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硬皮病中X染色体失活偏斜

Skewed X-chromosome inactivation in scleroderma.

作者信息

Uz Elif, Loubiere Laurence S, Gadi Vijayakrishna K, Ozbalkan Zeynep, Stewart Jeffrey, Nelson J Lee, Ozcelik Tayfun

机构信息

Department of Molecular Biology and Genetics, Faculty of Science, Bilkent University, Bilkent, Ankara, 06800, Turkey.

出版信息

Clin Rev Allergy Immunol. 2008 Jun;34(3):352-5. doi: 10.1007/s12016-007-8044-z.

Abstract

Scleroderma is a female-prevalent autoimmune disease of unclear etiology. Two fundamental gender differences, skewed X-chromosome inactivation (XCI) and pregnancy-related microchimerism, have been implicated in scleroderma. We investigated the XCI patterns of female scleroderma patients and the parental origin of the inactive X chromosome in those patients having skewed XCI patterns (>80%). In addition, we investigated whether a correlation exists between XCI patterns and microchimerism in a well-characterized cohort. About 195 female scleroderma patients and 160 female controls were analyzed for the androgen receptor locus to assess XCI patterns in the DNA extracted from peripheral blood cells. Skewed XCI was observed in 67 (44.9%) of 149 informative patients and in 10 of 124 healthy controls (8.0%) [odds ratio (OR) = 9.3 (95% confidence interval (CI) 4.3-20.6, P < 0.0001)]. Extremely skewed XCI (>90%) was present in 44 of 149 patients (29.5%) but only in 3 of 124 controls (2.4%; OR = 16.9; 95% CI 4.8-70.4, P < 0.0001). Parental origin of the inactive X chromosome was investigated for ten patients for whom maternal DNA was informative, and the inactive X chromosome was of maternal origin in eight patients and of paternal origin in two patients. Skewed XCI mosaicism could be considered as an important risk factor in scleroderma.

摘要

硬皮病是一种病因不明的女性多发自身免疫性疾病。硬皮病与两个基本的性别差异有关,即X染色体失活(XCI)偏态和妊娠相关微嵌合体。我们研究了女性硬皮病患者的XCI模式以及XCI模式偏态(>80%)患者中失活X染色体的亲本来源。此外,我们在一个特征明确的队列中研究了XCI模式与微嵌合体之间是否存在相关性。对约195名女性硬皮病患者和160名女性对照者的雄激素受体基因座进行分析,以评估从外周血细胞中提取的DNA中的XCI模式。在149名信息充分的患者中有67名(44.9%)观察到XCI偏态,在124名健康对照者中有10名(8.0%)观察到XCI偏态[优势比(OR)=9.3(95%置信区间(CI)4.3 - 20.6,P < 0.0001)]。在149名患者中有44名(29.5%)存在极度偏态的XCI(>90%),但在124名对照者中只有3名(2.4%)存在极度偏态的XCI(OR = 16.9;95% CI 4.8 - 70.4,P < 0.0001)。对10名母亲DNA信息充分的患者进行了失活X染色体的亲本来源研究,其中8名患者的失活X染色体来自母亲,2名患者的失活X染色体来自父亲。XCI偏态嵌合体可被视为硬皮病的一个重要危险因素。

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