Comprehensive microRNA profiling in acetaminophen toxicity identifies novel circulating biomarkers for human liver and kidney injury

نویسندگان

  • A. D. B. Vliegenthart
  • J. M. Shaffer
  • J. I. Clarke
  • L. E. J. Peeters
  • A. Caporali
  • D. N. Bateman
  • D. M. Wood
  • P. I. Dargan
  • D. G. Craig
  • J. K. Moore
  • A. I. Thompson
  • N. C. Henderson
  • D. J. Webb
  • J. Sharkey
  • D. J. Antoine
  • B. K. Park
  • M. A. Bailey
  • E. Lader
  • K. J. Simpson
  • J. W. Dear
چکیده

Our objective was to identify microRNA (miRNA) biomarkers of drug-induced liver and kidney injury by profiling the circulating miRNome in patients with acetaminophen overdose. Plasma miRNAs were quantified in age- and sex-matched overdose patients with (N = 27) and without (N = 27) organ injury (APAP-TOX and APAP-no TOX, respectively). Classifier miRNAs were tested in a separate cohort (N = 81). miRNA specificity was determined in non-acetaminophen liver injury and murine models. Sensitivity was tested by stratification of patients at hospital presentation (N = 67). From 1809 miRNAs, 75 were 3-fold or more increased and 46 were 3-fold or more decreased with APAP-TOX. A 16 miRNA classifier model accurately diagnosed APAP-TOX in the test cohort. In humans, the miRNAs with the largest increase (miR-122-5p, miR-885-5p, miR-151a-3p) and the highest rank in the classifier model (miR-382-5p) accurately reported non-acetaminophen liver injury and were unaffected by kidney injury. miR-122-5p was more sensitive than ALT for reporting liver injury at hospital presentation, especially combined with miR-483-3p. A miRNA panel was associated with human kidney dysfunction. In mice, miR-122-5p, miR-151a-3p and miR-382-5p specifically reported APAP toxicity - being unaffected by drug-induced kidney injury. Profiling of acetaminophen toxicity identified multiple miRNAs that report acute liver injury and potential biomarkers of drug-induced kidney injury.

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عنوان ژورنال:

دوره 5  شماره 

صفحات  -

تاریخ انتشار 2015