Wengler G S, Parolini O, Fiorini M, Mella P, Smith H, Ugazio A G, Notarangelo L D
Department of Pediatrics, University of Brescia, Italy.
Life Sci. 1997;61(14):1405-11. doi: 10.1016/s0024-3205(97)00686-3.
The Wiskott-Aldrich syndrome (WAS), X-linked severe combined immunodeficiency (SCIDX1), and X-linked agammaglobulinemia (XLA) are severe congenital immunodeficiencies with X-linked inheritance. Although rare, they are all associated with severe infections from early in life, and high morbidity and mortality. Female carriers of these diseases can be identified by a non-random pattern of X-chromosomal inactivation in cell lineages targeted by each gene defect. For patients with WAS, SCIDX1 or XLA, the demonstration of non random X-Chromosome inactivation in their mothers can be used to confirm clinical diagnosis. Furthermore, analysis of X-Chromosome inactivation in at risk females allows preconceptional carrier detection, thus representing an important aid in genetic counseling. For each disease we established a PCR-based, non radioactive assay at the human androgen receptor (HUMARA) locus, that allows analysis of X-Chromosome inactivation in the affected cell types and in tissue specific controls to exclude the issue of skewed X-chromosomal inactivation. In our study, 50 females with a known family history of XLA [19], WAS [18], and SCIDX1 [13],were examined. A carrier status was established in 19 females (7 XLA, 6 WAS, 6 SCIDX1) and excluded in 29 ( 11 XLA, 11 WAS, 7 SCIDX1). Only in 2 cases (4%) the assay was not informative.
维斯科特-奥尔德里奇综合征(WAS)、X连锁重症联合免疫缺陷病(SCIDX1)和X连锁无丙种球蛋白血症(XLA)是具有X连锁遗传的严重先天性免疫缺陷病。尽管罕见,但它们都与生命早期的严重感染以及高发病率和高死亡率相关。这些疾病的女性携带者可通过每个基因缺陷所靶向的细胞谱系中X染色体失活的非随机模式来识别。对于患有WAS、SCIDX1或XLA的患者,证明其母亲存在非随机X染色体失活可用于确诊临床诊断。此外,对有风险女性的X染色体失活进行分析可在孕前检测携带者,因此在遗传咨询中是一项重要帮助。对于每种疾病,我们在人类雄激素受体(HUMARA)基因座建立了一种基于PCR的非放射性检测方法,该方法可分析受影响细胞类型和组织特异性对照中的X染色体失活情况,以排除X染色体失活偏斜的问题。在我们的研究中,对50名有已知XLA家族史的女性(19名)、WAS家族史的女性(18名)和SCIDX1家族史的女性(13名)进行了检测。确定19名女性为携带者状态(7名XLA、6名WAS、6名SCIDX1),排除29名女性(11名XLA、11名WAS、7名SCIDX1)。仅在2例(4%)中检测结果无信息价值。
