The human organic cation transporter OCT1 and its role as a target for drug responses

Nicolas Brosseau, Dindial Ramotar*

*Corresponding author for this work

Research output: Contribution to journalReview articlepeer-review

23 Citations (Scopus)

Abstract

The human organic cation uptake transporter OCT1, encoded by the SLC22A1 gene, is highly expressed in the liver and reported to possess a broad substrate specificity. OCT1 operates by facilitated diffusion and allows the entry of nutrients into cells. Recent findings revealed that OCT1 can mediate the uptake of drugs for treating various diseases such as cancers. The levels of OCT1 expression correlate with the responses towards many drugs and functionally defective OCT1 lead to drug resistance. It has been recently proposed that OCT1 should be amongst the crucial drug targets used for pharmacogenomic analyses. Several single nucleotide polymorphisms exist and are distributed across the entire OCT1 gene. While there are differences in the OCT1 gene polymorphisms between populations, there are at least five variants that warrant consideration in any genetic screen. To date, and despite two decades of research into OCT1 functional role, it still remains uncertain what are the define substrates for this uptake transporter, although studies from mice revealed that one of the substrates is vitamin B1. It is also unclear how OCT1 recognizes a broad array of ligands and whether this involves specific modifications and interactions with other proteins. In this review, we highlight the current findings related to OCT1 with the aim of propelling further studies on this key uptake transporter.

Original languageEnglish
Pages (from-to)389-407
Number of pages19
JournalDrug Metabolism Reviews
Volume51
Issue number4
DOIs
Publication statusPublished - 2 Oct 2019
Externally publishedYes

Keywords

  • OCT1
  • Organic cation transporters
  • cancers
  • drug resistance
  • human OCT1 homologs
  • plasma membrane proteins
  • polymorphisms
  • post-translational modifications
  • substrates

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