PLoS ONE (Jan 2013)

Hepatic mitochondrial function analysis using needle liver biopsy samples.

  • Michael J J Chu,
  • Anthony R J Phillips,
  • Alexander W G Hosking,
  • Julia R MacDonald,
  • Adam S J R Bartlett,
  • Anthony J R Hickey

DOI
https://doi.org/10.1371/journal.pone.0079097
Journal volume & issue
Vol. 8, no. 10
p. e79097

Abstract

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Backgrounds and aimCurrent assessment of pre-operative liver function relies upon biochemical blood tests and histology but these only indirectly measure liver function. Mitochondrial function (MF) analysis allows direct measurement of cellular metabolic function and may provide an additional index of hepatic health. Conventional MF analysis requires substantial tissue samples (>100 mg) obtained at open surgery. Here we report a method to assess MF using MethodsAn 18G Bard® Max-core® biopsy instrument was used to collect samples. The optimal Tru-cut® sample weight, stability in ice-cold University of Wisconsin solution, reproducibility and protocol utility was initially evaluated in Wistar rat livers then confirmed in human samples. MF was measured in saponin-permeabilized samples using high-resolution respirometry.ResultsThe average mass of a single rat and human liver Tru-cut® biopsy was 5.60±0.30 and 5.16±0.15 mg, respectively (mean; standard error of mean). Two milligram of sample was found the lowest feasible mass for the MF assay. Tissue MF declined after 1 hour of cold storage. Six replicate measurements within rats and humans (n = 6 each) showed low coefficient of variation (ConclusionConsistent measurement of liver MF and detection of derangement in a disease state was successfully demonstrated using less than half the tissue from a single Tru-cut® biopsy. Using this technique outpatient assessment of liver MF is now feasible, providing a new assay for the evaluation of hepatic function.