Genome sequencing as a platform for pharmacogenetic genotyping: a pediatric cohort study

Cohn, Iris; Paton, Tara; Marshall, Christian R.; Basran, Raveen K.; Stavropoulos, Dimitri J.; Ray, Peter N.; Monfared, Nasim; Hayeems, Robin Z.; Meyn, Stephen; Bowdin, Sarah; Scherer, Stephen W.; Cohn, Ronald D.; Itô, Shinya

doi:10.1038/s41525-017-0021-8

Cited by 47 publications

(53 citation statements)

References 44 publications

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“…Similarly, mitochondrial genomes in each cell may not all be identical, and a variant in only a subset is called heteroplasmy. 14,15 To gain further insight into the spectrum of genomic variation, we assessed the disease-causing potential of all disease-associated variants in accordance with guidelines of the American College of Medical Genetics and Genomics. Variants were sorted into categories of standard terminology: "benign," "likely benign," "variant of uncertain significance" (VUS), "likely pathogenic" or "pathogenic," 16 by applying specified information from the published literature and various disease-and populationbased databases.…”

Section: Box 1: Human Genome Variationmentioning

confidence: 99%

The Personal Genome Project Canada: findings from whole genome sequences of the inaugural 56 participants

Reuter

Walker²,

Thiruvahindrapuram³

et al. 2018

CMAJ

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Section: Box 1: Human Genome Variationmentioning

confidence: 99%

The Personal Genome Project Canada: findings from whole genome sequences of the inaugural 56 participants

Reuter

Walker²,

Thiruvahindrapuram³

et al. 2018

CMAJ

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“…Главной целью сбора и анализа фармакогенетической информации в настоящее время является возможность оптимизации терапии -выбор препарата, который улучшил бы соотношение риска и пользы для конкретного пациента. В одной из описанных ранее когорт 95 из 98 детей имели по крайней мере один клинически значимый фармакогеномный вариант, следовательно, превентивный фармакогенетический скрининг может способствовать безопасности пациентов [24].…”

Section: обмен опытомunclassified

High-performance DNA sequencing to identify genetically determined diseases in pediatric practice

Воинова

Николаева

Shcherbakova

et al. 2019

Ross. vestn. perinatol. pediatr.

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Технология секвенирования нового поколения (NGS) за последние годы стала важным диагностическим инструментом в педиатрии. В генетической педиатрической клинике проанализированы результаты применения полноэкзомного секвенирования у 42 детей с задержкой психического, физического развития и/или аномалиями различных органов и систем. У 19 больных был установлен первичный генетический диагноз, и, таким образом, эффективность экзомного секвенирования составила 45%, что несколько выше эффективности NGS, приводимой в источниках литературы. В статье представлены клинические наблюдения случаев первичного, возможного, двойного диагноза, прогностического вторичного варианта, примеры ошибок в интерпретации данных секвенирования. Подчеркивается важность исследования выявленных мутаций в семьях не только у родителей, но и других родственников пациента. В частности, в случае идентификации Х-сцепленных генетических вариантов обосновывается необходимость их анализа в трех поколениях семьи. Ключевые слова: дети, наследственные болезни, полноэкзомное секвенирование, секвенирование нового поколения, интерпретация данных секвенирования, первичный диагноз, возможный диагноз, двойной диагноз, прогностический вторичный вариант.

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“…While these exome cases did not meet criteria for Stavropoulos' technical comparison study, outcome data prompted by WES result disclosure remain relevant to the study reported here. As well, while pharmacogenomics variants were identified in this cohort [41], medical management implications of these variants were not captured because identified variants had not been validated or reported back to patients at the time these data were ascertained. The absence of cascade family testing is surprising, but perhaps attributable to de novo findings or the absence of documentation related to cascade family testing in the proband's medical record.…”

Section: Disscussionmentioning

confidence: 99%

Care and cost consequences of pediatric whole genome sequencing compared to chromosome microarray

et al. 2017

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The clinical use of whole-genome sequencing (WGS) is expected to alter pediatric medical management. The study aimed to describe the type and cost of healthcare activities following pediatric WGS compared to chromosome microarray (CMA). Healthcare activities prompted by WGS and CMA were ascertained for 101 children with developmental delay over 1 year. Activities following receipt of non-diagnostic CMA were compared to WGS diagnostic and non-diagnostic results. Activities were costed in 2016 Canadian dollars (CDN). Ongoing care accounted for 88.6% of post-test activities. The mean number of lab tests was greater following CMA than WGS (0.55 vs. 0.09; p = 0.007). The mean number of specialist visits was greater following WGS than CMA (0.41 vs. 0; p = 0.016). WGS results (diagnostic vs. non-diagnostic) modified the effect of test type on mean number of activities (p < 0.001). The cost of activities prompted by diagnostic WGS exceeded $557CDN for 10% of cases. In complex pediatric care, CMA prompted additional diagnostic investigations while WGS prompted tailored care guided by genotypic variants. Costs for prompted activities were low for the majority and constitute a small proportion of total test costs. Optimal use of WGS depends on robust evaluation of downstream care and cost consequences.

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Genome sequencing as a platform for pharmacogenetic genotyping: a pediatric cohort study

Cited by 47 publications

References 44 publications

The Personal Genome Project Canada: findings from whole genome sequences of the inaugural 56 participants

The Personal Genome Project Canada: findings from whole genome sequences of the inaugural 56 participants

High-performance DNA sequencing to identify genetically determined diseases in pediatric practice

Care and cost consequences of pediatric whole genome sequencing compared to chromosome microarray

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