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氨磷汀:一种使正常组织免受放化疗所致毒性的选择性细胞保护剂(综述)

Amifostine: A selective cytoprotective agent of normal tissues from chemo-radiotherapy induced toxicity (Review).

作者信息

Orditura M, De Vita F, Roscigno A, Infusino S, Auriemma A, Iodice P, Ciaramella F, Abbate G, Catalano G

机构信息

Medical Oncology, Department of Clinical and Experimental Medicine <F. Magrassi>, Second University of Naples School of Medicine, C/o II Policlinico, 80131 Naples, Italy.

出版信息

Oncol Rep. 1999 Nov-Dec;6(6):1357-62. doi: 10.3892/or.6.6.1357.

Abstract

Patients receiving systemic cancer chemotherapy must often have their dose intensity of therapeutic agents reduced, because a broad range of organs are adversely affected. Therefore, research and the development of agents protecting the normal tissues from the toxicity of antineoplastic therapy, without reducing the antitumour efficacy, are very important. Amifostine, a prodrug that forms an activated free thiol, when dephosphorylated by alkaline phosphatase, appears selective in its entry in non-malignant cells, and exerts a protective effect from toxicity induced by chemo- or radiotherapy on normal tissues, through free radical scavenging, hydrogen donation and inhibition of DNA damage. Studies in vitro and experimental models have confirmed the protective properties of amifostine in normal cells. In clinical trials pretreatment with amifostine reduced the frequency of cyclophosphamide induced neutropenia and nephro-, oto- and neurotoxicity of platinum compounds. In some cases the use of amifostine have also potentiated the effects of several drugs, such as alkylating agents and, in recent studies, taxanes. The main potentially dose-limiting adverse effect is hypotension, that is often asymptomatic. Amifostine is thus usefully employed in order to obtain a better quality of life in patients receiving oncologic treatments.

摘要

接受全身性癌症化疗的患者常常必须降低其治疗药物的剂量强度,因为多种器官会受到不利影响。因此,研发在不降低抗肿瘤疗效的情况下保护正常组织免受抗肿瘤治疗毒性影响的药物非常重要。氨磷汀是一种前体药物,在被碱性磷酸酶去磷酸化时会形成活化的游离硫醇,它进入非恶性细胞具有选择性,并通过清除自由基、提供氢和抑制DNA损伤,对化疗或放疗诱导的正常组织毒性发挥保护作用。体外研究和实验模型已证实氨磷汀对正常细胞具有保护特性。在临床试验中,氨磷汀预处理降低了环磷酰胺诱导的中性粒细胞减少症的发生率以及铂类化合物的肾毒性、耳毒性和神经毒性。在某些情况下,使用氨磷汀还增强了几种药物的作用,如烷化剂,以及在最近的研究中,紫杉烷类药物。主要的潜在剂量限制性不良反应是低血压,通常无症状。因此,氨磷汀可有效用于改善接受肿瘤治疗患者的生活质量。

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