Brazilian Berry Extract Differentially Induces Inflammatory and Immune Responses in Androgen Dependent and Independent Prostate Cancer Cells

Larissa Akemi Kido; Isabela Maria Urra Rossetto; Andressa Mara Baseggio; Gabriela Bortolanza Chiarotto; Letícia Ferreira Alves; Felipe Rabelo Santos; Celina de Almeida Lamas; Mário Roberto Maróstica JR; Valéria Helena Alves Cagnon

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Brazilian Berry Extract Differentially Induces Inflammatory and Immune Responses in Androgen Dependent and Independent Prostate Cancer Cells

Author: Larissa Akemi KIDO ¹ ; Isabela Maria URRA ROSSETTO ; Andressa Mara BASEGGIO ; Gabriela Bortolanza CHIAROTTO ; Letícia Ferreira ALVES ; Felipe Rabelo SANTOS ; Celina de ALMEIDA LAMAS ; Mário Roberto MARÓSTICA JR ; Valéria Helena ALVES CAGNON
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1. Department of Structural and Functional Biology, Institute of Biology, São Paulo, Brazil
Publication Type:Original Article
From:Journal of Cancer Prevention 2022;27(3):182-191
CountryRepublic of Korea
Language:English
Abstract: Jaboticaba is a Brazilian berry, which is rich in fibers and bioactive compounds and shows high antioxidant and antiproliferative activities. Prostate cancer (PCa) is the second most common type of cancer among men and its progression is influenced by androgens and inflammation. Previous studies reported the ability of the jaboticaba to modulate pathways involved in prostate diseases. The main objective of this study was to provide significant data about molecular targets of the jaboticaba peel extract (JPE) and its mechanisms of action in PCa cell lines with different androgenic status (LNCaP and PC-3). The results showed that JPE was able to decrease cell viability in both cell lines. LNCaP showed more sensitivity to JPE exposure, indicating the efficacy of the JPE treatment in terms of androgen responsiveness. JPE showed a distinct hormone dependent effect on the NF-κB signaling, with reduced NF-κB levels for LNCaP and increased NF-κB levels in PC-3 cells. Mechanisms related to cell death by apoptosis were stimulated after the JPE treatment, modulating B-cell lymphoma 2 and BAX for LNCaP and PC-3. Particularly for PC-3, the JPE treatment resulted in cytokine-cytokine receptor interaction activation mostly by up regulating pro-inflammatory, pro-angiogenic, immunostimulatory and immunosuppressive genes. Also, a set of genes related to angiogenesis and metastasis were down-regulated by JPE. In conclusion, JPE exerted an antitumor effect on PCa for both cell lines which can be enhanced if androgenic reliance is considered.