Association of the VDR gene with clinical manifestations, complications, and vitamin D status in children with juvenile idiopathic arthritis

Q3 Medicine
E. Loshkova, E. Kondratyeva, L. Klimov, N. S. Podchernyaeva, N. Ilyenkova, S. Chebysheva, E. Shitkovskaya, S. Dolbnya, V. A. Kuryaninova, E. Zhekayte, M. I. Tikhaya, Yuliia V. Kotova, Y. Melyanovskaya, M. I. Erokhina, A. Khavkin
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引用次数: 0

Abstract

Objective. To conduct an association search between genetic variants (c.1206T>C, c.152T>C, c.1174+283G>A) of the VDR gene and clinical manifestations of juvenile idiopathic arthritis (JIA), need for genetically engineered biological drugs (GEBDs) and vitamin D status in children. Patients and methods. This study included 150 children (mean age: 9.11 ± 2.21 years) with JIA and 333 healthy controls. The determination of serum calcidiol concentrations was performed in all patients. Polymorphic variants of the VDR gene (c.1206T>C, c.1175-9G>T, c.152T>C, c.1174+283G>A) were tested by polymerase chain reaction (PCR) and restriction fragment length polymorphism (RFLP) technique. Results. Carriers of the minor TT genotype of the genetic variant c.1206T>C(A>G) TaqI are 4 time more likely to develop systemic JIA, 5 time more likely to have high disease activity and uveitis, as well as 9.9 times more often require prescription of GEBDs. Carriers of the minor genotype TT of the genetic variant c.152T>C FokI are 7.7 times more likely to develop systemic JIA and 4.3 times – polyarticular JIA, 6.2 times more likely to have high disease activity and 5.6 times – uveitis, 8 times more often have a severe calcidiol deficiency and 4 times more often require prescription of GEBDs. Carrying the minor AA genotype of the BsmlI polymorphism (c.1174+283G>A) increases the risk of systemic-onset JIA by 17 times, high disease activity and uveitis – by 18 times, and need for GEBDs – by 15 times; carrying the AA and GA genotypes increases the risk of calcidiol deficiency by 5 times and severe calcidiol deficiency by 9 times. Conclusion. All studied genetic variants of the VDR gene verifiably affect the development of clinical manifestations, complications, calcidiol levels and response to therapy in JIA. Key words: VDR gene, juvenile idiopathic arthritis, children, vitamin D, autoimmune disease
VDR基因与幼年特发性关节炎儿童临床表现、并发症和维生素D状况的相关性
目标。研究VDR基因基因变异(C . 1206t >C、C . 152t >C、C .1174+283G>A)与儿童特发性关节炎(JIA)临床表现、基因工程生物药物(gebd)需求及维生素D状况的相关性。患者和方法。本研究纳入150例JIA患儿(平均年龄:9.11±2.21岁)和333例健康对照。所有患者均进行血清钙二醇浓度测定。采用聚合酶链反应(PCR)和限制性片段长度多态性(RFLP)技术检测了VDR基因(C . 1206t >C、C .1175- 9g >T、C . 152t >C、C .1174+283G>A)的多态性变异。结果。遗传变异C . 1206t >C(A>G) TaqI的次要TT基因型携带者发生全身性JIA的可能性是其携带者的4倍,疾病高活动性和葡萄膜炎的可能性是其携带者的5倍,需要处方gebd的可能性是其携带者的9.9倍。遗传变异C . 152t >C . FokI的次要基因型TT携带者发生全身性JIA的可能性是7.7倍,多关节性JIA的可能性是4.3倍,疾病活动性高的可能性是6.2倍,葡萄膜炎的可能性是5.6倍,严重钙二醇缺乏的可能性是8倍,需要处方gebd的可能性是4倍。携带BsmlI多态性的小AA基因型(c.1174+283G>A)使全身性JIA的风险增加17倍,高疾病活动性和葡萄膜炎的风险增加18倍,需要gebd的风险增加15倍;携带AA和GA基因型的人患钙二醇缺乏症的风险增加5倍,严重钙二醇缺乏症的风险增加9倍。结论。所有研究的VDR基因变异均可证实影响JIA的临床表现、并发症、钙二醇水平和治疗反应的发展。关键词:VDR基因,青少年特发性关节炎,儿童,维生素D,自身免疫性疾病
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来源期刊
Voprosy Detskoi Dietologii
Voprosy Detskoi Dietologii Medicine-Pediatrics, Perinatology and Child Health
CiteScore
1.20
自引率
0.00%
发文量
17
期刊介绍: The scientific journal Voprosy Detskoi Dietologii is included in the Scopus database. Publisher country is RU. The main subject areas of published articles are Food Science, Pediatrics, Perinatology, and Child Health, Nutrition and Dietetics, Клиническая медицина.
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