4.7 Article

Identification and Characterization of a Secondary Sodium-Binding Site and the Main Selectivity Determinants in the Human Concentrative Nucleoside Transporter 3

Journal

MOLECULAR PHARMACEUTICS
Volume 14, Issue 6, Pages 1980-1987

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.molpharmaceut.7b00085

Keywords

concentrative transporters; homology modelin; sodium-binding site; selectivity; nucleoside transport

Funding

  1. Spanish Ministerio de Economia [SAF2012-33481, SAF2014-57094-R]
  2. Catalan government [2014SGR1189]
  3. Spanish Secretariat of Research (MINECO) [SAF2011-23660, SAF2014-52067-R]
  4. predoctoral fellowships FPI from Ministerio de Ciencia e Innovacion

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The family of concentrative Ne+/nudeoside cotransporters in humans is constituted by three subtypes, namely, hCNT1, hCNT2, and hCNT3. Besides their different nucleoside selectivity, hCNT1 and hCNT2 have a Na+/nucleoside stoichiometry of 1:1, while for hCNT3 it is 2:1. This distinct stoichiometry of subtype 3 might hint the existence of a secondary sodium-binding site that is not present in the other two subtypes, but to date their three-dimensional structures remain unknown and the residues implicated in Na+ binding are unclear. In this work, we have identified and characterized the Na+ binding sites of hCNT3 by combining molecular modeling and mutagenesis studies. A model of the transporter was obtained by homology modeling, and key residues of two sodium-binding sites were identified and verified with a mutagenesis strategy. The structural model explains the altered sodium-binding properties of the hCNT3C602R polymorphic variant and supports previously generated data identifying the determinant residues of nucleoside selectivity, paving the way to understand how drugs can target this plasma membrane transporter.

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