Whole-genome sequencing for identification of Mendelian disorders in critically ill infants: a retrospective analysis of diagnostic and clinical findings

Willig, Laurel K.; Petrikin, Josh E; Smith, Laurie D.; Saunders, Carol J.; Thiffault, Isabelle; Miller, Neil; Soden, Sarah E; Cakici, Julie A.; Herd, Suzanne; Twist, Greyson P; Noll, Aaron; Creed, Mitchell; Alba, Patria; Carpenter, Shannon L.; Clements, Mark A.; Fischer, Ryan T.; Hays, J Allyson; Kilbride, Howard W.; McDonough, Ryan; Rosterman, Jamie L.; Tsai, Sarah L; Zellmer, Lee; Farrow, Emily; Kingsmore, Stephen F.

doi:10.1016/s2213-2600(15)00139-3

Cited by 338 publications

(487 citation statements)

References 51 publications

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“…15 In a study of wholegenome sequencing in children retrospectively identified after an inpa tient stay in either the neonatal or pediatric inten sive care unit, a diagnosis was achieved in 57% (20/35) of cases. 11 These wholegenome sequencing studies required highthroughput sequencers, bioinformatics support, automation and experts in the field of translational genomics, resources that are not readily available to most diagnostic laboratories at this time. Another option, wholeexome sequencing, focuses on the protein coding regions of the approximately 22 000 human genes.…”

Section: Discussionmentioning

confidence: 99%

Next-generation sequencing for diagnosis of rare diseases in the neonatal intensive care unit

Daoud

Luco

et al. 2016

CMAJ

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Results: Of 20 newborns studied, 8 received a diagnosis on the basis of next-generation sequencing (diagnostic rate 40%). The diagnoses were renal tubular dysgenesis, SCN1A-related encephalopathy syndrome, myotubular myo pathy, FTO deficiency syndrome, cranioectodermal dysplasia, congenital myasthenic syndrome, autosomal dominant intellectual disability syndrome type 7 and Denys-Drash syndrome.Interpretation: This pilot study highlighted the potential of next-generation sequencing to deliver molecular diagnoses rapidly with a high success rate. With broader use, this approach has the potential to alter health care delivery in the NICU. AbstractSee also www.cmaj.ca/lookup/doi/10.1503/cmaj.160490Research CMAJ, August 9, 2016, 188(11) E255and clinicians providing care. 7 The inability to arrive at a timely and efficient diagnosis repre sents a substantial lost opportunity, as a diagno sis can limit or even halt further invasive, and at times futile, investigations for the neonate. Importantly, an accurate diagnosis informs prog nosis and may guide management decisions.The advent of nextgeneration sequencing has greatly advanced the ability to rapidly identify the novel genes responsible for disease. 8 Whole exome sequencing (sequencing of the coding portion of the genome) is beginning to be used on a clinical basis in tertiary care centres.9,10 In these initial clinical cohort studies, a molecular diagnosis was provided by wholeexome sequencing for about 25% of families. The pro portion increased to 31% when the patient's par ents were also analyzed. 9 Another study used retro spective wholegenome sequencing to make a diagnosis in 57% of 35 children from the inten sive care setting. 11Although wholeexome and wholegenome sequencing are powerful tools, important condi tions are required for translation of these meth ods to the clinic or hospital setting. The avail ability of highthroughput sequencers, complex and costly infrastructure, and personnel with bioinformatics expertise are prerequisites. These resources may not be broadly available within some health care systems, and other strategies may be more relevant and effective.Another attractive alternative is analysis based on nextgeneration sequencing that focuses only on the clinically relevant genes with known associated clinical phenotypes. 12This strategy offers several advantages over wholeexome or wholegenome sequencinginterpretation of variants may be more straight forward, a higher depth of coverage can be read ily achieved, and less infrastructure and fewer personnel are required -all of which contribute to a more rapid return of results.For this pilot study, we evaluated the perform ance of a targeted nextgeneration sequencing panel that included 4813 "diseaserelevant" genes in a cohort of newborns with rare disease in the NICU and assessed the effectiveness of this method to accurately diagnose these critically ill babies. Methods ParticipantsWe recruited patients for this pilot study between January and December 2014 from the NICUs of 2 regional hospi...

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Section: Discussionmentioning

confidence: 99%

Next-generation sequencing for diagnosis of rare diseases in the neonatal intensive care unit

Daoud

Luco

et al. 2016

CMAJ

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“…3,[31][32][33][34][35][36][37][38][39][40][41][42] Seven studies presented data on the costs of WES or WGS testing pathways, [24][25][26][27][43][44][45] and eight studies presented data on clinically relevant outcome measures for these tests. 5,6,[8][9][10][46][47][48] Of the eight full economic evaluations, two were CUAs 22,23 and six were CEAs, published between 2014 and 2017 in Australia (2), the United States (1), the UK (1), the Netherlands (1), and Canada (1). [18][19][20][21][28][29][30] Of these publications, the study by Soden et al 29 did not directly report WES costs but estimated Population unclear 2 (6) No study population 6 (17) WES, whole-exome sequencing; WGS, whole-genome sequencing.…”

Section: Study Characteristicsmentioning

confidence: 99%

“…Seven of these studies investigated WES; 5,6,[8][9][10]46,47 the eighth evaluated WGS. 48 Four publications used the traditional care pathway in the investigated condition as a comparator. 6,10,46,48 Three publications were retrospective analyses 6,47,48 and three were diagnostic studies, estimating the diagnostic yield of WES in a variety of conditions.…”

Section: Study Characteristicsmentioning

confidence: 99%

“…48 Four publications used the traditional care pathway in the investigated condition as a comparator. 6,10,46,48 Three publications were retrospective analyses 6,47,48 and three were diagnostic studies, estimating the diagnostic yield of WES in a variety of conditions. 5,8,9 The final two studies were case studies on single probands and families.…”

Section: Study Characteristicsmentioning

confidence: 99%

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Are whole-exome and whole-genome sequencing approaches cost-effective? A systematic review of the literature

Schwarze

Buchanan

Taylor

et al. 2018

Genetics in Medicine

415

198

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Purpose: We conducted a systematic literature review to summarize the current health economic evidence for wholeexome sequencing (WES) and whole-genome sequencing (WGS).Methods: Relevant studies were identified in the EMBASE, MEDLINE, Cochrane Library, EconLit and University of York Centre for Reviews and Dissemination databases from January 2005 to July 2016. Publications were included in the review if they were economic evaluations, cost studies, or outcome studies.Results: Thirty-six studies met our inclusion criteria. These publications investigated the use of WES and WGS in a variety of genetic conditions in clinical practice, the most common being neurological or neurodevelopmental disorders. Study sample size varied from a single child to 2,000 patients. Cost estimates for a single test ranged from $555 to $5,169 for WES and from $1,906 to $24,810 for WGS. Few cost analyses presented data transparently and many publications did not state which components were included in cost estimates. Conclusion:The current health economic evidence base to support the more widespread use of WES and WGS in clinical practice is very limited. Studies that carefully evaluate the costs, effectiveness, and cost-effectiveness of these tests are urgently needed to support their translation into clinical practice.Genet Med advance online publication 15 February 2018

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“…BRCA-negative familial breast cancer), and even to screen healthy individuals for future planning and predictive outcomes. Though WES is not generally applied to newborns, in critically ill infants it has shown a high rate of diagnosis of genetic disorders that have a direct effect on management and outcome (Saunders et al, 2012;Willig et al, 2015).…”

Section: Discussionmentioning

confidence: 99%

Challenges of using next generation sequencing in newborn screening

Reinstein

2015

Genet. Res.

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SummaryWhole-genome and whole-exome sequencing for clinical applications is now an integral part of medical genetics practice. The term newborn screening refers to public health programs designed to screen newborns for various treatable metabolic conditions, by measuring levels of circulating blood metabolites. The availability and significant decrease in sequencing costs has raised the question of whether metabolic newborn screening should be replaced by whole-genome or whole-exome sequencing. While newborn genome sequencing can potentially increase the number of disorders identified by newborn screening, the generalization of its practice raises a number of important ethical issues. This short article argues that there are medical, psychological, ethical and economic reasons why widespread dissemination of newborn screening is still premature.

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Whole-genome sequencing for identification of Mendelian disorders in critically ill infants: a retrospective analysis of diagnostic and clinical findings

Cited by 338 publications

References 51 publications

Next-generation sequencing for diagnosis of rare diseases in the neonatal intensive care unit

Next-generation sequencing for diagnosis of rare diseases in the neonatal intensive care unit

Are whole-exome and whole-genome sequencing approaches cost-effective? A systematic review of the literature

Challenges of using next generation sequencing in newborn screening

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