首页> 外文期刊>Journal of Agricultural and Food Chemistry >Pomegranate ellagitannin-derived metabolites inhibit prostate cancer growth and localize to the mouse prostate gland
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Pomegranate ellagitannin-derived metabolites inhibit prostate cancer growth and localize to the mouse prostate gland

机译:石榴来自鞣花单宁的代谢产物可抑制前列腺癌的生长并定位于小鼠前列腺

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Our group has shown in a phase 11 clinical trial that pomegranate juice (PJ) increases prostate specific antigen (PSA) doubling time in prostate cancer (CaP) patients with a rising PSA. Ellagitannins (ETs) are the most abundant polyphenols present in PJ and contribute greatly towards its reported biological properties. On consumption, ETs hydrolyze to release ellagic acid (EA), which is then converted by gut microflora. to 3,8-dihydroxy-6H-dibenzo[b,d]pyran-6-one (urolithin A, UA) derivatives. Despite the accumulating knowledge of ET metabolism in animals and humans, there is no available data on the pharmacokinetics and tissue disposition of urolithins. Using a standardized ET-enriched pomegranate extract (PE), we sought to further define the metabolism and tissue distribution of ET metabolites. PE and UA (synthesized in our laboratory) were administered to C57BL/6 wild-type male mice, and metabolite levels in plasma and tissues were determined over 24 h. ET metabolites were concentrated at higher levels in mouse prostate, colon, and intestinal tissues as compared to other tissues after administration of PE or UA. We also evaluated the effects of PE on CaP growth in severe combined immunodeficient (SCID) mice injected subcutaneously with human CaP cells (LAPC-4). PE significantly inhibited LAPC-4 xenograft growth in SCID mice as compared to vehicle control. Finally, EA and several synthesized urolithins were shown to inhibit the growth of human CaP cells in vitro. The chemopreventive potential of pomegranate ETs and localization of their bioactive metabolites in mouse prostate tissue suggest that pomegranate may play a role in CaP treatment and chemoprevention. This warrants future human tissue bioavailability studies and further clinical studies in men with CaP.
机译:我们的小组在一项11期临床试验中表明,石榴汁(PJ)在PSA升高的前列腺癌(CaP)患者中将前列腺特异性抗原(PSA)的时间增加了一倍。鞣花单宁(ETs)是PJ中含量最丰富的多酚,对报告的生物学特性有很大贡献。食用后,ETs水解释放鞣花酸(EA),然后通过肠道菌群将其转化。 3,8-二羟基-6H-二苯并[b,d]吡喃-6-一(尿石素A,UA)衍生物。尽管在动物和人类中积累了ET代谢的知识,但尚无关于尿石素的药代动力学和组织处置的可用数据。我们使用标准化的富含ET的石榴提取物(PE),试图进一步定义ET代谢物的代谢和组织分布。将PE和UA(在我们的实验室中合成)施用给C57BL / 6野生型雄性小鼠,并在24小时内测定血浆和组织中的代谢物水平。与施用PE或UA后的其他组织相比,小鼠前列腺,结肠和肠组织中的ET代谢产物浓度更高。我们还评估了皮下注射人CaP细胞(LAPC-4)的严重联合免疫缺陷(SCID)小鼠中PE对CaP生长的影响。与载体对照相比,PE显着抑制SCID小鼠中LAPC-4异种移植物的生长。最后,显示了EA和几种合成的尿石素在体外抑制人CaP细胞的生长。石榴ET的化学预防潜力及其生物活性代谢物在小鼠前列腺组织中的定位表明,石榴可能在CaP治疗和化学预防中发挥作用。这保证了将来在CaP男性中进行人体组织生物利用度研究和进一步的临床研究。

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