Study of relationships between HLA-G gene polymorphism, intrauterine infection and recurrent miscarriage in women

L. Gordeeva, E. Voronina, E. Polenok, S. Mun, S. L. Nersesyan, R. V. Olennikova, M. Filipenko, A. Glushkov
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Abstract

The relationship between the HLA-G gene polymorphism (rs41551813, rs12722477, rs41557518), intrauterine infection and recurrent miscarriage (RM) in women were studied. The case group consisted of 180 patients with RM, defined as two or more consecutive miscarriages (min = 2; max = 8) at up to 20 weeks of gestation, and with clinically confirmed pregnancies and non-viable fetuses. At the time of examination. the women were enrolled from the Genetic Counseling Center at the Kemerovo Regional Clinical Hospital, Kemerovo, Russia, and were not pregnant. Each patient underwent a gynecological examination. We excluded women with a history of medical abortion, birth, and ectopic pregnancies. In addition, we excluded women with endocrine (e.g. diabetes) disorders. To exclude other known causes of spontaneous abortion, the following tests were performed: ultrasound examination of pelvic organs, and karyotyping in women and men. The women’s mean age in the RM group, was 29.6±4.8 (SD) years. The control group comprised 408 fertile women. These women didn’t have a history of spontaneous abortion, or a family history of congenital malformations. They have born, at least, 1-2 healthy children. Women’s mean age at birth of last child was 26.8±5.2 (SD) years. Influence of the intrauterine infection was analyzed on the basis of laboratory tests. Diagnostics of bacterial vaginosis and vulvo-vaginal candidiasis by microscopic examination was conducted. Viral agent infections (herpes simplex virus type 2, cytomegalovirus, human papilloma virus type 16/18), Chlamydia trachomatis, Mycoplasma hominis, Ureaplasma urealyticum, Gardnerella vaginalis and Trichomonas vaginalis were detected by enzyme-linked immunoassay and polymerase chain reaction (PCR). The data were obtained from the medical cards of the surveyed women. All the women gave a written informed consent before participating in the study. Typing of polymorphisms of Thr31Ser (rs41551813, HLA-G*01:03) in exon 2, Leu110Ile (rs12722477, HLA-G*01:04) and 1597 delС (rs41557518, HLA-G*01:05N) in exon 3 HLA-G genes were performed by realtime PCR followed by melting analysis. The study showed that the intrauterine infection was not a risk factor for RM (p = 0.30) in the examined women. It was found that the 110 Ile allele (HLA-G *01:04) was a risk factor for RM both in women with intrauterine infection [ORa = 4.50 (2.41-8.38), p = 2.09e-06], and in women without infection [ORa = 2.46 (1.44-4.21), p = 0.0009]. The cooperative influence of genetic and infections factors with the risk of RM in women was revealed [ORa+f = 3.50 (2.01-6.09), p = 8.78e-06]. Our results will be useful in understanding the molecular mechanisms of immune disorders in fetomaternal interface, and for choosing the strategy of management and treatment in women with RM. 
HLA-G基因多态性与女性宫内感染及复发性流产关系的研究
研究女性HLA-G基因多态性(rs41551813、rs12722477、rs41557518)与宫内感染及复发性流产(RM)的关系。病例组由180例RM患者组成,定义为连续两次或两次以上流产(min = 2;Max = 8),妊娠20周以内,临床证实妊娠且胎儿不能存活。在考试的时候。这些妇女来自俄罗斯克麦罗沃地区临床医院的遗传咨询中心,没有怀孕。每位患者都进行了妇科检查。我们排除了有药物流产、分娩和异位妊娠史的妇女。此外,我们排除了患有内分泌(如糖尿病)疾病的女性。为了排除其他已知的自然流产原因,进行了以下检查:盆腔器官超声检查和男女核型分析。RM组女性的平均年龄为29.6±4.8 (SD)岁。对照组由408名育龄妇女组成。这些妇女没有自然流产史,也没有先天性畸形的家族史。他们至少生了1-2个健康的孩子。产妇最后一胎平均年龄为26.8±5.2 (SD)岁。在实验室检查的基础上,分析了宫内感染的影响。对细菌性阴道病和外阴阴道念珠菌病进行镜检诊断。采用酶联免疫法和聚合酶链反应(PCR)检测单纯疱疹病毒2型、巨细胞病毒、人乳头瘤病毒16/18型、沙眼衣原体、人支原体、解脲原体、阴道加德纳菌和阴道毛滴虫等病毒感染。数据来自被调查妇女的医疗卡。所有女性在参与研究前都有书面的知情同意书。采用实时聚合酶链反应(real - time PCR)和熔解分析方法,对2外显子Thr31Ser (rs41551813, HLA-G*01:03)、3外显子Leu110Ile (rs12722477, HLA-G*01:04)和1597 delС (rs41557518, HLA-G*01:05N)基因多态性进行分型。研究表明,宫内感染不是RM的危险因素(p = 0.30)。发现110 Ile等位基因(HLA-G *01:04)是宫内感染妇女(ORa = 4.50 (2.41-8.38), p = 2.09e-06)和未感染妇女(ORa = 2.46 (1.44-4.21), p = 0.0009)发生RM的危险因素。遗传和感染因素对女性RM风险的共同影响[ORa+f = 3.50 (2.01-6.09), p = 8.78e-06]。我们的研究结果将有助于了解母婴界面免疫紊乱的分子机制,以及选择RM妇女的管理和治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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