EuPA Open Proteomics (Mar 2016)

Profiling the tumor microenvironment proteome in prostate cancer using laser capture microdissection coupled to LC–MS—A technical report

  • L. Staunton,
  • C. Tonry,
  • R. Lis,
  • S. Finn,
  • J. O’Leary,
  • M. Loda,
  • M. Bowden,
  • S.R. Pennington

DOI
https://doi.org/10.1016/j.euprot.2015.11.001
Journal volume & issue
Vol. 10, no. C
pp. 19 – 23

Abstract

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Laser capture microdissection (LCM) allows microscopic procurement of specific cell types from tissue sections. Here, we present an optimized workflow for coupling LCM to LC–MS/MS including: sectioning of tissue, a standard LCM workflow, protein digestion and advanced LC–MS/MS. Soluble proteins extracted from benign epithelial cells, their associated stroma, tumor epithelial cells and their associated stromal cells from a single patient tissue sample were digested and profiled using advanced LC–MS/MS. The correlation between technical replicates was R2 = 0.99 with a mean % CV of 9.55% ± 8.73. The correlation between sample replicates was R2 = 0.97 with a mean % CV of 13.83% ± 10.17. This represents a robust, systematic approach for profiling of the tumor microenvironment using LCM coupled to label-free LC–MS/MS.

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