A Path to Implement Precision Child Health Cardiovascular Medicine

A Path to Implement Precision Child Health Cardiovascular Medicine

Congenital heart defects (CHDs) affect approximately 1% of live births and are a major source of childhood morbidity and mortality even in countries with advanced healthcare systems. Along with phenotypic heterogeneity, the underlying etiology of CHDs is multifactorial, involving genetic, epigenetic...

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Main Authors: Marlin Touma, Brian Reemtsen, Nancy Halnon, Juan Alejos, J. Paul Finn, Stanley F. Nelson, Yibin Wang
Format: Article
Language:English
Published: Frontiers Media S.A. 2017-06-01
Series:Frontiers in Cardiovascular Medicine
Subjects:
congenital heart defects
bio banking
whole-exome sequencing
RNA-sequencing
transcriptome
variants
Online Access:http://journal.frontiersin.org/article/10.3389/fcvm.2017.00036/full
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spelling doaj-aff27d8caa9749cdbf231b38255a018b2020-11-24T23:45:58ZengFrontiers Media S.A.Frontiers in Cardiovascular Medicine2297-055X2017-06-01410.3389/fcvm.2017.00036263277A Path to Implement Precision Child Health Cardiovascular MedicineMarlin Touma0Marlin Touma1Brian Reemtsen2Nancy Halnon3Juan Alejos4J. Paul Finn5Stanley F. Nelson6Yibin Wang7Yibin Wang8Department of Pediatrics, Children’s Discovery and Innovation Institute, University of California at Los Angeles, Los Angeles, CA, United StatesCardiovascular Research Laboratory, University of California at Los Angeles, Los Angeles, CA, United StatesDepartment of Cardiothoracic Surgery, University of California at Los Angeles, Los Angeles, CA, United StatesDepartment of Pediatrics, University of California at Los Angeles, Los Angeles, CA, United StatesDepartment of Pediatrics, University of California at Los Angeles, Los Angeles, CA, United StatesDepartment of Radiology, Cardiovascular Imaging, University of California at Los Angeles, Los Angeles, CA, United StatesDepartment of Human Genetics, University of California at Los Angeles, Los Angeles, CA, United StatesCardiovascular Research Laboratory, University of California at Los Angeles, Los Angeles, CA, United StatesDepartment of Anesthesiology, Physiology and Medicine, University of California at Los Angeles, Los Angeles, CA, United StatesCongenital heart defects (CHDs) affect approximately 1% of live births and are a major source of childhood morbidity and mortality even in countries with advanced healthcare systems. Along with phenotypic heterogeneity, the underlying etiology of CHDs is multifactorial, involving genetic, epigenetic, and/or environmental contributors. Clear dissection of the underlying mechanism is a powerful step to establish individualized therapies. However, the majority of CHDs are yet to be clearly diagnosed for the underlying genetic and environmental factors, and even less with effective therapies. Although the survival rate for CHDs is steadily improving, there is still a significant unmet need for refining diagnostic precision and establishing targeted therapies to optimize life quality and to minimize future complications. In particular, proper identification of disease associated genetic variants in humans has been challenging, and this greatly impedes our ability to delineate gene–environment interactions that contribute to the pathogenesis of CHDs. Implementing a systematic multileveled approach can establish a continuum from phenotypic characterization in the clinic to molecular dissection using combined next-generation sequencing platforms and validation studies in suitable models at the bench. Key elements necessary to advance the field are: first, proper delineation of the phenotypic spectrum of CHDs; second, defining the molecular genotype/phenotype by combining whole-exome sequencing and transcriptome analysis; third, integration of phenotypic, genotypic, and molecular datasets to identify molecular network contributing to CHDs; fourth, generation of relevant disease models and multileveled experimental investigations. In order to achieve all these goals, access to high-quality biological specimens from well-defined patient cohorts is a crucial step. Therefore, establishing a CHD BioCore is an essential infrastructure and a critical step on the path toward precision child health cardiovascular medicine.http://journal.frontiersin.org/article/10.3389/fcvm.2017.00036/fullcongenital heart defectsbio bankingwhole-exome sequencingRNA-sequencingtranscriptomevariants
collection DOAJ
language English
format Article
sources DOAJ
author Marlin Touma
Marlin Touma
Brian Reemtsen
Nancy Halnon
Juan Alejos
J. Paul Finn
Stanley F. Nelson
Yibin Wang
Yibin Wang
spellingShingle Marlin Touma
Marlin Touma
Brian Reemtsen
Nancy Halnon
Juan Alejos
J. Paul Finn
Stanley F. Nelson
Yibin Wang
Yibin Wang
A Path to Implement Precision Child Health Cardiovascular Medicine
Frontiers in Cardiovascular Medicine
congenital heart defects
bio banking
whole-exome sequencing
RNA-sequencing
transcriptome
variants
author_facet Marlin Touma
Marlin Touma
Brian Reemtsen
Nancy Halnon
Juan Alejos
J. Paul Finn
Stanley F. Nelson
Yibin Wang
Yibin Wang
author_sort Marlin Touma
title A Path to Implement Precision Child Health Cardiovascular Medicine
title_short A Path to Implement Precision Child Health Cardiovascular Medicine
title_full A Path to Implement Precision Child Health Cardiovascular Medicine
title_fullStr A Path to Implement Precision Child Health Cardiovascular Medicine
title_full_unstemmed A Path to Implement Precision Child Health Cardiovascular Medicine
title_sort path to implement precision child health cardiovascular medicine
publisher Frontiers Media S.A.
series Frontiers in Cardiovascular Medicine
issn 2297-055X
publishDate 2017-06-01
description Congenital heart defects (CHDs) affect approximately 1% of live births and are a major source of childhood morbidity and mortality even in countries with advanced healthcare systems. Along with phenotypic heterogeneity, the underlying etiology of CHDs is multifactorial, involving genetic, epigenetic, and/or environmental contributors. Clear dissection of the underlying mechanism is a powerful step to establish individualized therapies. However, the majority of CHDs are yet to be clearly diagnosed for the underlying genetic and environmental factors, and even less with effective therapies. Although the survival rate for CHDs is steadily improving, there is still a significant unmet need for refining diagnostic precision and establishing targeted therapies to optimize life quality and to minimize future complications. In particular, proper identification of disease associated genetic variants in humans has been challenging, and this greatly impedes our ability to delineate gene–environment interactions that contribute to the pathogenesis of CHDs. Implementing a systematic multileveled approach can establish a continuum from phenotypic characterization in the clinic to molecular dissection using combined next-generation sequencing platforms and validation studies in suitable models at the bench. Key elements necessary to advance the field are: first, proper delineation of the phenotypic spectrum of CHDs; second, defining the molecular genotype/phenotype by combining whole-exome sequencing and transcriptome analysis; third, integration of phenotypic, genotypic, and molecular datasets to identify molecular network contributing to CHDs; fourth, generation of relevant disease models and multileveled experimental investigations. In order to achieve all these goals, access to high-quality biological specimens from well-defined patient cohorts is a crucial step. Therefore, establishing a CHD BioCore is an essential infrastructure and a critical step on the path toward precision child health cardiovascular medicine.
topic congenital heart defects
bio banking
whole-exome sequencing
RNA-sequencing
transcriptome
variants
url http://journal.frontiersin.org/article/10.3389/fcvm.2017.00036/full
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