Zhao Lei, Zhang Qinghua, Zhou Bingbo, Zhang Chuang, Zheng Lei, Wang Yupei, Hao Shengju, Hui Ling
School of Public Health, Gansu University of Traditional Chinese Medicine, Lanzhou, Gansu 730000, China.
Zhonghua Yi Xue Yi Chuan Xue Za Zhi. 2023 Jan 10;40(1):7-11. doi: 10.3760/cma.j.cn511374-20220125-00067.
To analyze the clinical phenotype and results of genetic testing in three children with Cornelia de Lange syndrome (CdLS).
Clinical data of the children and their parents were collected. Peripheral blood samples of the pedigrees were collected for next generation sequencing analysis.
The main clinical manifestations of the three children have included growth delay, mental retardation, peculiar facies and other accompanying symptoms. Based on the criteria proposed by the International Diagnostic Consensus, all three children were suspected for CdLS. As revealed by whole exome sequencing, child 1 has harbored NIPBL gene c.5567_5569delGAA insTAT missense variant, child 2 has harbored SMC1A gene c.607A>G missense variant, and child 3 has harbored HDAC8 gene c.628+1G>A splicing variant. All of the variants were de novo in origin.
All of the children were diagnosed with CdLS due to pathogenic variants of the associated genes, among which the variants of NIPBL and HDAC8 genes were unreported previously. Above finding has enriched the spectrum of pathogenic variants underlying CdLS.
分析3例科妮莉亚·德朗热综合征(CdLS)患儿的临床表型及基因检测结果。
收集患儿及其父母的临床资料。采集家系外周血样本进行二代测序分析。
3例患儿的主要临床表现包括生长发育迟缓、智力障碍、特殊面容及其他伴随症状。根据国际诊断共识提出的标准,3例患儿均疑似CdLS。全外显子组测序结果显示,患儿1携带NIPBL基因c.5567_5569delGAA insTAT错义变异,患儿2携带SMC1A基因c.607A>G错义变异,患儿3携带HDAC8基因c.628+1G>A剪接变异。所有变异均为新发。
所有患儿均因相关基因的致病变异被诊断为CdLS,其中NIPBL和HDAC8基因的变异此前未见报道。上述发现丰富了CdLS潜在致病变异谱。
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