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Aspects of vincristine-induced neuropathy in hematologic malignancies: a systematic review

机译:血液学恶性肿瘤中的血管内诱导的神经病变的方面:系统评价

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Purpose Vincristine is widely used as anticancer therapy for a variety of hematological malignancies. The treatment is limited by progressive vincristine-induced neuropathy, possibly including both peripheral sensory and motor nerves, autonomic nervous functions, and the central nervous system. This dose-limiting side-effect can diminish quality of life and, furthermore, cause discontinuation of vincristine treatment. The present review elucidates the current knowledge regarding vincristine-induced neuropathy in hematologic malignancies, focusing on neuropathy assessment, clinical and molecular predictive markers, drug-drug interference, prevention, and treatment. Methods This review is conducted by a systematic search strategy for the identification of relevant literature in the PubMed and Embase databases. Results No clinical parameters displayed convincing potential as predictors of vincristine-induced neuropathy; however, preexisting neuropathy was consistently reported to be associated with an increased risk of neurotoxicity. In contrast, molecular markers, including polymorphisms in genes involved in the pharmacodynamics and pharmacokinetics of vincristine, displayed great potential as predictive markers of neuropathy incidence and severity. Furthermore, antifungal drugs, such as itraconazole and voriconazole, decrease the metabolism of vincristine and consequently lead to severe neuropathy when co-administered with vincristine, underscoring why fluconazole should be the antifungal drug of choice. Conclusion Reports from the 71 included studies clearly emphasize the lack of consistency in neuropathy assessment, grading systems, and reporting, making it difficult to interpret results between studies. Thus, truer clinical and molecular markers could emerge if the consistency of neuropathy detection and reporting increases by the use of conventional standardized neuropathy assessment tools and grading scales.
机译:目的血酮被广泛用作各种血液恶性肿瘤的抗癌治疗。该治疗受进步血管氨酸诱导的神经病变的限制,可能包括外周感官和运动神经,自主神经功能和中枢神经系统。这种剂量限制的副作用可以减少生活质量,而且还会导致血管内处理的停止。本综述阐明了目前关于血液病恶性肿瘤中的血管神经病变的目前的知识,重点是神经病变评估,临床和分子预测标志物,药物干扰,预防和治疗。方法本次审查是通过系统搜索策略进行,用于识别PubMed和Embase数据库中的相关文献。结果无临床参数显示令人信服的潜力,作为血管内诱导的神经病变的预测因子;然而,始终据报道预先存在的神经病变与神经毒性的风险增加有关。相反,分子标记包括参与中文体动力学和药代动力学的基因中的多态性,表现为神经病变发病率和严重程度的预测标志性巨大潜力。此外,抗真菌药物,如伊唑康唑和伏立康唑,减少了长春酮的代谢,因此当与血管内共同施用时导致严重的神经病变,强调为什么氟康唑应该是抗真菌药物的抗真菌药物。结论71所包括的研究报告显然强调了神经病评估,评分系统和报告中缺乏一致性,使得难以解释研究之间的结果。因此,如果通过使用常规的标准化神经病变评估工具和分级尺度,则可以出现如果神经病变检测和报告的一致性增加,则可以出现术临床和分子标记。

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