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顺铂对体内外外周血白细胞中DNA的损伤及修复作用

Cisplatin-DNA damage and repair in peripheral blood leukocytes in vivo and in vitro.

作者信息

Dabholkar M, Bradshaw L, Parker R J, Gill I, Bostick-Bruton F, Muggia F M, Reed E

机构信息

Section of Genitourinary Cancer, National Cancer Institute, Bethesda, MD 20892.

出版信息

Environ Health Perspect. 1992 Nov;98:53-9. doi: 10.1289/ehp.929853.

DOI:10.1289/ehp.929853
PMID:1486863
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1519597/
Abstract

We have extended our studies on the relationship between cisplatin/carboplatin-induced DNA damage in readily accessible tissue(s) and clinical response to therapy. Such an approach may assist in the study of cancer drug resistance and in establishing parameters for assessing human populations for sensitivity to DNA damaging agents in the environment. Platinum-DNA adduct levels were measured by atomic absorbance spectrometry. DNA repair capacity was assessed in human T-lymphocytes by the ability to repair cisplatin lesions in cellular DNA or in transfected plasmid DNA. In a "blinded" study of 21 patients receiving combination cisplatin/carboplatin drug therapy, there was a direct relationship between DNA damage in leukocytes and disease response (summary two-sided p = 0.00011). The cohort of patients had 15 different tumor types, suggesting that blood tissue and tumor tissue of an individual may process platinum-DNA damage similarly regardless of the tissue of origin of the tumor. In leukocytes in vivo, persistence and accumulation were prominent features of the cisplatin-DNA adduct profile. Functional DNA repair capacity has been studied in eight human leukocyte cell lines in vitro (three, T-cells; three, B-cells; one, monocytic; one, promyelocytic), using a host cell reactivation assay with cisplatin-damaged pRSVcat. In the three T cell lines studied, host cell reactivation efficiency was directly related to the cells' abilities to repair cisplatin-damaged cellular DNA (correlation coefficient = 0.993).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

我们扩展了关于顺铂/卡铂在易于获取的组织中诱导的DNA损伤与临床治疗反应之间关系的研究。这种方法可能有助于癌症耐药性的研究,并有助于建立评估人群对环境中DNA损伤剂敏感性的参数。通过原子吸收光谱法测量铂-DNA加合物水平。通过修复细胞DNA或转染质粒DNA中顺铂损伤的能力,在人T淋巴细胞中评估DNA修复能力。在一项对21名接受顺铂/卡铂联合药物治疗患者的“盲法”研究中,白细胞中的DNA损伤与疾病反应之间存在直接关系(双侧汇总p = 0.00011)。该患者队列有15种不同的肿瘤类型,这表明个体的血液组织和肿瘤组织处理铂-DNA损伤的方式可能相似,而与肿瘤的组织起源无关。在体内白细胞中,顺铂-DNA加合物谱的突出特征是持续存在和积累。使用顺铂损伤的pRSVcat进行宿主细胞再激活试验,在体外对8种人白细胞细胞系(3种T细胞;3种B细胞;1种单核细胞;1种早幼粒细胞)的功能性DNA修复能力进行了研究。在所研究的3种T细胞系中,宿主细胞再激活效率与细胞修复顺铂损伤的细胞DNA的能力直接相关(相关系数 = 0.993)。(摘要截短于250字)

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