Structural basis for antibiotic transport and inhibition in PepT2, the mammalian proton-coupled peptide transporter.

Author:

Newstead Simon1ORCID,Parker Joanne1ORCID,Deme Justin2ORCID,Lichtinger Simon1ORCID,Kuteyi Gabriel1,Biggin Philip1ORCID,Lea Susan3ORCID

Affiliation:

1. University of Oxford

2. National Cancer Institute, National Institutes of Health

3. Center for Structural Biology, Center for Cancer Research, National Cancer Institute

Abstract

Abstract

The uptake and elimination of beta-lactam antibiotics in the human body are facilitated by the proton-coupled peptide transporters PepT1 (SLC15A1) and PepT2 (SLC15A2). The mechanism by which SLC15 family transporters recognize and discriminate between different drug classes and dietary peptides remains unclear, hampering efforts to improve antibiotic pharmacokinetics through targeted drug design and delivery. Here, we present cryo-EM structures of the mammalian proton-coupled peptide transporter, PepT2, in complex with the widely used beta-lactam antibiotics cefadroxil, amoxicillin and cloxacillin. Our structures, combined with pharmacophore mapping, molecular dynamics simulations and biochemical assays, establish the mechanism of antibiotic recognition and the important role of protonation in drug binding and transport.

Publisher

Research Square Platform LLC

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