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首页> 外文期刊>The International journal of biological markers >The Impact of CDA A79C Gene Polymorphisms on the Response and Hematologic Toxicity in Gemcitabine-Treated Patients: A Meta-Analysis
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The Impact of CDA A79C Gene Polymorphisms on the Response and Hematologic Toxicity in Gemcitabine-Treated Patients: A Meta-Analysis

机译:CDA A79C基因多态性对吉西他滨治疗患者的反应和血液学毒性的影响:一项荟萃分析

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摘要

To investigate the impact of the cytidine deaminase (CDA) A79C polymorphism on both the response to gemcitabine in non-small cell lung cancer (NSCLC) patients and the risk of hematologic toxicities in patients bearing any kind of cancer taking gemcitabine. The PubMed and Embase databases were searched from the first available article to January 2013. Eligible studies included clinical trials that contained the keywords “gemcitabine” or “cytidine deaminase” and information about response rate of NSCLC patients or hematologic toxicities in patients with any kind of cancer. Relative risk (RR) of different genotypes and 95% confidence intervals (CI) were calculated. A total of 7 articles (623 patients from 6 studies) were included. The results showed that patients with wild type CDA (AA and AC) had a significantly lower rate of severe anemia than the homozygote mutant type CC (RR=0.308; 95%CI, 0.113-0.021, p=0.021). However, the rate of severe neutropenia, thrombocytopenia, and the response rate were identical between different CDA genotypes. The A79C CDA polymorphism did not show a significant impact on the response rate to gemcitabine in NSCLC patients, while the wild type CDA genotype was indeed correlated to a lower rate of incidence of severe anemia in patients taking gemcitabine.
机译:为了研究胞苷脱氨酶(CDA)A79C多态性对非小细胞肺癌(NSCLC)患者对吉西他滨反应的影响以及患有吉西他滨的任何癌症患者的血液学毒性风险。从第一篇可用文章到2013年1月,检索PubMed和Embase数据库。符合条件的研究包括包含关键词“吉西他滨”或“胞苷脱氨酶”的临床试验以及关于NSCLC患者的反应率或任何类型的患者血液学毒性的信息。癌症。计算了不同基因型的相对风险(RR)和95%置信区间(CI)。共纳入7篇文章(来自6项研究的623例患者)。结果表明,野生型CDA(AA和AC)患者的严重贫血发生率明显低于纯合突变体CC型(RR = 0.308; 95%CI,0.113-0.021,p = 0.021)。但是,不同CDA基因型之间的严重中性粒细胞减少症,血小板减少症的发生率和反应率相同。 A79C CDA多态性对NSCLC患者的吉西他滨缓解率没有显着影响,而野生型CDA基因型确实与服用吉西他滨的严重贫血发生率较低相关。

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