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一名患有X染色体失活偏倚的女性的威斯科特-奥尔德里奇综合征。

Wiskott-Aldrich syndrome in a female with skewed X-chromosome inactivation.

作者信息

Andreu Nuria, Pujol-Moix Núria, Martinez-Lostao Luis, Oset Marta, Muñiz-Diaz Eduardo, Estivill Xavier, Volpini Victor, Fillat Cristina

机构信息

Programa Gens i malaltia, Centre de Regulació Genòmica, Passeig Marítim 37-49, Barcelona 08003, Spain.

出版信息

Blood Cells Mol Dis. 2003 Nov-Dec;31(3):332-7. doi: 10.1016/s1079-9796(03)00168-2.

Abstract

Wiskott-Aldrich syndrome (WAS) is an X-linked recessive disorder characterized by immunodeficiency, eczema, and thrombocytopenia with small platelets. The phenotype of affected males is usually severe, although female carriers of the disorder have no clinical signs of the genetic defect. This is explained by the preferential selection of the normal, nonmutated X-chromosome, as the active allele in hematopoietic cells. In the present article we describe a female case of WAS, with a G-to-A transition in the WASP gene at nucleotide 291. She displays mild thrombocytopenia, with both normal and small-sized platelets. A methylation analysis of the HUMARA gene showed a nonrandom X-chromosome inactivation pattern in which the X-chromosome carrying the normal WASP gene was preferentially inactivated, leaving the mutant gene active. Thus, our results suggest that skewed X-inactivation, favoring the WASP-mutated allele, is the mechanism underlying the WAS phenotype of this girl. Moreover the results alert us to the fact that particular females, with a family history of WAS, may develop certain signs of the disease.

摘要

威斯科特-奥尔德里奇综合征(WAS)是一种X连锁隐性疾病,其特征为免疫缺陷、湿疹以及血小板减少伴小血小板。受影响男性的表型通常较为严重,尽管该疾病的女性携带者没有该基因缺陷的临床症状。这是由于在造血细胞中,正常的、未突变的X染色体作为活性等位基因被优先选择。在本文中,我们描述了一例WAS女性病例,其WASP基因第291位核苷酸发生了G到A的转换。她表现出轻度血小板减少,同时存在正常大小和小尺寸的血小板。对HUMARA基因的甲基化分析显示出一种非随机的X染色体失活模式,其中携带正常WASP基因的X染色体被优先失活,而突变基因保持活性。因此,我们的结果表明,偏向于WASP突变等位基因的X染色体失活是该女孩WAS表型的潜在机制。此外,这些结果提醒我们,有WAS家族病史的特定女性可能会出现该疾病的某些症状。

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