Abstract

BackgroundAutophagy is a catabolic cellular process used for degradation of cytoplasmic organelles and preservation of cell viability. In this study we aimed to analyse the level of autophagy markers in benign and malignant prostate tissue and to evaluate the prognostic properties for patients with prostate cancer (PCa).ResultsLC3b expression was significantly upregulated in PCa, especially in metastatic and castration-resistant PCa samples compared to benign prostate tissue (p<0.001). Evaluation of expression in malignant radical prostatectomy specimens revealed an inverse association with preoperative serum PSA levels (p=0.02) and Gleason Score (p=0.07). LC3b immunoreactivity was identified as a novel predictor of PCa specific death after radical prostatectomy, independent of Gleason score, tumour stage, and surgical margin status in a multivariable cox regression analysis (hazard ratio 0.09, 95% confidence interval 0.01-0.69, p=0.021). A significant association of ATG-5 and Beclin 1 with LC3b expression could be noticed (p<0.001), but no link with other clincopathologic parameters was observed.Materials and MethodsA Tissue microarray containing 468 formalin-fixed, paraffin-embedded prostate tissue cores was stained immunohistochemically for major autophagy proteins LC3b, ATG5 and Beclin 1. Immunoreactivity was semiquantitatively scored and correlated with pathologic and clinical parameters, including tumour stage, Gleason score, preoperative PSA level, biochemical recurrence rate and survival. The median clinical follow-up was 132 months.ConclusionLC3b was significantly overexpressed in malignant compared to benign prostate tissue. However, positive LC3b immunoreactivity in PCa, as a marker of increased autophagy, was independently associated with a reduced disease-specific mortality.

Highlights

  • When prostate cancer (PCa) is localized in the prostate and considered significant, the treatment of choice is prostatectomy or radiation [1]

  • A total of 420/468 (89.7%) cores could be evaluated for LC3b, 429/468 (91.7%) for Beclin 1 and 417/468 (89.1%) for ATG5 immunostaining

  • LC3b and Beclin 1 expressions were significantly increased in primary malignant radical prostatectomy (RP) specimen (36.1% and 65.9%, p

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Summary

Introduction

When prostate cancer (PCa) is localized in the prostate and considered significant, the treatment of choice is prostatectomy or radiation [1]. In advanced and metastatic PCa androgen ablation is the standard of care to palliate symptoms and postpone cancer related complications [2]. Autophagy is a catabolic cellular mechanism involving degradation of unnecessary or dysfunctional cellular components through autophagosomes allowing maintenance of homeostasis and ensuring cell survival under stress conditions. Three types of LC3 were reported; A, B and C, with LC3b expression being the most valid marker of autophagosome formation [8] and one of the most widely used in situ techniques of autophagy measurement in benign and malignant tissue [9]. In this study we aimed to analyse the level of autophagy markers in benign and malignant prostate tissue and to evaluate the prognostic properties for patients with prostate cancer (PCa)

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