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New Insights in Prostate Cancer Development and Tumor Therapy: Modulation of Nuclear Receptors and the Specific Role of Liver X Receptors

机译:前列腺癌发展和肿瘤治疗的新见解:核受体的调节和肝X受体的特定作用

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摘要

Prostate cancer (PCa) incidence has been dramatically increasing these last years in westernized countries. Though localized PCa is usually treated by radical prostatectomy, androgen deprivation therapy is preferred in locally advanced disease in combination with chemotherapy. Unfortunately, PCa goes into a castration-resistant state in the vast majority of the cases, leading to questions about the molecular mechanisms involving the steroids and their respective nuclear receptors in this relapse. Interestingly, liver X receptors (LXRα/NR1H3 and LXRβ/NR1H2) have emerged as new actors in prostate physiology, beyond their historical roles of cholesterol sensors. More importantly LXRs have been proposed to be good pharmacological targets in PCa. This rational has been based on numerous experiments performed in PCa cell lines and genetic animal models pointing out that using selective liver X receptor modulators (SLiMs) could actually be a good complementary therapy in patients with a castration resistant PCa. Hence, this review is focused on the interaction among the androgen receptors (AR/NR3C4), estrogen receptors (ERα/NR3A1 and ERβ/NR3A2), and LXRs in prostate homeostasis and their putative pharmacological modulations in parallel to the patients’ support.
机译:近年来,在西方国家,前列腺癌(PCa)的发病率急剧上升。尽管局部PCa通常通过根治性前列腺切除术来治疗,但是雄激素剥夺疗法在局部晚期疾病与化学疗法联合治疗中更可取。不幸的是,在大多数情况下,PCa进入去势抵抗状态,这引发了有关这种复发中涉及类固醇及其各自核受体的分子机制的问题。有趣的是,肝脏X受体(LXRα/ NR1H3和LXRβ/ NR1H2)已成为前列腺生理学的新角色,超越了胆固醇传感器的历史地位。更重要的是,已提出LXR在PCa中是良好的药理学靶标。这种合理性基于在PCa细胞系和遗传动物模型中进行的大量实验,指出使用选择性肝X受体调节剂(SLiMs)实际上可能是去势抵抗性PCa患者的良好补充疗法。因此,本综述着眼于前列腺稳态中雄激素受体(AR / NR3C4),雌激素受体(ERα/ NR3A1和ERβ/ NR3A2)和LXR之间的相互作用,以及与患者支持平行的推定药理作用。

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