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Proximal tubular secretion of creatinine by organic cation transporter OCT2 in cancer patients

  • Giuliano Ciarimboli
  • , Cynthia S. Lancaster
  • , Eberhard Schlatter
  • , Ryan M. Franke
  • , Jason A. Sprowl
  • , Hermann Pavenstädt
  • , Vivian Massmann
  • , Denise Guckel
  • , Ron H.J. Mathijssen
  • , Wenjian Yang
  • , Ching Hon Pui
  • , Mary V. Relling
  • , Edwin Herrmann
  • , Alex Sparreboom
  • University of Münster
  • St. Jude Children Research Hospital
  • Erasmus University Rotterdam

Research output: Contribution to journalArticlepeer-review

151 Scopus citations

Abstract

Purpose: Knowledge of transporters responsible for the renal secretion of creatinine is key to a proper interpretation of serum creatinine and/or creatinine clearance as markers of renal function in cancer patients receiving chemotherapeutic agents. Experimental Design: Creatinine transport was studied in transfected HEK293 cells in vitro and in wildtype mice and age-matched organic cation transporter 1 and 2-deficient [Oct1/2(-/-)] mice ex vivo and in vivo. Clinical pharmacogenetic and transport inhibition studies were done in two separate cohorts of cancer patients. Results: Compared with wild-type mice, creatinine clearance was significantly impaired in Oct1/2(-/-) mice. Furthermore, creatinine inhibited organic cation transport in freshly isolated proximal tubules from wild-type mice and humans, but not in those from Oct1/2(-/-) mice. In a genetic association analysis (n =590), several polymorphisms around the OCT2/SLC22A2 gene locus, including rs2504954 (P=0.000873), were significantly associated with age-adjusted creatinine levels. Furthermore, in cancer patients (n = 68), the OCT2 substrate cisplatin caused an acute elevation of serum creatinine (P = 0.0083), consistent with inhibition of an elimination pathway. Conclusions: Collectively, this study shows that OCT2 plays a decisive role in the renal secretion of creatinine. This process can be inhibited by OCT2 substrates, which impair the usefulness of creatinine as a marker of renal function.

Original languageEnglish
Pages (from-to)1101-1108
Number of pages8
JournalClinical Cancer Research
Volume18
Issue number4
DOIs
StatePublished - Feb 15 2012

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