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萝卜硫素联合维生素 D 通过调节 JNK/MAPK 通路诱导氧化应激、DNA 损伤、自噬诱导人前列腺癌细胞的细胞毒性。

Sulforaphane Combined with Vitamin D Induces Cytotoxicity Mediated by Oxidative Stress, DNA Damage, Autophagy, and JNK/MAPK Pathway Modulation in Human Prostate Tumor Cells.

机构信息

Department of Genetics, Ribeirão Preto School of Medicine, University of São Paulo-USP, Ribeirão Preto 14049-900, SP, Brazil.

Department of Clinical Analysis, Toxicology, and Food Sciences, Ribeirão Preto School of Pharmaceutical Sciences, University of São Paulo-USP, Ribeirão Preto 14040-903, SP, Brazil.

出版信息

Nutrients. 2023 Jun 14;15(12):2742. doi: 10.3390/nu15122742.

DOI:10.3390/nu15122742
PMID:37375646
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10302480/
Abstract

Prostate cancer ranks second in incidence worldwide. To date, there are no available therapies to effectively treat advanced and metastatic prostate cancer. Sulforaphane and vitamin D alone are promising anticancer agents in vitro and in vivo, but their low bioavailability has limited their effects in clinical trials. The present study examined whether sulforaphane combined with vitamin D at clinically relevant concentrations improved the cytotoxicity of the compounds alone towards DU145 and PC-3 human prostate tumor cells. To assess the anticancer activity of this combination, we analyzed cell viability (MTT assay), oxidative stress (CM-HDCFDA), autophagy (fluorescence), DNA damage (comet assay), and protein expression (Western blot). The sulforaphane-vitamin D combination (i) decreased cell viability, induced oxidative stress, DNA damage, and autophagy, upregulated BAX, CASP8, CASP3, JNK, and NRF2 expression, and downregulated BCL2 expression in DU145 cells; and (ii) decreased cell viability, increased autophagy and oxidative stress, upregulated BAX and NRF2 expression, and downregulated JNK, CASP8, and BCL2 expression in PC-3 cells. Therefore, sulforaphane and vitamin D in combination have a potential application in prostate cancer therapy, and act to modulate the JNK/MAPK signaling pathway.

摘要

前列腺癌在全球发病率中排名第二。迄今为止,还没有有效的疗法可以有效治疗晚期和转移性前列腺癌。在体外和体内,萝卜硫素和维生素 D 单独作为有前途的抗癌剂,但它们的生物利用度低,限制了它们在临床试验中的效果。本研究探讨了萝卜硫素和维生素 D 以临床相关浓度联合使用是否能提高化合物单独对 DU145 和 PC-3 人前列腺肿瘤细胞的细胞毒性。为了评估这种联合的抗癌活性,我们分析了细胞活力(MTT 测定)、氧化应激(CM-HDCFDA)、自噬(荧光)、DNA 损伤(彗星试验)和蛋白质表达(Western blot)。萝卜硫素-维生素 D 联合(i)降低了 DU145 细胞的活力,诱导了氧化应激、DNA 损伤和自噬,上调了 BAX、CASP8、CASP3、JNK 和 NRF2 的表达,下调了 BCL2 的表达;(ii)降低了 PC-3 细胞的活力,增加了自噬和氧化应激,上调了 BAX 和 NRF2 的表达,下调了 JNK、CASP8 和 BCL2 的表达。因此,萝卜硫素和维生素 D 的联合应用具有治疗前列腺癌的潜力,并作用于调节 JNK/MAPK 信号通路。

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