At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children

IMPORTANCE: Although the clinical utility of genome sequencing for critically ill children is well recognized, its utility for proactive pediatric screening is not well explored. OBJECTIVE: To evaluate molecular findings from screening ostensibly healthy children with genome sequencing compared with...

Descripción completa

Detalles Bibliográficos
Autores principales: Balciuniene, Jorune, Liu, Ruby, Bean, Lora, Guo, Fen, Nallamilli, Babi Ramesh Reddy, Guruju, Naga, Chen-Deutsch, Xiangwen, Yousaf, Rizwan, Fura, Kristina, Chin, Ephrem, Mathur, Abhinav, Ma, Zeqiang, Carmichael, Jonathan, da Silva, Cristina, Collins, Christin, Hegde, Madhuri
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Medical Association 2023
Materias:
Original Investigation
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10391308/
https://www.ncbi.nlm.nih.gov/pubmed/37523181
http://dx.doi.org/10.1001/jamanetworkopen.2023.26445
_version_ 1785082678350970880
author Balciuniene, Jorune
Liu, Ruby
Bean, Lora
Guo, Fen
Nallamilli, Babi Ramesh Reddy
Guruju, Naga
Chen-Deutsch, Xiangwen
Yousaf, Rizwan
Fura, Kristina
Chin, Ephrem
Mathur, Abhinav
Ma, Zeqiang
Carmichael, Jonathan
da Silva, Cristina
Collins, Christin
Hegde, Madhuri
author_facet Balciuniene, Jorune
Liu, Ruby
Bean, Lora
Guo, Fen
Nallamilli, Babi Ramesh Reddy
Guruju, Naga
Chen-Deutsch, Xiangwen
Yousaf, Rizwan
Fura, Kristina
Chin, Ephrem
Mathur, Abhinav
Ma, Zeqiang
Carmichael, Jonathan
da Silva, Cristina
Collins, Christin
Hegde, Madhuri
author_sort Balciuniene, Jorune
collection PubMed
description IMPORTANCE: Although the clinical utility of genome sequencing for critically ill children is well recognized, its utility for proactive pediatric screening is not well explored. OBJECTIVE: To evaluate molecular findings from screening ostensibly healthy children with genome sequencing compared with a gene panel for medically actionable pediatric conditions. DESIGN, SETTING, AND PARTICIPANTS: This case series study was conducted among consecutive, apparently healthy children undergoing proactive genetic screening for pediatric disorders by genome sequencing (n = 562) or an exome-based panel of 268 genes (n = 606) from March 1, 2018, through July 31, 2022. EXPOSURES: Genetic screening for pediatric-onset disorders using genome sequencing or an exome-based panel of 268 genes. MAIN OUTCOMES AND MEASURES: Molecular findings indicative of genetic disease risk. RESULTS: Of 562 apparently healthy children (286 girls [50.9%]; median age, 29 days [IQR, 9-117 days]) undergoing screening by genome sequencing, 46 (8.2%; 95% CI, 5.9%-10.5%) were found to be at risk for pediatric-onset disease, including 22 children (3.9%) at risk for high-penetrance disorders. Sequence analysis uncovered molecular diagnoses among 32 individuals (5.7%), while copy number variant analysis uncovered molecular diagnoses among 14 individuals (2.5%), including 4 individuals (0.7%) with chromosome scale abnormalities. Overall, there were 47 molecular diagnoses, with 1 individual receiving 2 diagnoses; of the 47 potential diagnoses, 22 (46.8%) were associated with high-penetrance conditions. Pathogenic variants in medically actionable pediatric genes were found in 6 individuals (1.1%), constituting 12.8% (6 of 47) of all diagnoses. At least 1 pharmacogenomic variant was reported for 89.0% (500 of 562) of the cohort. In contrast, of 606 children (293 girls [48.3%]; median age, 26 days [IQR, 10-67 days]) undergoing gene panel screening, only 13 (2.1%; 95% CI, 1.0%-3.3%) resulted in potential childhood-onset diagnoses, a significantly lower rate than those screened by genome sequencing (P < .001). CONCLUSIONS AND RELEVANCE: In this case series study, genome sequencing as a proactive screening approach for children, due to its unrestrictive gene content and technical advantages in comparison with an exome-based gene panel for medically actionable childhood conditions, uncovered a wide range of heterogeneous high-penetrance pediatric conditions that could guide early interventions and medical management.
format Online
Article
Text
id pubmed-10391308
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher American Medical Association
record_format MEDLINE/PubMed
spelling pubmed-103913082023-08-02 At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children Balciuniene, Jorune Liu, Ruby Bean, Lora Guo, Fen Nallamilli, Babi Ramesh Reddy Guruju, Naga Chen-Deutsch, Xiangwen Yousaf, Rizwan Fura, Kristina Chin, Ephrem Mathur, Abhinav Ma, Zeqiang Carmichael, Jonathan da Silva, Cristina Collins, Christin Hegde, Madhuri JAMA Netw Open Original Investigation IMPORTANCE: Although the clinical utility of genome sequencing for critically ill children is well recognized, its utility for proactive pediatric screening is not well explored. OBJECTIVE: To evaluate molecular findings from screening ostensibly healthy children with genome sequencing compared with a gene panel for medically actionable pediatric conditions. DESIGN, SETTING, AND PARTICIPANTS: This case series study was conducted among consecutive, apparently healthy children undergoing proactive genetic screening for pediatric disorders by genome sequencing (n = 562) or an exome-based panel of 268 genes (n = 606) from March 1, 2018, through July 31, 2022. EXPOSURES: Genetic screening for pediatric-onset disorders using genome sequencing or an exome-based panel of 268 genes. MAIN OUTCOMES AND MEASURES: Molecular findings indicative of genetic disease risk. RESULTS: Of 562 apparently healthy children (286 girls [50.9%]; median age, 29 days [IQR, 9-117 days]) undergoing screening by genome sequencing, 46 (8.2%; 95% CI, 5.9%-10.5%) were found to be at risk for pediatric-onset disease, including 22 children (3.9%) at risk for high-penetrance disorders. Sequence analysis uncovered molecular diagnoses among 32 individuals (5.7%), while copy number variant analysis uncovered molecular diagnoses among 14 individuals (2.5%), including 4 individuals (0.7%) with chromosome scale abnormalities. Overall, there were 47 molecular diagnoses, with 1 individual receiving 2 diagnoses; of the 47 potential diagnoses, 22 (46.8%) were associated with high-penetrance conditions. Pathogenic variants in medically actionable pediatric genes were found in 6 individuals (1.1%), constituting 12.8% (6 of 47) of all diagnoses. At least 1 pharmacogenomic variant was reported for 89.0% (500 of 562) of the cohort. In contrast, of 606 children (293 girls [48.3%]; median age, 26 days [IQR, 10-67 days]) undergoing gene panel screening, only 13 (2.1%; 95% CI, 1.0%-3.3%) resulted in potential childhood-onset diagnoses, a significantly lower rate than those screened by genome sequencing (P < .001). CONCLUSIONS AND RELEVANCE: In this case series study, genome sequencing as a proactive screening approach for children, due to its unrestrictive gene content and technical advantages in comparison with an exome-based gene panel for medically actionable childhood conditions, uncovered a wide range of heterogeneous high-penetrance pediatric conditions that could guide early interventions and medical management. American Medical Association 2023-07-31 /pmc/articles/PMC10391308/ /pubmed/37523181 http://dx.doi.org/10.1001/jamanetworkopen.2023.26445 Text en Copyright 2023 Balciuniene J et al. JAMA Network Open. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article distributed under the terms of the CC-BY-NC-ND License.
spellingShingle Original Investigation
Balciuniene, Jorune
Liu, Ruby
Bean, Lora
Guo, Fen
Nallamilli, Babi Ramesh Reddy
Guruju, Naga
Chen-Deutsch, Xiangwen
Yousaf, Rizwan
Fura, Kristina
Chin, Ephrem
Mathur, Abhinav
Ma, Zeqiang
Carmichael, Jonathan
da Silva, Cristina
Collins, Christin
Hegde, Madhuri
At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children
title At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children
title_full At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children
title_fullStr At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children
title_full_unstemmed At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children
title_short At-Risk Genomic Findings for Pediatric-Onset Disorders From Genome Sequencing vs Medically Actionable Gene Panel in Proactive Screening of Newborns and Children
title_sort at-risk genomic findings for pediatric-onset disorders from genome sequencing vs medically actionable gene panel in proactive screening of newborns and children
topic Original Investigation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10391308/
https://www.ncbi.nlm.nih.gov/pubmed/37523181
http://dx.doi.org/10.1001/jamanetworkopen.2023.26445
work_keys_str_mv AT balciunienejorune atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT liuruby atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT beanlora atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT guofen atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT nallamillibabirameshreddy atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT gurujunaga atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT chendeutschxiangwen atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT yousafrizwan atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT furakristina atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT chinephrem atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT mathurabhinav atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT mazeqiang atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT carmichaeljonathan atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT dasilvacristina atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT collinschristin atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren
AT hegdemadhuri atriskgenomicfindingsforpediatriconsetdisordersfromgenomesequencingvsmedicallyactionablegenepanelinproactivescreeningofnewbornsandchildren

Ejemplares similares