract = "Insulin resistance is a hallmark of diabetes and an unmet clinical need. Insulin inhibits hepatic glucose production and promotes lipogenesis by suppressing FOXO1-dependent activation of G6pase and inhibition of glucokinase, respectively. The tight coupling of these events poses a dual conundrum: mechanistically, as the FOXO1 corepressor of glucokinase is unknown, and clinically, as inhibition of glucose production is predicted to increase lipogenesis. Here, we report that SIN3A is the insulin-sensitive FOXO1 corepressor of glucokinase. Genetic ablation of SIN3A abolishes nutrient regulation of glucokinase without affecting other FOXO1 target genes and lowers glycemia without concurrent steatosis. To extend this work, we executed a small-molecule screen and discovered selective inhibitors of FOXO-dependent glucose production devoid of lipogenic activity in hepatocytes. In addition to identifying a novel mode of insulin action, these data raise the possibility of developing selective modulators of unliganded transcription factors to dial out adverse effects of insulin sensitizers. The transcriptional output of FOXO1 can be selectively modulated in a way that might reduce adverse effects of insulin sensitizers.",

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author = "Fanny Langlet and Haeusler, {Rebecca A.} and Daniel Lind{\'e}n and Elke Ericson and Tyrrell Norris and Anders Johansson and Cook, {Joshua R.} and Kumiko Aizawa and Ling Wang and Christoph Buettner and Domenico Accili",

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AU - Langlet, Fanny

AU - Haeusler, Rebecca A.

AU - Lindén, Daniel

AU - Ericson, Elke

AU - Norris, Tyrrell

AU - Johansson, Anders

AU - Cook, Joshua R.

AU - Aizawa, Kumiko

AU - Wang, Ling

AU - Buettner, Christoph

AU - Accili, Domenico

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AB - Insulin resistance is a hallmark of diabetes and an unmet clinical need. Insulin inhibits hepatic glucose production and promotes lipogenesis by suppressing FOXO1-dependent activation of G6pase and inhibition of glucokinase, respectively. The tight coupling of these events poses a dual conundrum: mechanistically, as the FOXO1 corepressor of glucokinase is unknown, and clinically, as inhibition of glucose production is predicted to increase lipogenesis. Here, we report that SIN3A is the insulin-sensitive FOXO1 corepressor of glucokinase. Genetic ablation of SIN3A abolishes nutrient regulation of glucokinase without affecting other FOXO1 target genes and lowers glycemia without concurrent steatosis. To extend this work, we executed a small-molecule screen and discovered selective inhibitors of FOXO-dependent glucose production devoid of lipogenic activity in hepatocytes. In addition to identifying a novel mode of insulin action, these data raise the possibility of developing selective modulators of unliganded transcription factors to dial out adverse effects of insulin sensitizers. The transcriptional output of FOXO1 can be selectively modulated in a way that might reduce adverse effects of insulin sensitizers.

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Selective Inhibition of FOXO1 Activator/Repressor Balance Modulates Hepatic Glucose Handling

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Keywords

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