Cargando…
Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin
An accurate and precisely annotated genome assembly is a fundamental requirement for functional genomic analysis. Here, the complete DNA sequence and gene annotation of mouse Chromosome 11 was used to test the efficacy of large-scale sequencing for mutation identification. We re-sequenced the 14,000...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Texto |
| Lenguaje: | English |
| Publicado: |
Public Library of Science
2009
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2782131/ https://www.ncbi.nlm.nih.gov/pubmed/20011118 http://dx.doi.org/10.1371/journal.pgen.1000759 |
| _version_ | 1782174607701180416 |
|---|---|
| author | Boles, Melissa K. Wilkinson, Bonney M. Wilming, Laurens G. Liu, Bin Probst, Frank J. Harrow, Jennifer Grafham, Darren Hentges, Kathryn E. Woodward, Lanette P. Maxwell, Andrea Mitchell, Karen Risley, Michael D. Johnson, Randy Hirschi, Karen Lupski, James R. Funato, Yosuke Miki, Hiroaki Marin-Garcia, Pablo Matthews, Lucy Coffey, Alison J. Parker, Anne Hubbard, Tim J. Rogers, Jane Bradley, Allan Adams, David J. Justice, Monica J. |
| author_facet | Boles, Melissa K. Wilkinson, Bonney M. Wilming, Laurens G. Liu, Bin Probst, Frank J. Harrow, Jennifer Grafham, Darren Hentges, Kathryn E. Woodward, Lanette P. Maxwell, Andrea Mitchell, Karen Risley, Michael D. Johnson, Randy Hirschi, Karen Lupski, James R. Funato, Yosuke Miki, Hiroaki Marin-Garcia, Pablo Matthews, Lucy Coffey, Alison J. Parker, Anne Hubbard, Tim J. Rogers, Jane Bradley, Allan Adams, David J. Justice, Monica J. |
| author_sort | Boles, Melissa K. |
| collection | PubMed |
| description | An accurate and precisely annotated genome assembly is a fundamental requirement for functional genomic analysis. Here, the complete DNA sequence and gene annotation of mouse Chromosome 11 was used to test the efficacy of large-scale sequencing for mutation identification. We re-sequenced the 14,000 annotated exons and boundaries from over 900 genes in 41 recessive mutant mouse lines that were isolated in an N-ethyl-N-nitrosourea (ENU) mutation screen targeted to mouse Chromosome 11. Fifty-nine sequence variants were identified in 55 genes from 31 mutant lines. 39% of the lesions lie in coding sequences and create primarily missense mutations. The other 61% lie in noncoding regions, many of them in highly conserved sequences. A lesion in the perinatal lethal line l11Jus13 alters a consensus splice site of nucleoredoxin (Nxn), inserting 10 amino acids into the resulting protein. We conclude that point mutations can be accurately and sensitively recovered by large-scale sequencing, and that conserved noncoding regions should be included for disease mutation identification. Only seven of the candidate genes we report have been previously targeted by mutation in mice or rats, showing that despite ongoing efforts to functionally annotate genes in the mammalian genome, an enormous gap remains between phenotype and function. Our data show that the classical positional mapping approach of disease mutation identification can be extended to large target regions using high-throughput sequencing. |
| format | Text |
| id | pubmed-2782131 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2009 |
| publisher | Public Library of Science |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-27821312009-12-15 Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin Boles, Melissa K. Wilkinson, Bonney M. Wilming, Laurens G. Liu, Bin Probst, Frank J. Harrow, Jennifer Grafham, Darren Hentges, Kathryn E. Woodward, Lanette P. Maxwell, Andrea Mitchell, Karen Risley, Michael D. Johnson, Randy Hirschi, Karen Lupski, James R. Funato, Yosuke Miki, Hiroaki Marin-Garcia, Pablo Matthews, Lucy Coffey, Alison J. Parker, Anne Hubbard, Tim J. Rogers, Jane Bradley, Allan Adams, David J. Justice, Monica J. PLoS Genet Research Article An accurate and precisely annotated genome assembly is a fundamental requirement for functional genomic analysis. Here, the complete DNA sequence and gene annotation of mouse Chromosome 11 was used to test the efficacy of large-scale sequencing for mutation identification. We re-sequenced the 14,000 annotated exons and boundaries from over 900 genes in 41 recessive mutant mouse lines that were isolated in an N-ethyl-N-nitrosourea (ENU) mutation screen targeted to mouse Chromosome 11. Fifty-nine sequence variants were identified in 55 genes from 31 mutant lines. 39% of the lesions lie in coding sequences and create primarily missense mutations. The other 61% lie in noncoding regions, many of them in highly conserved sequences. A lesion in the perinatal lethal line l11Jus13 alters a consensus splice site of nucleoredoxin (Nxn), inserting 10 amino acids into the resulting protein. We conclude that point mutations can be accurately and sensitively recovered by large-scale sequencing, and that conserved noncoding regions should be included for disease mutation identification. Only seven of the candidate genes we report have been previously targeted by mutation in mice or rats, showing that despite ongoing efforts to functionally annotate genes in the mammalian genome, an enormous gap remains between phenotype and function. Our data show that the classical positional mapping approach of disease mutation identification can be extended to large target regions using high-throughput sequencing. Public Library of Science 2009-12-11 /pmc/articles/PMC2782131/ /pubmed/20011118 http://dx.doi.org/10.1371/journal.pgen.1000759 Text en Boles et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited. |
| spellingShingle | Research Article Boles, Melissa K. Wilkinson, Bonney M. Wilming, Laurens G. Liu, Bin Probst, Frank J. Harrow, Jennifer Grafham, Darren Hentges, Kathryn E. Woodward, Lanette P. Maxwell, Andrea Mitchell, Karen Risley, Michael D. Johnson, Randy Hirschi, Karen Lupski, James R. Funato, Yosuke Miki, Hiroaki Marin-Garcia, Pablo Matthews, Lucy Coffey, Alison J. Parker, Anne Hubbard, Tim J. Rogers, Jane Bradley, Allan Adams, David J. Justice, Monica J. Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin |
| title | Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin |
| title_full | Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin |
| title_fullStr | Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin |
| title_full_unstemmed | Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin |
| title_short | Discovery of Candidate Disease Genes in ENU–Induced Mouse Mutants by Large-Scale Sequencing, Including a Splice-Site Mutation in Nucleoredoxin |
| title_sort | discovery of candidate disease genes in enu–induced mouse mutants by large-scale sequencing, including a splice-site mutation in nucleoredoxin |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2782131/ https://www.ncbi.nlm.nih.gov/pubmed/20011118 http://dx.doi.org/10.1371/journal.pgen.1000759 |
| work_keys_str_mv | AT bolesmelissak discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT wilkinsonbonneym discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT wilminglaurensg discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT liubin discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT probstfrankj discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT harrowjennifer discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT grafhamdarren discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT hentgeskathryne discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT woodwardlanettep discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT maxwellandrea discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT mitchellkaren discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT risleymichaeld discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT johnsonrandy discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT hirschikaren discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT lupskijamesr discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT funatoyosuke discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT mikihiroaki discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT maringarciapablo discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT matthewslucy discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT coffeyalisonj discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT parkeranne discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT hubbardtimj discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT rogersjane discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT bradleyallan discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT adamsdavidj discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin AT justicemonicaj discoveryofcandidatediseasegenesinenuinducedmousemutantsbylargescalesequencingincludingasplicesitemutationinnucleoredoxin |