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Literature DB >> 22585771

Incidental medical information in whole-exome sequencing.

Benjamin D Solomon¹, Donald W Hadley, Daniel E Pineda-Alvarez, Aparna Kamat, Jamie K Teer, Praveen F Cherukuri, Nancy F Hansen, Pedro Cruz, Alice C Young, Benjamin E Berkman, Settara C Chandrasekharappa, James C Mullikin.

Abstract

Genomic technologies, such as whole-exome sequencing, are a powerful tool in genetic research. Such testing yields a great deal of incidental medical information, or medical information not related to the primary research target. We describe the management of incidental medical information derived from whole-exome sequencing in the research context. We performed whole-exome sequencing on a monozygotic twin pair in which only 1 child was affected with congenital anomalies and applied an institutional review board-approved algorithm to determine what genetic information would be returned. Whole-exome sequencing identified 79525 genetic variants in the twins. Here, we focus on novel variants. After filtering artifacts and excluding known single nucleotide polymorphisms and variants not predicted to be pathogenic, the twins had 32 novel variants in 32 genes that were felt to be likely to be associated with human disease. Eighteen of these novel variants were associated with recessive disease and 18 were associated with dominantly manifesting conditions (variants in some genes were potentially associated with both recessive and dominant conditions), but only 1 variant ultimately met our institutional review board-approved criteria for return of information to the research participants.

Entities: Disease Species

Mesh：

Year: 2012 PMID： 22585771 PMCID： PMC3362899 DOI： 10.1542/peds.2011-0080

Source DB: PubMed Journal: Pediatrics ISSN： 0031-4005 Impact factor: 7.124

74 in total

1. Dyssegmental dysplasia, Silverman-Handmaker type, is caused by functional null mutations of the perlecan gene.

Authors: E Arikawa-Hirasawa; W R Wilcox; A H Le; N Silverman; P Govindraj; J R Hassell; Y Yamada
Journal: Nat Genet Date: 2001-04 Impact factor: 38.330

2. Perlecan, the major proteoglycan of basement membranes, is altered in patients with Schwartz-Jampel syndrome (chondrodystrophic myotonia).

Authors: S Nicole; C S Davoine; H Topaloglu; L Cattolico; D Barral; P Beighton; C B Hamida; H Hammouda; C Cruaud; P S White; D Samson; J A Urtizberea; F Lehmann-Horn; J Weissenbach; F Hentati; B Fontaine
Journal: Nat Genet Date: 2000-12 Impact factor: 38.330

3. Identification of a missense mutation (G329A;Arg(110)--> GLN) in the human FUT7 gene.

Authors: P Bengtson; C Larson; A Lundblad; G Larson; P Påhlsson
Journal: J Biol Chem Date: 2001-06-12 Impact factor: 5.157

4. Neonatal pulmonary hypertension--urea-cycle intermediates, nitric oxide production, and carbamoyl-phosphate synthetase function.

Authors: D L Pearson; S Dawling; W F Walsh; J L Haines; B W Christman; A Bazyk; N Scott; M L Summar
Journal: N Engl J Med Date: 2001-06-14 Impact factor: 91.245

5. Chromosome 1 loci in Finnish schizophrenia families.

Authors: J Ekelund; I Hovatta; A Parker; T Paunio; T Varilo; R Martin; J Suhonen; P Ellonen; G Chan; J S Sinsheimer; E Sobel; H Juvonen; R Arajärvi; T Partonen; J Suvisaari; J Lönnqvist; J Meyer; L Peltonen
Journal: Hum Mol Genet Date: 2001-07-15 Impact factor: 6.150

6. Mutations in DNAH5 cause primary ciliary dyskinesia and randomization of left-right asymmetry.

Authors: Heike Olbrich; Karsten Häffner; Andreas Kispert; Alexander Völkel; Andreas Volz; Gürsel Sasmaz; Richard Reinhardt; Steffen Hennig; Hans Lehrach; Nikolaus Konietzko; Maimoona Zariwala; Peadar G Noone; Michael Knowles; Hannah M Mitchison; Maggie Meeks; Eddie M K Chung; Friedhelm Hildebrandt; Ralf Sudbrak; Heymut Omran
Journal: Nat Genet Date: 2002-01-14 Impact factor: 38.330

7. Association between polymorphisms in dopamine metabolic enzymes and tobacco consumption in smokers.

Authors: E F McKinney; R T Walton; P Yudkin; A Fuller; N A Haldar; D Mant; M Murphy; K I Welsh; S E Marshall
Journal: Pharmacogenetics Date: 2000-08

8. Disruption of two novel genes by a translocation co-segregating with schizophrenia.

Authors: J K Millar; J C Wilson-Annan; S Anderson; S Christie; M S Taylor; C A Semple; R S Devon; D M St Clair; W J Muir; D H Blackwood; D J Porteous
Journal: Hum Mol Genet Date: 2000-05-22 Impact factor: 6.150

9. Mutations in the dopamine beta-hydroxylase gene are associated with human norepinephrine deficiency.

Authors: Chun-Hyung Kim; Cyrus P Zabetian; Joseph F Cubells; Sonhae Cho; Italo Biaggioni; Bruce M Cohen; David Robertson; Kwang-Soo Kim
Journal: Am J Med Genet Date: 2002-03-01

10. Evidence for allelic association of the dopamine beta-hydroxylase gene (DBH) with susceptibility to typical migraine.

Authors: R A Lea; A Dohy; K Jordan; S Quinlan; P J Brimage; L R Griffiths
Journal: Neurogenetics Date: 2000-09 Impact factor: 2.660

22 in total

1. Prenatal whole genome sequencing: just because we can, should we?

Authors: Greer Donley; Sara Chandros Hull; Benjamin E Berkman
Journal: Hastings Cent Rep Date: 2012-06-20 Impact factor: 2.683

Review 2. Applications of high-throughput DNA sequencing to benign hematology.

Authors: Vijay G Sankaran; Patrick G Gallagher
Journal: Blood Date: 2013-09-10 Impact factor: 22.113

3. Whole-genome sequencing in health care. Recommendations of the European Society of Human Genetics.

Authors: Carla G van El; Martina C Cornel; Pascal Borry; Ros J Hastings; Florence Fellmann; Shirley V Hodgson; Heidi C Howard; Anne Cambon-Thomsen; Bartha M Knoppers; Hanne Meijers-Heijboer; Hans Scheffer; Lisbeth Tranebjaerg; Wybo Dondorp; Guido M W R de Wert
Journal: Eur J Hum Genet Date: 2013-06 Impact factor: 4.246

Incidental medical information in whole-exome sequencing.

1. Dyssegmental dysplasia, Silverman-Handmaker type, is caused by functional null mutations of the perlecan gene.

2. Perlecan, the major proteoglycan of basement membranes, is altered in patients with Schwartz-Jampel syndrome (chondrodystrophic myotonia).

3. Identification of a missense mutation (G329A;Arg(110)--> GLN) in the human FUT7 gene.

4. Neonatal pulmonary hypertension--urea-cycle intermediates, nitric oxide production, and carbamoyl-phosphate synthetase function.

5. Chromosome 1 loci in Finnish schizophrenia families.

6. Mutations in DNAH5 cause primary ciliary dyskinesia and randomization of left-right asymmetry.

7. Association between polymorphisms in dopamine metabolic enzymes and tobacco consumption in smokers.

8. Disruption of two novel genes by a translocation co-segregating with schizophrenia.

9. Mutations in the dopamine beta-hydroxylase gene are associated with human norepinephrine deficiency.

10. Evidence for allelic association of the dopamine beta-hydroxylase gene (DBH) with susceptibility to typical migraine.

1. Prenatal whole genome sequencing: just because we can, should we?

Review 2. Applications of high-throughput DNA sequencing to benign hematology.

3. Whole-genome sequencing in health care. Recommendations of the European Society of Human Genetics.

4. Clinical genomic database.

5. Applying Genomic Analysis to Newborn Screening.

6. Applying deep DNA sequencing to common, complex pediatric traits.

7. Incomplete knowledge of the clinical context as a barrier to interpreting incidental genetic research findings.

8. Whole-genome sequencing in health care: recommendations of the European Society of Human Genetics.

9. Enhancing the incidental pipeline in genomic sequencing.

10. Potential Role of Genomic Sequencing in the Early Diagnosis of Treatable Genetic Conditions.