Parallel Tests of Whole Exome Sequencing and Copy Number Variant Sequencing Increase the Diagnosis Yields of Rare Pediatric Disorders

被引:13
作者
Hu, Xuyun [1 ,2 ,3 ]
Guo, Ruolan [1 ,2 ,3 ]
Guo, Jun [1 ,2 ,3 ]
Qi, Zhan [1 ,2 ,3 ]
Li, Wei [1 ,2 ,3 ]
Hao, Chanjuan [1 ,2 ,3 ]
机构
[1] Capital Med Univ, Beijing Childrens Hosp, Natl Ctr Childrens Hlth, Beijing Pediat Res Inst,Beijing Key Lab Genet Bir, Beijing, Peoples R China
[2] Capital Med Univ, Beijing Childrens Hosp, Natl Ctr Childrens Hlth, MOE Key Lab Major Dis Children, Beijing, Peoples R China
[3] Beijing Childrens Hosp, Zhengzhou Hosp, Henan Key Lab Pediat Inherited & Metab Dis, Henan Childrens Hosp, Zhengzhou, Peoples R China
来源
FRONTIERS IN GENETICS | 2020年 / 11卷
关键词
whole exome sequencing; copy number variants sequencing; pediatric disorders; cost-effective; clinical utility; JOINT CONSENSUS RECOMMENDATION; SYNDROMIC SHORT STATURE; MEDICAL GENETICS; AMERICAN-COLLEGE; CHROMOSOMAL MICROARRAY; CLINICAL UTILITY; GUIDELINES; STANDARDS; IDENTIFICATION; GENOMICS;
D O I
10.3389/fgene.2020.00473
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Background:Both whole exome sequencing and copy number variants sequencing were applied to identify the genetic cause of rare pediatric disorders. In our study, we aimed to investigate the diagnostic yield of parallel tests of trio whole exome sequencing and copy number variants sequencing and its clinical utility. Methods:After collecting detailed clinical information, a total of 60 patients were referred to parallel tests of whole exome sequencing and copy number variants sequencing, which used shared initial libraries. Results:26 pathogenic or likely pathogenic single nucleotide variants and 11 copy number variants were identified in 32 patients. 65.4% (17/26) of the SNVs were novel. The overall diagnosis rate was 53.3%. For the patients with positive results, 22 (36.7%) patients were diagnosed by whole exome sequencing and 10 (16.7%) patients were diagnosed by copy number variants sequencing. We also reviewed clinical impact on selected cases. Conclusion:We adopted an approach by performing parallel tests of trio whole exome sequencing and copy number variants sequencing with shared initial libraries. This strategy is relatively efficient and cost-effective for the diagnosis of rare pediatric disorders with high heterogeneity.
引用
收藏
页数:7
相关论文
共 41 条
[1]   Practical Guidelines for Managing Patients with 22q11.2 Deletion Syndrome [J].
Bassett, Anne S. ;
McDonald-McGinn, Donna M. ;
Devriendt, Koen ;
Digilio, Maria Cristina ;
Goldenberg, Paula ;
Habel, Alex ;
Marino, Bruno ;
Oskarsdottir, Solveig ;
Philip, Nicole ;
Sullivan, Kathleen ;
Swillen, Ann ;
Vorstman, Jacob .
JOURNAL OF PEDIATRICS, 2011, 159 (02) :332-U213
[2]   Genomic diagnosis for children with intellectual disability and/or developmental delay [J].
Bowling, Kevin M. ;
Thompson, Michelle L. ;
Amaral, Michelle D. ;
Finnila, Candice R. ;
Hiatt, Susan M. ;
Engel, Krysta L. ;
Cochran, J. Nicholas ;
Brothers, Kyle B. ;
East, Kelly M. ;
Gray, David E. ;
Kelley, Whitley V. ;
Lamb, Neil E. ;
Lose, Edward J. ;
Rich, Carla A. ;
Simmons, Shirley ;
Whittle, Jana S. ;
Weaver, Benjamin T. ;
Nesmith, Amy S. ;
Myers, Richard M. ;
Barsh, Gregory S. ;
Bebin, E. Martina ;
Cooper, Gregory M. .
GENOME MEDICINE, 2017, 9
[3]   Next-generation sequencing for diagnosis of rare diseases in the neonatal intensive care unit [J].
Daoud, Hussein ;
Luco, Stephanie M. ;
Li, Rui ;
Bareke, Eric ;
Beaulieu, Chandree ;
Jarinova, Olga ;
Carson, Nancy ;
Nikkel, Sarah M. ;
Graham, Gail E. ;
Richer, Julie ;
Armour, Christine ;
Bulman, Dennis E. ;
Chakraborty, Pranesh ;
Geraghty, Michael ;
Lines, Matthew A. ;
Lacaze-Masmonteil, Thierry ;
Majewski, Jacek ;
Boycott, Kym M. ;
Dyment, David A. .
CANADIAN MEDICAL ASSOCIATION JOURNAL, 2016, 188 (11) :E254-E260
[4]   Haploinsufficiency of PAX9 is associated with autosomal dominant hypodontia [J].
Das, P ;
Stockton, DW ;
Bauer, C ;
Shaffer, LG ;
D'Souza, RN ;
Wright, JT ;
Patel, PI .
HUMAN GENETICS, 2002, 110 (04) :371-376
[5]   Diagnostic Yields of Trio-WES Accompanied by CNVseq for Rare Neurodevelopmental Disorders [J].
Gao, Chao ;
Wang, Xiaona ;
Mei, Shiyue ;
Li, Dongxiao ;
Duan, Jiali ;
Zhang, Pei ;
Chen, Baiyun ;
Han, Liang ;
Gao, Yang ;
Yang, Zhenhua ;
Li, Bing ;
Yang, Xiu-An .
FRONTIERS IN GENETICS, 2019, 10
[6]   Advantages of a next generation sequencing targeted approach for the molecular diagnosis of retinoblastoma [J].
Grotta, Simona ;
D'Elia, Gemma ;
Scavelli, Rossana ;
Genovese, Silvia ;
Surace, Cecilia ;
Sirleto, Pietro ;
Cozza, Raffaele ;
Romanzo, Antonino ;
De Ioris, Maria Antonietta ;
Valente, Paola ;
Tomaiuolo, Anna Cristina ;
Lepri, Francesca Romana ;
Franchin, Tiziana ;
Ciocca, Laura ;
Russo, Serena ;
Locatelli, Franco ;
Angioni, Adriano .
BMC CANCER, 2015, 15
[7]  
Han JY, 2020, CLIN EXP PEDIATR, V63, P195, DOI 10.3345/kjp.2019.00808
[8]   Identical deletion at 14q13.3 including PAX9 and NKX2-1 in siblings from mosaicism of unaffected parent [J].
Hayashi, Shin ;
Yagi, Mariko ;
Morisaki, Ichijiro ;
Inazawa, Johji .
JOURNAL OF HUMAN GENETICS, 2015, 60 (04) :203-206
[9]   Recurrent Copy Number Variants Associated with Syndromic Short Stature of Unknown Cause [J].
Homma, Thais K. ;
Krepischi, Ana C. V. ;
Furuya, Tatiane K. ;
Honjo, Rachel S. ;
Malaquias, Alexsandra C. ;
Bertola, Debora R. ;
Costa, Silvia S. ;
Canton, Ana P. ;
Roela, Rosimeire A. ;
Freire, Bruna L. ;
Kim, Chong A. ;
Rosenberg, Carla ;
Jorge, Alexander A. L. .
HORMONE RESEARCH IN PAEDIATRICS, 2018, 89 (01) :13-21
[10]   A novel 14q13.1-21.1 deletion identified by CNV-Seq in a patient with brain-lung-thyroid syndrome, tooth agenesis and immunodeficiency [J].
Hu, Xuyun ;
Liu, Jun ;
Guo, Ruolan ;
Guo, Jun ;
Zhao, Zhipeng ;
Li, Wei ;
Xu, Baoping ;
Hao, Chanjuan .
MOLECULAR CYTOGENETICS, 2019, 12 (01)
12345