Isozyme-nonselective N-Substituted Bipiperidylcarboxamide Acetyl-CoA Carboxylase Inhibitors Reduce Tissue Malonyl-CoA Concentrations, Inhibit Fatty Acid Synthesis, and Increase Fatty Acid Oxidation in Cultured Cells and in Experimental Animals

Harwood, H. James; Petras, Stephen F.; Shelly, Lorraine D.; Zaccaro, Lawrence M.; Perry, David A.; Makowski, M.; Hargrove, Diane M.; Martin, Kelly A.; Tracey, W. Ross; Chapman, Justin; Magee, William P.; Dalvie, Deepak; Soliman, Victor F.; Martin, William H.; Mularski, Christian J.; Eisenbeis, Shane A.

doi:10.1074/jbc.m304481200

Cited by 224 publications

(231 citation statements)

References 54 publications

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“…CP-640186, an inhibitor of acetyl-CoA carboxylase [21], partially inhibited insulin release from pancreatic islets and INS-1 832/13 cells (Figures 4 and 5). Triclosan is a potent inhibitor of the enoyl-acyl carrier protein reductase enzyme of the prokaryotic type II fatty acid synthase complex.…”

Section: Inhibition Of Insulin Release By Inhibitors Of Lipogenesismentioning

confidence: 91%

“…TOFA (5-(tetradecyloxy)-2-furoic acid) was from Alexis Biochemicals. CP-640186 was from H. James Harwood at Pfizer [21]. Triclosan (5-chloro-2-(2,4-dichlorophenoxy)-phenol) was from Fluka BioChemika.…”

Section: Experimental Procedures Materialsmentioning

confidence: 99%

“…Triclosan (5-chloro-2-(2,4-dichlorophenoxy)-phenol) was from Fluka BioChemika. Anti-actin (20)(21)(22)(23)(24)(25)(26)(27)(28)(29)(30)(31)(32)(33) antibody (catalog number A5060) and other chemicals were from Sigma. INS-1 832/13 cells were from Chris Newgard [22].…”

Section: Experimental Procedures Materialsmentioning

confidence: 99%

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The role of rapid lipogenesis in insulin secretion: Insulin secretagogues acutely alter lipid composition of INS-1 832/13 cells

MacDonald

Dobrzyń

Ntambi

et al. 2008

Archives of Biochemistry and Biophysics

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Pancreatic beta cell mitochondria convert insulin secretagogues into products that support insulin exocytosis. We explored the idea that lipids are some of these products formed from acyl group transfer out of mitochondria to the cytosol, the site of lipid synthesis. There are two isoforms of acetyl-CoA carboxylase, the enzyme that forms malonyl-CoA from which C 2 units for lipid synthesis are formed. We found that ACC1, the isoform seen in lipogenic tissues, is the only isoform present in human and rat pancreatic islets and INS-1 832/13 cells. Inhibitors of ACC and fatty acid synthase inhibited insulin release in islets and INS-1 cells. Carbon from glucose and pyruvate were rapidly incorporated into many lipid classes in INS-1 cells. Glucose and other insulin secretagogues acutely increased many lipids with C 14 -C 24 chains including individual cholesterol esters, phospholipids and fatty acids. Many phosphatidylcholines and phosphatidylserines were increased and many phosphatidylinositols and several phosphatidylethanolamines were decreased. The results suggest that lipid remodeling and rapid lipogenesis from secretagogue carbon support insulin secretion.

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Section: Inhibition Of Insulin Release By Inhibitors Of Lipogenesismentioning

confidence: 91%

Section: Experimental Procedures Materialsmentioning

confidence: 99%

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The role of rapid lipogenesis in insulin secretion: Insulin secretagogues acutely alter lipid composition of INS-1 832/13 cells

MacDonald

Dobrzyń

Ntambi

et al. 2008

Archives of Biochemistry and Biophysics

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“…One of the proposed medical applications of the enzymes depends on their inhibition, which is associated with inhibition of fatty acids synthesis and stimulation of fatty acids oxidation, and which, in consequence, might reduce cardiovascular risk in metabolic syndrome. Compound CP-610431 bipiperidine derivative, and its analog of higher metabolic stability CP-640186, isolated by high-throughput screening, are such inhibitors active against both ACCase isoforms (Harwood, Jr., et al 2003). Kinetic studies on ACCase -CP-610431 complex and the crystal structure of yeast CT domain -CP-640186 complex have revealed that the binding site for these inhibitors is located on the carboxyl transferase domain (Zhang et al, 2004).…”

Section: Human Accase As Target In Diseases Treatmentmentioning

confidence: 99%

OPINIONS Acetyl-coenzyme A carboxylase – an attractive enzyme for biotechnology

Podkowiński¹,

Tworak²

2011

bta

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Acetyl-CoA carboxylase catalyzes the carboxylation of acetyl-CoA to malonyl-CoA. This reaction constitutes the first committed step of fatty acid synthesis in most organisms, while its product also serves as a universal precursor for various other high-value compounds. The important regulatory and rate-limiting role of acetyl-CoA carboxylase makes this enzyme a powerful tool in a variety of biotechnological and medical projects. This review presents the current knowledge on structural and functional features of the enzyme and focuses on its divergent applications. Different metabolic engineering attempts that lead to the production of various compounds, such as fatty acids, polyketides or flavonoids, are presented and their advantages and limitations discussed. The importance of studies on acetyl-CoA carboxylase activity for design and development of new herbicides and antibiotics as well as for medical intervention is also highlighted. Acetyl-coenzyme A carboxylase -enzyme architecture, biochemistry and its role in cell physiologyA variety of biotechnological projects targeted to modulate acetyl-coenzyme A carboxylase activity in bacteria, plants and humans have been proposed and experimentally tested. Here, we would like to present a comprehensive review of these strategies together with a survey of the potential of acetyl-CoA carboxylase for biotechnology.Acetyl-coenzyme A carboxylase (ACC, E.C.6.4.1.2), recognized as an essential enzyme for all Eukaryotes and the majority of Bacteria, is responsible for carboxylation of acetyl-CoA that results in malonyl-coenzyme A formation (Fig. 1). Malonyl-CoA is a major building block for compounds such as fatty acids, polyketides and flavonoids -important components for cell growth, as well as for food, pharmaceuticals and energy production.The malonyl-CoA synthesis consists of two half-reactions (Nikolau et al., 2003). The first one, adenosine triphosphate-dependent carboxylation of biotin prosthetic group covalently bound to a module named biotin carboxyl carrier protein (BCCP), is catalyzed by ACCase segment of biotin carboxylase activity (BC) (Fig. 2). This reaction is immediately followed by the second half-re action: the transfer of a carboxyl group from carboxylated biotin to acetyl-CoA, resulting in malonyl-CoA formation. Carboxyl transferase (CT) is a module that catalyzes the second reaction and provides the required specificity in recognition of the carboxyl acceptor (acetyl-CoA). The ACCase model usually presents BCCP, a module with covalently attached biotin, as a beam responsible for biotin dislocation between two active centers -one with BT and the other with CT activity. The three (Fig. 3). The prokaryotic and eukaryotic types of ACCases are evolutionary related and the phylogeny of the modules provides some hints about their cenancestor, a split between Archaea and Bacteria, and arising of Eukaryota (Lombard and Moreira, 2011).Phylogeny is out of scope of this manuscript, but acetyl-coenzyme A carboxylases from various organisms representing v...

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“…Second, the first Acc2 KO animals did not show a switching of fuels (i.e. change in respiratory exchange ratio [RER]), but rather an increase in Á V O 2 , which was not predicted by bioenergetics or evident with a dual Acc1 and Acc2 inhibitor in rats [12]. Recently, the Acc2 KO model was independently generated and resulted in an opposite phenotype [13].…”

Section: The Premisementioning

confidence: 99%

Targeting energy expenditure via fuel switching and beyond

Geisler

2010

Diabetologia

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Since over-nutrition accelerates the development of obesity, progression to type 2 diabetes, and the associated co-morbidity and mortality, there has been a keen interest in therapeutic interventions targeting mechanisms that may curb appetite, increase energy expenditure or at least attenuate insulin resistance. Over the past decade, numerous peri-mitochondrial targets in the de novo lipid synthesis pathway have been linked to an increase in energy expenditure and the drug development industry has pursued the gene products involved as candidates to develop drugs against. The basis of this link, and specifically the premise that lowering tissue and cellular malonyl-CoA can increase energy expenditure, is scrutinised here. The argument presented is that fuel switching as effected by changes in cellular malonyl-CoA concentrations will not trigger the mitochondria to increase energy expenditure because: (1) an increase in beta-oxidation by lowering respiratory exchange ratio (indicative of the metabolic fuel consumed) does not equal an increase in energy expenditure (how rapidly fuel is consumed); (2) the ATP:oxygen ratios (i.e. ATP energy made:oxygen required for the reaction) are similar when metabolising lipids (2.8) vs glucose (3.0); (3) substrate availability (NEFA) does not drive energy expenditure in vivo; and (4) the availability of ADP in the mitochondrial matrix determines the rate of energy expenditure, not the availability of fuel to enter the mitochondrial matrix. To increase mitochondrial energy expenditure, work must be done (exercise) and/or the mitochondrial proton leak must be enhanced, both of which increase availability of ADP. In fact, despite the historic taboo of chemical uncoupling, this mechanism validated in humans is closest on task to increasing whole-body energy expenditure. Chemical uncoupling mimics the naturally occurring phenomenon of proton leak, accelerating the metabolism of glucose and lipids. However, it is completely non-genomic (i.e. the target is a location, not a gene product) and is not associated with addiction or mood alterations common to satiety agents. A significant hurdle for drug development is to discover a safe mitochondrial uncoupler and to formulate it potentially as a pro-drug and/or oral pump, to avoid the issue of overdosing experienced in the 1930s. The potential therapeutic impact of such a compound for an overnutritioned patient population could be profound. If effective, the mitochondrial uncoupler mechanism could resolve many of the associated diseases such as type 2 diabetes, hypertension, obesity, depression, sleep apnoea, non-alcoholic steatohepatitis, insulin resistance and hyperlipidaemia, therefore becoming a 'disease-modifying therapy'.

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Isozyme-nonselective N-Substituted Bipiperidylcarboxamide Acetyl-CoA Carboxylase Inhibitors Reduce Tissue Malonyl-CoA Concentrations, Inhibit Fatty Acid Synthesis, and Increase Fatty Acid Oxidation in Cultured Cells and in Experimental Animals

Cited by 224 publications

References 54 publications

The role of rapid lipogenesis in insulin secretion: Insulin secretagogues acutely alter lipid composition of INS-1 832/13 cells

The role of rapid lipogenesis in insulin secretion: Insulin secretagogues acutely alter lipid composition of INS-1 832/13 cells

OPINIONS Acetyl-coenzyme A carboxylase – an attractive enzyme for biotechnology

Targeting energy expenditure via fuel switching and beyond

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