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Factor V Leiden, Prothrombin G20210A, and MTHFR C677T Polymorphisms in Cancer Patients with Venous Thromboembolism

机译:患有静脉血栓栓塞的癌症患者中的因子V Leiden,凝血酶原G20210A和MTHFR C677T多态性

摘要

Intro/Aims: Venous thromboembolism (VTE) is a common complication in cancer patients. The role of thrombophilic polymorphisms in cancer related VTE remains poorly explored. Aim 1 of this study was to determine if Factor V Leiden (G1691A), Prothrombin (PT) G20210A or methylenetetrahydrofolate reductase (MTHFR) C677T are associated with the increased occurrence of VTE in adult oncology subjects compared to nononcology subjects. Aim 2 of this study was to determine if cancer patients with the MTHFR C677T polymorphism who are treated with antimetabolite therapy have an increased incidence of VTE compared to cancer patients who are treated with other chemotherapy.Setting/Methods: A descriptive, comparative, retrospective chart analysis was utilized for this study in an outpatient hematology, oncology clinic in Southern Arizona. Enrolled were 100 adult subjects (age 18 - 85) with documented history of VTE (27 subjects with cancer and 73 noncancer). Subjects were evaluated for Factor V Leiden, PT G20210A, and MTHFR C677T prior to the study. Eleven subjects were treated with antimetabolite chemotherapy and 8 subjects were treated with other chemotherapy.Results: The overall polymorphism frequency for Factor V Leiden was 21%, PT G20210A 4%, and MTHFR C677T 50%. Factor V Leiden was found in 11.1% of cancer subjects and 24.7% of noncancer subjects. Prothrombin G20210A was found in 3.7% of cancer subjects and 4.1% of noncancer subjects. MTHFR C677T was present in 25.9% of cancer subjects and 58.9% of noncancer subjects. No statistical significance was observed between subjects treated with an antimetabolite and positive for MTHFR C677T compared with those treated with other types of chemotherapy.Conclusion: Analysis of the data collected in this study demonstrated overall higher rates than the expected frequencies of all polymorphism for both the cancer and noncancer patients with documented VTE. In this small retrospective study, the only significant finding was that the MTHFR C677T polymorphism was more prevalent in the noncancer group.Currently, there are no specific guidelines for VTE prevention in the outpatient oncology setting. Identification of risk factors, including prothrombotic mutations may reduce risk of VTE and provide guidance for prophylactic treatment recommendations in the outpatient setting.
机译:简介/目的:静脉血栓栓塞症(VTE)是癌症患者的常见并发症。血栓形成的多态性在癌症相关的VTE中的作用仍未得到很好的研究。这项研究的目的1是确定与非肿瘤科目相比,成年肿瘤科目中VTE发生率升高与凝血因子V莱顿(G1691A),凝血酶原(PT)G20210A或亚甲基四氢叶酸还原酶(MTHFR)C677T是否相关。本研究的目的2是确定与其他化学疗法治疗的癌症患者相比,接受抗代谢药物治疗的MTHFR C677T基因多态性癌症患者的VTE发生率是否增加。背景/方法:描述性,比较性,回顾性图表本研究在亚利桑那州南部的一家门诊血液学,肿瘤学诊所进行了分析。入选了100名具有VTE病史的成人受试者(18-85岁)(27名癌症患者和73名非癌患者)。在研究之前,对受试者进行因子V Leiden,PT G20210A和MTHFR C677T的评估。结果:因子V Leiden的多态性总频率为21%,PT G20210A为4%,MTHFR C677T为50%。在11.1%的癌症受试者和24.7%的非癌症受试者中发现了因子V莱顿。在3.7%的癌症受试者和4.1%的非癌症受试者中发现了凝血酶原G20210A。 MTHFR C677T存在于25.9%的癌症受试者和58.9%的非癌症受试者中。与其他类型的化学疗法治疗的受试者相比,抗代谢物治疗且MTHFR C677T阳性的受试者之间没有统计学意义。结论:本研究收集的数据分析表明,总体而言,所有受试者的多态性率均高于预期的所有多态性频率有记录的VTE的癌症和非癌患者。在这项小型回顾性研究中,唯一的重要发现是MTHFR C677T多态性在非癌组中更为普遍。目前,在门诊肿瘤科中尚无针对VTE预防的具体指南。识别包括血栓前突变在内的危险因素可以降低VTE的风险,并为门诊患者的预防性治疗建议提供指导。

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    Lattimore Lois Eileen;

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  • 年度 2010
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