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评估一氧化氮供体对各种卵巢癌细胞系顺铂耐药性的影响。

Evaluation of nitric oxide donors impact on cisplatin resistance in various ovarian cancer cell lines.

作者信息

Kielbik Michal, Szulc-Kielbik Izabela, Nowak Marek, Sulowska Zofia, Klink Magdalena

机构信息

Institute of Medical Biology, Polish Academy of Sciences, Lodz, Poland.

Department of Gynecology and Gynecologic Oncology, Polish Mother's Memorial Hospital-Research Institute, Lodz, Poland.

出版信息

Toxicol In Vitro. 2016 Oct;36:26-37. doi: 10.1016/j.tiv.2016.07.005. Epub 2016 Jul 15.

Abstract

Ovarian cancer chemoresistance, both intrinsic and acquired, is the main obstacle in improving the outcome of anticancer therapies. Therefore the development of new treatment strategies, including the use of new compounds that can support the standard therapeutics is required. Among many candidates, nitric oxide (NO) donors, agents with multivalent targeted activities in cancer cells, are worth considering. The aim of this study was evaluation of SPER/NO and DETA/NO ability to enhance cisplatin cytotoxicity against different ovarian cancer cell lines. Obtained data indicate that NO donors action varies between different cancer cell lines and is strongest in low aggressive and cisplatin sensitive cells. While statistically significant, the enhancement of cisplatin cytotoxicity by NO donors is of low magnitude. The rise in the percentage of late apoptotic/necrotic ovarian cancer cells may suggest that NO donors enhancement action might be based on the cellular ATP depletion. Nevertheless, no significant impact of the NO donors, cisplatin or their combination on the expressions of ABCB1, BIRC5 and PTEN genes has been found. Although our data puts the therapeutical potential of NO donors to aid cisplatin action in question it may also point out at the further approach to utilize these compounds in therapies.

摘要

卵巢癌的化疗耐药性,包括内在耐药性和获得性耐药性,是改善抗癌治疗效果的主要障碍。因此,需要开发新的治疗策略,包括使用能够辅助标准疗法的新化合物。在众多候选物中,一氧化氮(NO)供体,这类在癌细胞中具有多价靶向活性的试剂,值得考虑。本研究的目的是评估SPER/NO和DETA/NO增强顺铂对不同卵巢癌细胞系细胞毒性的能力。获得的数据表明,NO供体的作用在不同癌细胞系之间存在差异,在低侵袭性和顺铂敏感细胞中作用最强。虽然具有统计学意义,但NO供体对顺铂细胞毒性的增强幅度较小。晚期凋亡/坏死卵巢癌细胞百分比的增加可能表明,NO供体的增强作用可能基于细胞内ATP的消耗。然而,未发现NO供体、顺铂或它们的组合对ABCB1、BIRC5和PTEN基因的表达有显著影响。尽管我们的数据对NO供体辅助顺铂作用的治疗潜力提出了质疑,但也可能指出了在治疗中利用这些化合物的进一步方法。

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