TY - JOUR T1 - Cellular Responses to the Metal-Binding Properties of Metformin A1 - Logie,Lisa A1 - Harthill,Jean A1 - Patel,Kashyap A1 - Bacon,Sandra A1 - Hamilton,D. Lee A1 - Macrae,Katherine A1 - McDougall,Gordon A1 - Wang,Huan-Huan A1 - Xue,Lin A1 - Jiang,Hua A1 - Sakamoto,Kei A1 - Prescott,Alan R. A1 - Rena,Graham AU - Logie,Lisa AU - Harthill,Jean AU - Patel,Kashyap AU - Bacon,Sandra AU - Hamilton,D. Lee AU - Macrae,Katherine AU - McDougall,Gordon AU - Wang,Huan-Huan AU - Xue,Lin AU - Jiang,Hua AU - Sakamoto,Kei AU - Prescott,Alan R. AU - Rena,Graham PY - 2012/6 Y1 - 2012/6 N2 -

In recent decades, the antihyperglycemic biguanide metformin has been used extensively in the treatment of type 2 diabetes, despite continuing uncertainty over its direct target. In this article, using two independent approaches, we demonstrate that cellular actions of metformin are disrupted by interference with its metal-binding properties, which have been known for over a century but little studied by biologists. We demonstrate that copper sequestration opposes known actions of metformin not only on AMP-activated protein kinase (AMPK)-dependent signaling, but also on S6 protein phosphorylation. Biguanide/metal interactions are stabilized by extensive pi-electron delocalization and by investigating analogs of metformin; we provide evidence that this intrinsic property enables biguanides to regulate AMPK, glucose production, gluconeogenic gene expression, mitochondrial respiration, and mitochondrial copper binding. In contrast, regulation of S6 phosphorylation is prevented only by direct modification of the metal-liganding groups of the biguanide structure, supporting recent data that AMPK and S6 phosphorylation are regulated independently by biguanides. Additional studies with pioglitazone suggest that mitochondrial copper is targeted by both of these clinically important drugs. Together, these results suggest that cellular effects of biguanides depend on their metal-binding properties. This link may illuminate a better understanding of the molecular mechanisms enabling antihyperglycemic drug action. Diabetes 61:1423-1433, 2012

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In recent decades, the antihyperglycemic biguanide metformin has been used extensively in the treatment of type 2 diabetes, despite continuing uncertainty over its direct target. In this article, using two independent approaches, we demonstrate that cellular actions of metformin are disrupted by interference with its metal-binding properties, which have been known for over a century but little studied by biologists. We demonstrate that copper sequestration opposes known actions of metformin not only on AMP-activated protein kinase (AMPK)-dependent signaling, but also on S6 protein phosphorylation. Biguanide/metal interactions are stabilized by extensive pi-electron delocalization and by investigating analogs of metformin; we provide evidence that this intrinsic property enables biguanides to regulate AMPK, glucose production, gluconeogenic gene expression, mitochondrial respiration, and mitochondrial copper binding. In contrast, regulation of S6 phosphorylation is prevented only by direct modification of the metal-liganding groups of the biguanide structure, supporting recent data that AMPK and S6 phosphorylation are regulated independently by biguanides. Additional studies with pioglitazone suggest that mitochondrial copper is targeted by both of these clinically important drugs. Together, these results suggest that cellular effects of biguanides depend on their metal-binding properties. This link may illuminate a better understanding of the molecular mechanisms enabling antihyperglycemic drug action. Diabetes 61:1423-1433, 2012

U2 - 10.2337/db11-0961 DO - 10.2337/db11-0961 M1 - Article JO - Diabetes JF - Diabetes SN - 0012-1797 IS - 6 VL - 61 SP - 1423 EP - 1433 ER -