在分子水平上理解前列腺癌雄激素剥夺抗性的机制。
Understanding the mechanisms of androgen deprivation resistance in prostate cancer at the molecular level.
作者信息
Karantanos Theodoros, Evans Christopher P, Tombal Bertrand, Thompson Timothy C, Montironi Rodolfo, Isaacs William B
机构信息
Department of Genitourinary Medical Oncology-Research, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.
Department of Urology, UC Davis Comprehensive Cancer Center, Sacramento, CA, USA.
出版信息
Eur Urol. 2015 Mar;67(3):470-9. doi: 10.1016/j.eururo.2014.09.049. Epub 2014 Oct 8.
CONTEXT
Various molecular mechanisms play a role in the development of resistance to androgen deprivation therapy in castration-resistant prostate cancer (CRPC).
OBJECTIVE
To understand the mechanisms and biological pathways associated with the progression of prostate cancer (PCa) under systemic androgen depletion or administration of the novel antiandrogens abiraterone, enzalutamide, and ARN-509. This review also examines the introduction of novel combinational approaches for patients with CRPC.
EVIDENCE ACQUISITION
PubMed was the data source. Keywords for the search were castrate resistant prostate cancer, abiraterone, enzalutamide resistance mechanisms, resistance to androgen deprivation, AR mutations, amplifications, splice variants, and AR alterations. Papers published before 1990 were excluded from the review, and only English-language papers were included.
EVIDENCE SYNTHESIS
This review summarizes the current literature regarding the mechanisms implicated in the development of CRPC and the acquisition of resistance to novel antiandrogen axis agents. The review focuses on androgen biosynthesis in the tumor microenvironment, androgen receptor (AR) alterations and post-transcriptional modifications, the role of glucocorticoid receptor, and alternative oncogenic signaling that is derepressed on maximum AR inhibition and thus promotes cancer survival and progression.
CONCLUSIONS
The mechanisms implicated in the development of resistance to AR inhibition in PCa are multiple and complex, involving virtually all classes of genomic alteration and leading to a host of selective/adaptive responses. Combinational therapeutic approaches targeting both AR signaling and alternative oncogenic pathways may be reasonable for patients with CRPC.
PATIENT SUMMARY
We looked for mechanisms related to the progression of PCa in patients undergoing hormonal therapy and treatment with novel drugs targeting the AR. Based on recent data, combining maximal AR inhibition with novel agents targeting other tumor-compensatory, non-AR-related pathways may improve the survival and quality of life of patients with castration-resistant PCa.
背景
多种分子机制在去势抵抗性前列腺癌(CRPC)对雄激素剥夺治疗的耐药性发展中起作用。
目的
了解在全身雄激素耗竭或使用新型抗雄激素药物阿比特龙、恩杂鲁胺和ARN-509的情况下,与前列腺癌(PCa)进展相关的机制和生物学途径。本综述还探讨了针对CRPC患者的新型联合治疗方法。
证据获取
以PubMed作为数据来源。搜索关键词为去势抵抗性前列腺癌、阿比特龙、恩杂鲁胺耐药机制、对雄激素剥夺的耐药性、AR突变、扩增、剪接变体和AR改变。1990年以前发表的论文被排除在本综述之外,仅纳入英文论文。
证据综合
本综述总结了当前关于CRPC发生机制以及对新型抗雄激素轴药物耐药性获得的文献。综述重点关注肿瘤微环境中的雄激素生物合成、雄激素受体(AR)改变和转录后修饰、糖皮质激素受体的作用,以及在最大程度抑制AR时被解除抑制从而促进癌症存活和进展的替代致癌信号通路。
结论
PCa中对AR抑制产生耐药性的机制是多样且复杂的,几乎涉及所有类型的基因组改变,并导致一系列选择性/适应性反应。针对AR信号通路和替代致癌途径的联合治疗方法可能对CRPC患者是合理的。
患者总结
我们寻找了接受激素治疗和使用靶向AR的新型药物治疗的PCa患者中与疾病进展相关的机制。基于近期数据,将最大程度的AR抑制与靶向其他肿瘤代偿性、非AR相关途径的新型药物联合使用,可能会改善去势抵抗性PCa患者的生存率和生活质量。
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