采用高分辨率阵列比较基因组杂交(CGH)技术对21例Wolf-Hirschhorn综合征患者进行基因型-表型相关性研究。
Genotype-phenotype correlation in 21 patients with Wolf-Hirschhorn syndrome using high resolution array comparative genome hybridisation (CGH).
作者信息
Maas N M C, Van Buggenhout G, Hannes F, Thienpont B, Sanlaville D, Kok K, Midro A, Andrieux J, Anderlid B-M, Schoumans J, Hordijk R, Devriendt K, Fryns J-P, Vermeesch J R
机构信息
Center for Human Genetics, University Hospital, Catholic University of Leuven, Leuven, Belgium.
出版信息
J Med Genet. 2008 Feb;45(2):71-80. doi: 10.1136/jmg.2007.052910. Epub 2007 Sep 14.
BACKGROUND
The Wolf-Hirschhorn syndrome (WHS) is usually caused by terminal deletions of the short arm of chromosome 4 and is phenotypically defined by growth and mental retardation, seizures, and specific craniofacial manifestations. Large variation is observed in phenotypic expression of these features. In order to compare the phenotype with the genotype, we localised the breakpoints of the 4 pter aberrations using a chromosome 4 specific tiling BAC/PAC array.
METHODS
In total, DNA from 21 patients was analysed, of which 8 had a cytogenetic visible and 13 a submicroscopic deletion.
RESULTS AND CONCLUSION
In addition to classical terminal deletions sized between 1.9 and 30 Mb, we observed the smallest terminal deletion (1.4 Mb) ever reported in a patient with mild WHS stigmata. In addition, we identified and mapped interstitial deletions in four patients. This study positions the genes causing microcephaly, intrauterine and postnatal growth retardation between 0.3 and 1.4 Mb and further refines the regions causing congenital heart disease, cleft lip and/or palate, oligodontia, and hypospadias.
背景
沃尔夫-赫希霍恩综合征(WHS)通常由4号染色体短臂的末端缺失引起,其表型特征为生长发育迟缓和智力障碍、癫痫发作以及特定的颅面部表现。这些特征的表型表达存在很大差异。为了将表型与基因型进行比较,我们使用4号染色体特异性平铺BAC/PAC阵列定位了4pter畸变的断点。
方法
共分析了21例患者的DNA,其中8例有细胞遗传学可见的缺失,13例有亚显微缺失。
结果与结论
除了经典的大小在1.9至30 Mb之间的末端缺失外,我们还观察到一名有轻度WHS体征的患者报告的最小末端缺失(1.4 Mb)。此外,我们在4例患者中鉴定并定位了中间缺失。本研究将导致小头畸形、宫内和出生后生长发育迟缓的基因定位在0.3至1.4 Mb之间,并进一步细化了导致先天性心脏病、唇裂和/或腭裂、少牙症和尿道下裂的区域。
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