Key features of inhibitor binding to the human mitochondrial pyruvate carrier hetero-dimer

Sotiria Tavoulari; Tom J J Schirris; Vasiliki Mavridou; Chancievan Thangaratnarajah; Martin S King; Daniel T D Jones; Shujing Ding; Ian M Fearnley; Edmund R S Kunji

doi:10.1016/j.molmet.2022.101469

Key features of inhibitor binding to the human mitochondrial pyruvate carrier hetero-dimer

Mol Metab. 2022 Jun:60:101469. doi: 10.1016/j.molmet.2022.101469. Epub 2022 Mar 10.

Authors

Sotiria Tavoulari¹, Tom J J Schirris², Vasiliki Mavridou², Chancievan Thangaratnarajah², Martin S King², Daniel T D Jones², Shujing Ding², Ian M Fearnley², Edmund R S Kunji³

Affiliations

¹ Medical Research Council Mitochondrial Biology Unit, University of Cambridge, Keith Peters Building, Cambridge Biomedical Campus, Hills Road, Cambridge, CB2 0XY, United Kingdom. Electronic address: st632@mrc-mbu.cam.ac.uk.
² Medical Research Council Mitochondrial Biology Unit, University of Cambridge, Keith Peters Building, Cambridge Biomedical Campus, Hills Road, Cambridge, CB2 0XY, United Kingdom.
³ Medical Research Council Mitochondrial Biology Unit, University of Cambridge, Keith Peters Building, Cambridge Biomedical Campus, Hills Road, Cambridge, CB2 0XY, United Kingdom. Electronic address: ek@mrc-mbu.cam.ac.uk.

Abstract

Objective: The mitochondrial pyruvate carrier (MPC) has emerged as a promising drug target for metabolic disorders, including non-alcoholic steatohepatitis and diabetes, metabolically dependent cancers and neurodegenerative diseases. A range of structurally diverse small molecule inhibitors have been proposed, but the nature of their interaction with MPC is not understood, and the composition of the functional human MPC is still debated. The goal of this study was to characterise the human MPC protein in vitro, to understand the chemical features that determine binding of structurally diverse inhibitors and to develop novel higher affinity ones.

Methods: We recombinantly expressed and purified human MPC hetero-complexes and studied their composition, transport and inhibitor binding properties by establishing in vitro transport assays, high throughput thermostability shift assays and pharmacophore modeling.

Results: We determined that the functional unit of human MPC is a hetero-dimer. We compared all different classes of MPC inhibitors to find that three closely arranged hydrogen bond acceptors followed by an aromatic ring are shared characteristics of all inhibitors and represent the minimal requirement for high potency. We also demonstrated that high affinity binding is not attributed to covalent bond formation with MPC cysteines, as previously proposed. Following the basic pharmacophore properties, we identified 14 new inhibitors of MPC, one outperforming compound UK5099 by tenfold. Two are the commonly prescribed drugs entacapone and nitrofurantoin, suggesting an off-target mechanism associated with their adverse effects.

Conclusions: This work defines the composition of human MPC and the essential MPC inhibitor characteristics. In combination with the functional assays we describe, this new understanding will accelerate the development of clinically relevant MPC modulators.

Keywords: Inhibition; Mitochondria; Mitochondrial pyruvate carrier; Mitochondrial transport; Small molecules.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Humans
Mitochondria / metabolism
Mitochondrial Membrane Transport Proteins* / metabolism
Mitochondrial Proteins / metabolism
Monocarboxylic Acid Transporters* / metabolism
Pyruvic Acid / metabolism

Key features of inhibitor binding to the human mitochondrial pyruvate carrier hetero-dimer

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