肿瘤细胞从PARP抑制介导的辐射诱导衰老中恢复。
Tumor Cell Recovery from Senescence Induced by Radiation with PARP Inhibition.
作者信息
Gewirtz David A, Alotaibi Moureq, Yakovlev Vasily A, Povirk Lawrence F
机构信息
Department of a Pharmacology, Toxicology and Medicine and.
c College of Pharmacy, King Saud University, Riyadh 11451, Kingdom of Saudi Arabia.
出版信息
Radiat Res. 2016 Oct;186(4):327-332. doi: 10.1667/RR14437.1. Epub 2016 Sep 2.
Abstract
Inhibitors of poly(ADP-ribose) polymerase (PARP) are clinically used as single-agent therapy for tumors with BRCA1 or BRCA2 mutations. One approach to expanding the use of PARP inhibitors to a wider range of tumors is to combine them with cytotoxic chemotherapy or radiotherapy. Preclinical studies in experimental animals and tumor cells in culture indicate that PARP inhibition modestly sensitizes most tumor cells to ionizing radiation. Studies of cell behavior after these combined treatments show that radiosensitization is manifested predominantly in an increase in prolonged growth arrest and senescence, with little or no contribution from apoptosis. The secretory phenotype associated with senescence can target these tumor cells for immune surveillance, and therefore increased senescence can effectively contribute to tumor control. However, the possible recovery of senescent cells and re-entry into cell cycle after prolonged arrest also needs to be considered. Such recovery could lead to tumor recurrence, yet may not be reflected in short-term assays commonly used to assess radiosensitization.
摘要
聚(ADP - 核糖)聚合酶(PARP)抑制剂在临床上被用作BRCA1或BRCA2基因突变肿瘤的单药治疗。将PARP抑制剂的使用范围扩大到更广泛肿瘤的一种方法是将它们与细胞毒性化疗或放疗联合使用。在实验动物和培养的肿瘤细胞中进行的临床前研究表明,PARP抑制可适度使大多数肿瘤细胞对电离辐射敏感。这些联合治疗后细胞行为的研究表明,放射增敏主要表现为延长的生长停滞和衰老增加,而凋亡的贡献很小或没有。与衰老相关的分泌表型可将这些肿瘤细胞作为免疫监视的目标,因此增加的衰老可有效促进肿瘤控制。然而,也需要考虑衰老细胞在长期停滞后可能恢复并重新进入细胞周期的情况。这种恢复可能导致肿瘤复发,但可能不会在常用于评估放射增敏的短期试验中体现出来。
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2
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3
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