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Literature DB >> 23035047

Rapid whole-genome sequencing for genetic disease diagnosis in neonatal intensive care units.

Carol Jean Saunders¹, Neil Andrew Miller, Sarah Elizabeth Soden, Darrell Lee Dinwiddie, Aaron Noll, Noor Abu Alnadi, Nevene Andraws, Melanie LeAnn Patterson, Lisa Ann Krivohlavek, Joel Fellis, Sean Humphray, Peter Saffrey, Zoya Kingsbury, Jacqueline Claire Weir, Jason Betley, Russell James Grocock, Elliott Harrison Margulies, Emily Gwendolyn Farrow, Michael Artman, Nicole Pauline Safina, Joshua Erin Petrikin, Kevin Peter Hall, Stephen Francis Kingsmore.

Abstract

Monogenic diseases are frequent causes of neonatal morbidity and mortality, and disease presentations are often undifferentiated at birth. More than 3500 monogenic diseases have been characterized, but clinical testing is available for only some of them and many feature clinical and genetic heterogeneity. Hence, an immense unmet need exists for improved molecular diagnosis in infants. Because disease progression is extremely rapid, albeit heterogeneous, in newborns, molecular diagnoses must occur quickly to be relevant for clinical decision-making. We describe 50-hour differential diagnosis of genetic disorders by whole-genome sequencing (WGS) that features automated bioinformatic analysis and is intended to be a prototype for use in neonatal intensive care units. Retrospective 50-hour WGS identified known molecular diagnoses in two children. Prospective WGS disclosed potential molecular diagnosis of a severe GJB2-related skin disease in one neonate; BRAT1-related lethal neonatal rigidity and multifocal seizure syndrome in another infant; identified BCL9L as a novel, recessive visceral heterotaxy gene (HTX6) in a pedigree; and ruled out known candidate genes in one infant. Sequencing of parents or affected siblings expedited the identification of disease genes in prospective cases. Thus, rapid WGS can potentially broaden and foreshorten differential diagnosis, resulting in fewer empirical treatments and faster progression to genetic and prognostic counseling.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：

Year: 2012 PMID： 23035047 PMCID： PMC4283791 DOI： 10.1126/scitranslmed.3004041

Source DB: PubMed Journal: Sci Transl Med ISSN： 1946-6234 Impact factor: 17.956

66 in total

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4. Costs and end-of-life care in the NICU: lessons for the MICU?

Authors: John D Lantos; William L Meadow
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6. Constitutive transcriptional activation by a beta-catenin-Tcf complex in APC-/- colon carcinoma.

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8. Attenuated BMP1 function compromises osteogenesis, leading to bone fragility in humans and zebrafish.

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9. Essential role of BCL9-2 in the switch between beta-catenin's adhesive and transcriptional functions.

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10. A mitochondrial protein compendium elucidates complex I disease biology.

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229 in total

Rapid whole-genome sequencing for genetic disease diagnosis in neonatal intensive care units.

1. Wnt/wingless signaling requires BCL9/legless-mediated recruitment of pygopus to the nuclear beta-catenin-TCF complex.

2. Clan genomics and the complex architecture of human disease.

3. Human gene copy number spectra analysis in congenital heart malformations.

4. Costs and end-of-life care in the NICU: lessons for the MICU?

5. Contribution of birth defects to infant mortality among racial/ethnic minority groups, United States, 1983.

6. Constitutive transcriptional activation by a beta-catenin-Tcf complex in APC-/- colon carcinoma.

7. Zebrafish Nkd1 promotes Dvl degradation and is required for left-right patterning.

8. Attenuated BMP1 function compromises osteogenesis, leading to bone fragility in humans and zebrafish.

9. Essential role of BCL9-2 in the switch between beta-catenin's adhesive and transcriptional functions.

10. A mitochondrial protein compendium elucidates complex I disease biology.

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2. Challenges of using next generation sequencing in newborn screening.

Review 3. Return of genetic testing results in the era of whole-genome sequencing.

Review 4. Axons to Exons: the Molecular Diagnosis of Rare Neurological Diseases by Next-Generation Sequencing.

Review 5. Human genotype-phenotype databases: aims, challenges and opportunities.

6. Perceived Benefits, Risks, and Utility of Newborn Genomic Sequencing in the BabySeq Project.

7. Statistical Analysis of Nonuniform Volume Distributions for Droplet-Based Digital PCR Assays.

Review 8. Understanding human glycosylation disorders: biochemistry leads the charge.

Review 9. Peri-mortem evaluation of infants who die without a diagnosis: focus on advances in genomic technology.

10. Parent and public interest in whole-genome sequencing.