Brkanac Z, Cody J D, Leach R J, DuPont B R
Department of Cellular Biology, University of Texas Health Science Center at San Antonio, San Antonio, TX 78284, USA.
Am J Hum Genet. 1998 Jun;62(6):1500-6. doi: 10.1086/301854.
The majority of patients with 18q- syndrome appear cytogenetically to have a terminal deletion of the long arm of chromosome 18. These 18q- patients are diagnosed by use of standard cytogenetic banding techniques, which have resolution insufficient for precise genotyping. In our effort to obtain a thorough genotype, we have analyzed the DNA from 35 patients who originally were diagnosed as having de novo terminal deletions of chromosome 18. Molecular analysis was performed with polymorphic markers throughout the 18q- region. Cytogenetic FISH was performed with two human 18q telomeric probes, a chromosome 18-specific alpha-satellite probe, and whole chromosome 18-specific paint. Of 35 patients previously reported to have terminal deletions of 18q, we found that 5 (14%) have more-complex cryptic rearrangements and that 3 (9%) retain the most distal portion of 18q, consistent with an interstitial rather than a terminal deletion. These findings indicate that a standard karyotype can lead to insufficient characterization in 18q- syndrome. This has important ramifications for phenotype mapping of this syndrome, as well as for proper prognosis.
大多数18q-综合征患者在细胞遗传学上表现为18号染色体长臂的末端缺失。这些18q-患者通过使用标准细胞遗传学显带技术进行诊断,但其分辨率不足以进行精确的基因分型。为了获得全面的基因型,我们分析了35例最初被诊断为新发18号染色体末端缺失患者的DNA。在整个18q-区域使用多态性标记进行分子分析。使用两种人类18q端粒探针、一种18号染色体特异性α-卫星探针和全18号染色体特异性探针进行细胞遗传学荧光原位杂交(FISH)。在之前报道的35例有18q末端缺失的患者中,我们发现5例(14%)有更复杂的隐匿性重排,3例(9%)保留了18q的最远端部分,这与中间缺失而非末端缺失一致。这些发现表明,标准核型可能导致对18q-综合征的特征描述不足。这对该综合征的表型定位以及正确的预后评估都有重要影响。