4.7 Article

Thioredoxin 1 as a subcellular biomarker of redox imbalance in human prostate cancer progression

Journal

FREE RADICAL BIOLOGY AND MEDICINE
Volume 49, Issue 12, Pages 2078-2087

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.freeradbiomed.2010.10.691

Keywords

Thioredoxin 1; Reactive oxygen species; Redox state; Prostate cancer; Androgen; Free radicals

Funding

  1. University of Wisconsin Department of Pathology Research and Development Committee
  2. National Cancer Institute [P30 CA014520]
  3. NIH [RO1 CA073599, RO1 CA194853, RO1 AG012350, RO1 CA115801]

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We determined protein levels and subcellular distribution of thioredoxin 1 (Trx1) in human prostate tissues using tissue microarrays and analyzed redox changes in Trx1 in the nucleus and cytoplasm in cell culture models with a redox Western blot technique We demonstrated increased nuclear Trx1 levels in high- versus low-grade human prostate cancers Despite Increased protein levels the oxidized forms of nuclear Trx1 were higher in prostate cancer cell lines compared to their benign counterparts suggesting that nuclear redox imbalance occurred selectively in cancer cells A growth-stimulating dose of androgen caused transient oxidation of Trx1 in androgen-responsive prostate cancer cells only suggesting a loss of both androgen and redox-signaling mechanisms during cancer progression Androgen independent PC3 cells showed a significant Increase in nuclear and cytoplasmic Trx1 protein levels but a significant decrease in total Trx activity Trx1 redox state and activity correlated with the sensitivity of prostate cancer cells to pro-oxidant agents and downregulation of Trx1 sensitized cancer cells to these agents Our findings suggest that loss of Trx function because of oxidation and corresponding redox imbalance may play important roles in prostate cancer progression and response to therapies and Trx1 may serve as a biomarker of subcellular redox imbalance in prostate cancer Published by Elsevier Inc

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