A study of prevalence of polymorphic variants of genes of blood coagulation factors in onco-logical patients

T. Zykova, L. Vladimirova, O. V. Katelnitskaya, A. Maslov, E. A. Shevyakova, I. Lysenko, N. A. Abramova, A. E. Storozhakova, I. Popova, K. Novoselova, N. Tikhanovskaya, A. Lyanova, L. A. Ryadinskaya, A. V. Tishina, I. Tishchenko, S. N. Kabanov, E. Kalabanova
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Abstract

Aim . To study the prevalence of carriage of polymorphic allele variants of genes of blood coagulation factors in oncological patients. Materials and Methods. 213 Patients with morphologically confirmed oncological diseases were examined. Samples of genomic DNA of peripheral blood of the patients were examined. Using polymerase chain reaction (PCR), polymorphic sites of genes of hemostatic system were studied in real time: F2 (G20210А, rs1799963), F5 (G1691A, rs6025), F7 (G10976A, rs6046), F13 (G226A, rs5985), FGB G(-455)A (rs1800790), ITGA2-α2 (C807T, rs1126643), ITGB3-b (Т1565С, rs5918), PAI-1 4G(-675)5G, rs1799889). Results . The prevalence of carriage of alternative allele of F2 (G20210А) polymorphic locus in the studied group was 1.6%, of F5 (G1691A) – 3.5%, of F7 (G10976A) – 13.4%, of F13 (G226A) – 28.2%, of FGB G(-455)A – 24.9%, of ITGA2-α2 (C807T) – 41.5%, of ITGB3-b (Т1565С) – 15.5%, of PAI-1 4G(-675)5G – 56.6%. A statistically significant increase in the frequency of ‘risk alleles’ of F5 G1691A (р=0.0169), F13 G226A (р=0.0007), FGB G(-455)A (р<0.0001) and ITGA2-α2 C807T (р=0.0201) polymorphic loci was found in oncological patients as compared to the general population. In the same loci, except ITGA2-α2 (C807T), statistically significant differences in the frequency of alternative alleles were found in different localizations of the oncological process. In 92.0% of patients, SNR combination was determined in different components of hemostatic system. Conclusion . Taking into account a high frequency of identification of ‘risk alleles’ in all components of hemostatic system, it is reasonable to carry out additional research to determine the necessity of addition of antiaggregants to antithrombotic therapy in oncological patients.
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肿瘤患者凝血因子基因多态性变异的研究
的目标。目的研究肿瘤患者凝血因子基因多态性等位基因变异的携带情况。材料与方法:对213例经形态学证实的肿瘤患者进行检查。检测患者外周血基因组DNA样本。采用聚合酶链反应(PCR)技术实时检测止血系统基因多态性位点:F2 (G20210А, rs1799963)、F5 (G1691A, rs6025)、F7 (G10976A, rs6046)、F13 (G226A, rss5985)、FGB G(-455)A (rs1800790)、ITGA2-α2 (C807T, rs1126643)、ITGB3-b (Т1565С, rs5918)、PAI-1 4G(-675)5G、rs1799889)。结果。研究群体F2 (G20210А)多态性位点变异等位基因携带率为1.6%,F5 (G1691A) 3.5%, F7 (G10976A) 13.4%, F13 (G226A) 28.2%, FGB G(-455)A 24.9%, ITGA2-α2 (C807T) 41.5%, ITGB3-b (Т1565С) 15.5%, PAI-1 4G(-675)5G 56.6%。与普通人群相比,肿瘤患者F5 G1691A (χ =0.0169)、F13 G226A (χ =0.0007)、FGB G(χ = -455)A (χ = 0.0001)和ITGA2-α2 C807T (χ =0.0201)多态性位点的“风险等位基因”频率有统计学意义的增加。在同一基因座中,除ITGA2-α2 (C807T)外,肿瘤过程中不同部位的替代等位基因频率差异有统计学意义。92.0%的患者在止血系统的不同组分中进行信噪比联合测定。结论。考虑到在止血系统的所有组成部分中识别“风险等位基因”的频率很高,有理由进行额外的研究,以确定肿瘤患者在抗血栓治疗中添加抗聚集剂的必要性。
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