The possibility of dexrazoxane to prevent ovarian damage caused by toxicity

J. Kropp, D. Abbott, Elon C. Roti Roti
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Abstract

ABSTRACT Dexrazoxane (Dexra), a catalytic topoisomerase II inhibitor and strong chelator, has been safely used in the clinic to decrease cardiotoxicity and extravasation caused by the anthracycline class of chemotherapy agents. Dexra also effectively shields the ovary from doxorubicin (DXR) chemotherapy at a dose 10-fold lower than that clinically approved for cardioprotection, ameliorating concerns that this chemoprotectant may diminish anti-tumor efficacy or increase risk for secondary malignancies. Dexra prevents acute DNA damage caused by DXR in the ovary, prolongs the reproductive lifespan of the adult female mouse post-chemotherapy, and improves offspring health. Cross-application of clinically-approved Dexra pretreatment demonstrates timely drug-based ovoprotection can be clinically implemented to improve quality of life post-cancer.
dexrazoxane预防卵巢毒性损害的可能性
Dexrazoxane (Dexra)是一种催化拓扑异构酶II抑制剂和强螯合剂,已被安全地用于临床,以降低蒽环类化疗药物引起的心脏毒性和外渗。Dexra还有效地保护卵巢免受多柔比星(DXR)化疗的影响,其剂量比临床批准的用于心脏保护的剂量低10倍,减轻了这种化学保护剂可能降低抗肿瘤疗效或增加继发性恶性肿瘤风险的担忧。Dexra可预防DXR引起的卵巢急性DNA损伤,延长化疗后成年雌性小鼠的生殖寿命,改善后代健康。临床批准的Dexra预处理的交叉应用表明,及时的基于药物的卵巢保护可以在临床上实施,以提高癌症后的生活质量。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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