Association of Inherited Genotype and Severity of Clinical Presentation in Subjects with Verified Pas III Disorder.

Vanja Karlovic Beslic, Azra Burekovic, Zahida Drace, Zelija Velija-Asimi, Amela Dizdarevic-Bostandzic
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Abstract

Background: Polyglandular autoimmune syndrome type III (PAS III) is combination two most common autoimmune disease: Diabetes mellytus type 1 (DM1) and autoimmune thyroid disease (AITD).

Objectives: The aims of the study were a) to define conection between polymorphism of CTLA-4 gene, rs 231775 with PAS III; b) to establish the conection of inherited genotype with severity of clinical features; and c) to estimate the rate of risk for severe clinical presentation among subgroups in study population.

Methods: This research included 50 subjects with diagnosed PAS III syndrome, wich are on treatment in clinic for Nuclear medicine and andocrinology KCUS. As methods of research has used: hystory of disesase AND clinical examination. As material is used blood sample. From blood sample DNA was isolated withn Qiamp- DNA-mini kit, with accopanied protocol.

Results: In our study, 50 patients with polyglandular autoimmune syndrome type III (PAS III) were examined, and in the study population had 26 female subjects and 24 male subjects. The average age of the participants was 31.64 years, and in the subgroups: group GWT (G-wild type) the average age was 30.20 years, group GM (G-mutated) 32.40 years and group GH (G-heterozygote) 30 , 60 years. Using the Chi-square test, the association between the polymorphism rs231775 and PAS-III was demonstrated, x2 (2.100) = 18.258, where p < 0.0001. Using the Chi-square test, the association between the rs231775 polymorphism and the severity of the clinical picture, x2 (2.50) = 8.531, where p< 0.0140 was proved. The CTLA-4 rs231775 genotypes were also assessed for disease severity.

Conclusion: This study suggests that CTLA-4 expression plays a key role in balancing the immune system as well as the response against one's own tissues, and thus in the regulation of autoimmune diseases.

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遗传基因型与临床表现严重程度的相关性研究
背景:多腺体自身免疫性综合征III型(PAS III)是两种最常见的自身免疫性疾病:糖尿病1型(DM1)和自身免疫性甲状腺疾病(AITD)的合并。目的:研究CTLA-4基因rs231775多态性与PAS III的关系;B)建立遗传基因型与临床特征严重程度的关系;c)估计研究人群中亚组出现严重临床表现的风险率。方法:本研究纳入50例在核医学和内分泌科临床治疗的经诊断为PAS III型综合征的患者。研究方法常用:病史和临床检查。作为材料使用的是血液样本。在Qiamp- DNA-mini试剂盒中分离血样中的DNA,并遵循相应的规程。结果:在我们的研究中,检查了50例多腺体自身免疫综合征III型(PAS III)患者,研究人群中有26例女性和24例男性。平均年龄31.64岁,其中GWT (g -野生型)组平均年龄30.20岁,GM (g -突变)组平均年龄32.40岁,GH (g -杂合子)组平均年龄30,60岁。采用卡方检验,证实rs231775多态性与PAS-III存在相关性,x2(2.100) = 18.258,其中p < 0.0001。采用卡方检验,证实rs231775多态性与临床症状严重程度相关,x2(2.50) = 8.531,其中p< 0.0140。还评估了CTLA-4 rs231775基因型的疾病严重程度。结论:本研究提示CTLA-4的表达在平衡免疫系统和对自身组织的反应中起关键作用,从而调节自身免疫性疾病。
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