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卡瓦成分下调 AR 和 AR 剪接变异体的表达,并减少小鼠来源的前列腺癌异种移植瘤的生长。

Kava components down-regulate expression of AR and AR splice variants and reduce growth in patient-derived prostate cancer xenografts in mice.

机构信息

Department of Urology, University of California Irvine, Orange, California, United States of America.

出版信息

PLoS One. 2012;7(2):e31213. doi: 10.1371/journal.pone.0031213. Epub 2012 Feb 9.

Abstract

Men living in Fiji and drinking kava have low incidence of prostate cancer (PCa). However, the PCa incidence among Fijian men who had migrated to Australia, increased by 5.1-fold. We therefore examined the potential effects of kava root extracts and its active components (kavalactones and flavokawains) on PCa growth and androgen receptor (AR) expression. PCa cell lines (LNCaP, LAPC-4, 22Rv1, C4-2B, DU145 and PC-3) with different AR expression, and a transformed prostate myofibroblast cell line (WPMY-1), were treated with a commercial kava extract, kavalactones (kawain, 5'6'-dehydrokawain, yangonin, methysticin) and flavokawain B. Expression of AR and its target genes (PSA and TMPRSS2) was examined. Two novel patient-derived PCa xenograft models from high grade PCa specimens were established by implanting the specimens into nude mice and passing tumor pieces through subcutaneous injection in nude mice, and then treated with kava extract and flavokawain B to examine their effects on tumor growth, AR expression and serum PSA levels. The kava extract and flavokawain B effectively down-regulated the expression of both the full-length AR and AR splice variants. The kava extract and kavalactones accelerated AR protein degradation, while flavokawain B inhibited AR mRNA transcription via decreasing Sp1 expression and the binding of Sp1 to the AR promoter. The kava root extract and flavokawain B reduce tumor growth, AR expression in tumor tissues and levels of serum PSA in the patient-derived PCa xenograft models. These results suggest a potential usefulness of a safe kava product or its active components for prevention and treatment of advanced PCa by targeting AR.

摘要

斐济男性饮用卡瓦根可降低前列腺癌(PCa)的发病率。然而,移居澳大利亚的斐济男性的 PCa 发病率增加了 5.1 倍。因此,我们研究了卡瓦根提取物及其活性成分(卡瓦酮和黄烷酮)对 PCa 生长和雄激素受体(AR)表达的潜在影响。使用商业卡瓦提取物、卡瓦酮(kawain、5'6'-去氢卡瓦酮、yangonin、methysticin)和黄烷酮 B 处理具有不同 AR 表达的 PCa 细胞系(LNCaP、LAPC-4、22Rv1、C4-2B、DU145 和 PC-3)和转化的前列腺成纤维细胞系(WPMY-1),检测 AR 及其靶基因(PSA 和 TMPRSS2)的表达。通过将标本植入裸鼠并通过裸鼠皮下注射传递肿瘤块,建立了来自高等级 PCa 标本的两个新的患者衍生的 PCa 异种移植模型,然后用卡瓦提取物和黄烷酮 B 处理,以检查它们对肿瘤生长、AR 表达和血清 PSA 水平的影响。卡瓦提取物和黄烷酮 B 有效下调全长 AR 和 AR 剪接变体的表达。卡瓦提取物和卡瓦酮加速 AR 蛋白降解,而黄烷酮 B 通过降低 Sp1 表达和 Sp1 与 AR 启动子的结合来抑制 AR mRNA 转录。卡瓦根提取物和黄烷酮 B 减少肿瘤生长、肿瘤组织中 AR 表达和患者衍生的 PCa 异种移植模型中的血清 PSA 水平。这些结果表明,安全的卡瓦产品或其活性成分通过靶向 AR 用于预防和治疗晚期 PCa 具有潜在的用途。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ea1b/3276576/2226255c0c16/pone.0031213.g001.jpg

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