米内利德通过降低雄激素受体全长及剪接变体的表达来抑制雄激素依赖性、去势抵抗性前列腺癌的生长。
Minnelide Inhibits Androgen Dependent, Castration Resistant Prostate Cancer Growth by Decreasing Expression of Androgen Receptor Full Length and Splice Variants.
作者信息
Isharwal Sumit, Modi Shrey, Arora Nivedita, Uhlrich Charles, Giri Bhuwan, Barlass Usman, Soubra Ayman, Chugh Rohit, Dehm Scott M, Dudeja Vikas, Saluja Ashok, Banerjee Sulagna, Konety Badrinath
机构信息
Department of Urology, Institute for Prostate and Urologic Cancers, University of Minnesota, Minneapolis, Minnesota.
Department of Surgery, University of Minnesota, Minneapolis, Minnesota.
出版信息
Prostate. 2017 May;77(6):584-596. doi: 10.1002/pros.23298. Epub 2017 Feb 1.
BACKGROUND
With almost 30,000 deaths per year, prostate cancer is the second-leading cause of cancer-related death in men. Androgen Deprivation Therapy (ADT) has been the corner stone of prostate cancer treatment for decades. However, despite an initial response of prostate cancer to ADT, this eventually fails and the tumors recur, resulting in Castration Resistant Prostate Cancer (CRPC). Triptolide, a diterpene triepoxide, has been tested for its anti-tumor properties in a number of cancers for over a decade. Owing to its poor solubility in aqueous medium, its clinical application had been limited. To circumvent this problem, we have synthesized a water-soluble pro-drug of triptolide, Minnelide, that is currently being evaluated in a Phase 1 clinical trial against gastrointestinal tumors. In the current study, we assessed the therapeutic potential of Minnelide and its active compound triptolide against androgen dependent prostate cancer both in vitro as well as in vivo.
METHODS
Cell viability was measured by a MTT based assay after treating prostate cancer cells with multiple doses of triptolide. Apoptotic cell death was measured using a caspase 3/7 activity. Androgen Receptor (AR) promoter-binding activity was evaluated by using luciferase reporter assay. For evaluating the effect in vivo, 22Rv1 cells were implanted subcutaneously in animals, following which, treatment was started with 0.21 mg/kg Minnelide.
RESULTS
Our study showed that treatment with triptolide induced apoptotic cell death in CRPC cells. Triptolide treatment inhibited AR transcriptional activity and decreased the expression of AR and its splice variants both at the mRNA and the protein level. Our studies show that triptolide inhibits nuclear translocation of Sp1, resulting in its decreased transcriptional activity leading to downregulation of AR and its splice variants in prostate cancer cells. In vivo, Minnelide (0.21 mg/kg) regressed subcutaneous tumors derived from CRPC 22RV1 at our study endpoint. Our animal studies further confirmed that Minnelide was more efficacious than the standard of care therapies, Docetaxel and Enzalutamide.
CONCLUSION
Our study indicates that Minnelide is very effective as a therapeutic option against CRPC at a dose that is currently tolerated by patients in the ongoing clinical trials. Prostate 77: 584-596, 2017. © 2017 Wiley Periodicals, Inc.
背景
前列腺癌是男性癌症相关死亡的第二大原因,每年导致近30000人死亡。几十年来,雄激素剥夺疗法(ADT)一直是前列腺癌治疗的基石。然而,尽管前列腺癌对ADT最初有反应,但最终会失效,肿瘤复发,导致去势抵抗性前列腺癌(CRPC)。雷公藤内酯醇是一种二萜三环氧化物,十多年来一直在多种癌症中测试其抗肿瘤特性。由于其在水性介质中的溶解度差,其临床应用受到限制。为了解决这个问题,我们合成了雷公藤内酯醇的水溶性前药米内立德,目前正在针对胃肠道肿瘤的1期临床试验中进行评估。在本研究中,我们评估了米内立德及其活性化合物雷公藤内酯醇在体外和体内对雄激素依赖性前列腺癌的治疗潜力。
方法
用多剂量雷公藤内酯醇处理前列腺癌细胞后,通过基于MTT的试验测量细胞活力。使用半胱天冬酶3/7活性测量凋亡细胞死亡。通过荧光素酶报告基因试验评估雄激素受体(AR)启动子结合活性。为了评估体内效果,将22Rv1细胞皮下植入动物体内,然后开始用0.21mg/kg米内立德进行治疗。
结果
我们的研究表明,雷公藤内酯醇处理可诱导CRPC细胞凋亡。雷公藤内酯醇处理抑制AR转录活性,并在mRNA和蛋白质水平上降低AR及其剪接变体的表达。我们的研究表明,雷公藤内酯醇抑制Sp1的核转位,导致其转录活性降低,从而导致前列腺癌细胞中AR及其剪接变体的下调。在体内,在我们的研究终点,米内立德(0.21mg/kg)使源自CRPC 22RV1的皮下肿瘤消退。我们的动物研究进一步证实,米内立德比标准护理疗法多西他赛和恩杂鲁胺更有效。
结论
我们的研究表明,米内立德作为一种治疗CRPC的选择非常有效,其剂量是目前正在进行的临床试验中患者能够耐受的。《前列腺》77:584 - 596,2017。©2017威利期刊公司。
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