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长期激素治疗诱导的激素抵抗性前列腺癌的辐射反应

The radiation response of hormone-resistant prostate cancer induced by long-term hormone therapy.

作者信息

Wu Chun-Te, Chen Wen-Cheng, Liao Shuen-Kuei, Hsu Cheng-Lung, Lee Kuan-Der, Chen Miao-Fen

机构信息

Department of Urology, Chang Gung Memorial Hospital, Linko, Taiwan.

出版信息

Endocr Relat Cancer. 2007 Sep;14(3):633-43. doi: 10.1677/ERC-07-0073.

Abstract

Hormone therapy for prostate cancer eventually fails leading to a stage called hormone-resistant (HR) disease. To investigate the issue about the characteristics and the radiation response in HR prostate cancer, we established HR cell sub-lines, 22RV1-F and 22RV1-DF, from 22RV1 cells with androgen deprivation for 16 weeks, and obtained LNCaP-HR from LNCaP with long-term bicalutamide treatment. We examined their sensitivities to radiation therapy and the underlying mechanisms. In vitro and in vivo faster tumor growth rate was noted in the HR prostate cancer cells when compared with control. Moreover, HR prostate cancer cells had greater capacity to scavenge reactive oxygen species, and suffered less apoptosis and senescence, and subsequently were more likely to survive from irradiation as measured by clonogenic assay in vitro and growth delay in vivo. The decreased p53 and increased mouse double minute 2 oncogene (MDM2) might be the potential underlying mechanisms for the more aggressive growth and more radioresistance in HR prostate cancer cells. In conclusion, HR prostate cancer cells appeared to be more aggressive in tumor growth and in resistance to radiation treatment. Regulation of the expressions of p53 and MDM2 should be the promising treatment strategies for relative radioresistant prostate cancer.

摘要

前列腺癌的激素疗法最终会失效,导致进入激素抵抗(HR)阶段。为了研究HR前列腺癌的特征及放射反应问题,我们从经16周雄激素剥夺处理的22RV1细胞中建立了HR细胞亚系22RV1-F和22RV1-DF,并通过长期比卡鲁胺治疗从LNCaP细胞中获得了LNCaP-HR。我们检测了它们对放射治疗的敏感性及其潜在机制。与对照组相比,HR前列腺癌细胞在体外和体内均呈现出更快的肿瘤生长速度。此外,HR前列腺癌细胞清除活性氧的能力更强,凋亡和衰老程度更低,随后通过体外克隆形成试验和体内生长延迟测定发现,它们更有可能在照射后存活。p53表达降低和小鼠双微体2癌基因(MDM2)表达增加可能是HR前列腺癌细胞生长更具侵袭性和放射抗性更强的潜在机制。总之,HR前列腺癌细胞在肿瘤生长和放射治疗抵抗方面似乎更具侵袭性。调节p53和MDM2的表达应该是针对相对放射抵抗性前列腺癌的有前景的治疗策略。

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