IL-4 and its polymorphism (IL4-589C/T) in cervical neoplasia

Q4 Medicine
T. Abakumova, I. Myagdieva, D. Dolgova, S. Gening, I. Antoneeva, T. Gening
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引用次数: 0

Abstract

The transition of cervical neoplasia (CIN) to cervical cancer occurs with the active participation of IL-4, for which both pro- and antitumor effects have been shown with tumors of various localizations. The expression of cytokines is regulated at the transcriptional level in the promoter region of the gene. It has been shown that the genotype IL4 (589C/T) (rs2243250) is associated with the development of gastric and breast cancer. The contribution of IL-4 genotypic variations to the development of CIN has not yet been studied. The aim of the study was to assess the risk of developing cervical neoplasia by the presence polymorphism of IL4 (589C/T) and the level of IL-4. The object of the study was circulating neutrophils, serum and genomic DNA of 36 patients with CIN and 20 women without dysplasia (comparison group). Using ELISA, the level of IL-4 was determined in neutrophil lysate and serum. Phagocytic activity and adhesive ability (CD11b) of neutrophils were assessed. Allele-specific real-time PCR using Taq-Man probes was used to analyze of the IL4 589C/T (rs2243250). Statistical processing was carried out using Statistica 13 and Jamovi 1.6.5.0. As a result of the study, it was found that the level of IL-4 in serum and circulating neutrophils in patients with CIN is significantly higher than in the comparison group. The -589C* allele of the IL4 gene and the TT genotype are more common in the group with CIN (55.5%) than in the control (25%). At the same time, a direct relationship was established between the presence of polymorphism and increased adhesive ability and with indicators of the phagocytic number of circulating neutrophils. Analysis of the incidence of IL4 C589T by the «case-control» method showed that the chances of CIN formation in carriers of the -589C allele and the TT genotype were 3.75 (95% CI: 1.013 - 13.880, Chi-square = 4.161, p = 0.042). The -589C* allele and TT IL4 genotype, neutrophil and serum IL-4 levels are associated with HPV infection. Using a binary logistic regression model, we demonstrated the possibility of using IL-4 levels in circulating neutrophils and IL-4 gene polymorphism (589C/T) for the differential diagnosis of patients with CIN (χ2 = 15.6, p = 0.001). Significant significance for their combination was assessed by ROC-curve analysis (IL-4 in neutrophils; IL4 (-589С*), 75% probability. Thus, the IL4 (589C/T) is associated with the adhesive and phagocytic activity of circulating neutrophils. In HPV-infected patients, IL4 gene polymorphism (589C/T) can serve as a marker for early detection and prognosis of CIN.
宫颈肿瘤组织中IL-4及其多态性(IL4-589C/T
宫颈瘤变(cervical neoplasia, CIN)向宫颈癌的转变是在IL-4的积极参与下发生的,IL-4在不同部位的肿瘤中均有促瘤和抗瘤作用。细胞因子的表达在基因启动子区域的转录水平上受到调节。已有研究表明,基因型IL4 (589C/T) (rs2243250)与胃癌和乳腺癌的发生有关。IL-4基因型变异对CIN发展的贡献尚未得到研究。该研究的目的是通过IL-4 (589C/T)多态性和IL-4水平的存在来评估发生宫颈瘤变的风险。研究对象为36例CIN患者和20例非发育不良妇女(对照组)的循环中性粒细胞、血清和基因组DNA。采用ELISA法测定血清和中性粒细胞裂解液中IL-4的水平。观察中性粒细胞的吞噬活性和粘附能力(CD11b)。采用Taq-Man探针对IL4 589C/T (rs2243250)进行等位基因特异性实时PCR分析。采用Statistica 13和Jamovi 1.6.5.0进行统计处理。研究结果发现,CIN患者血清及循环中性粒细胞IL-4水平明显高于对照组。il - 4基因的-589C*等位基因和TT基因型在CIN组(55.5%)比对照组(25%)更常见。同时,多态性的存在与黏附能力的增强以及与循环中性粒细胞吞噬数的指标有直接关系。用“病例对照”方法分析IL4 C589T的发病率,结果显示- 589c等位基因携带者和TT基因型携带者形成CIN的几率为3.75 (95% CI: 1.013 ~ 13.880,卡方= 4.161,p = 0.042)。-589C*等位基因和TT IL-4基因型、中性粒细胞和血清IL-4水平与HPV感染有关。使用二元logistic回归模型,我们证明了使用循环中性粒细胞中IL-4水平和IL-4基因多态性(589C/T)对CIN患者鉴别诊断的可能性(χ2 = 15.6, p = 0.001)。通过roc曲线分析(中性粒细胞IL-4;IL4 (-589С*), 75%概率。因此,il - 4 (589C/T)与循环中性粒细胞的粘附和吞噬活性有关。在hpv感染患者中,il - 4基因多态性(589C/T)可作为CIN早期发现和预后的标志。
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来源期刊
Medical Immunology (Russia)
Medical Immunology (Russia) Medicine-Immunology and Allergy
CiteScore
0.70
自引率
0.00%
发文量
88
审稿时长
12 weeks
期刊介绍: The journal mission is to promote scientific achievements in fundamental and applied immunology to various medical fields, the publication of reviews, lectures, essays by leading domestic and foreign experts in the field of fundamental and experimental immunology, clinical immunology, allergology, immunodiagnostics and immunotherapy of infectious, allergy, autoimmune diseases and cancer.
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