Cargando…
Pathogenicity and selective constraint on variation near splice sites
Mutations that perturb normal pre-mRNA splicing are significant contributors to human disease. We used exome sequencing data from 7833 probands with developmental disorders (DDs) and their unaffected parents, as well as more than 60,000 aggregated exomes from the Exome Aggregation Consortium, to inv...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Cold Spring Harbor Laboratory Press
2019
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6360807/ https://www.ncbi.nlm.nih.gov/pubmed/30587507 http://dx.doi.org/10.1101/gr.238444.118 |
| _version_ | 1783392583484964864 |
|---|---|
| author | Lord, Jenny Gallone, Giuseppe Short, Patrick J. McRae, Jeremy F. Ironfield, Holly Wynn, Elizabeth H. Gerety, Sebastian S. He, Liu Kerr, Bronwyn Johnson, Diana S. McCann, Emma Kinning, Esther Flinter, Frances Temple, I. Karen Clayton-Smith, Jill McEntagart, Meriel Lynch, Sally Ann Joss, Shelagh Douzgou, Sofia Dabir, Tabib Clowes, Virginia McConnell, Vivienne P.M. Lam, Wayne Wright, Caroline F. FitzPatrick, David R. Firth, Helen V. Barrett, Jeffrey C. Hurles, Matthew E. |
| author_facet | Lord, Jenny Gallone, Giuseppe Short, Patrick J. McRae, Jeremy F. Ironfield, Holly Wynn, Elizabeth H. Gerety, Sebastian S. He, Liu Kerr, Bronwyn Johnson, Diana S. McCann, Emma Kinning, Esther Flinter, Frances Temple, I. Karen Clayton-Smith, Jill McEntagart, Meriel Lynch, Sally Ann Joss, Shelagh Douzgou, Sofia Dabir, Tabib Clowes, Virginia McConnell, Vivienne P.M. Lam, Wayne Wright, Caroline F. FitzPatrick, David R. Firth, Helen V. Barrett, Jeffrey C. Hurles, Matthew E. |
| author_sort | Lord, Jenny |
| collection | PubMed |
| description | Mutations that perturb normal pre-mRNA splicing are significant contributors to human disease. We used exome sequencing data from 7833 probands with developmental disorders (DDs) and their unaffected parents, as well as more than 60,000 aggregated exomes from the Exome Aggregation Consortium, to investigate selection around the splice sites and quantify the contribution of splicing mutations to DDs. Patterns of purifying selection, a deficit of variants in highly constrained genes in healthy subjects, and excess de novo mutations in patients highlighted particular positions within and around the consensus splice site of greater functional relevance. By using mutational burden analyses in this large cohort of proband–parent trios, we could estimate in an unbiased manner the relative contributions of mutations at canonical dinucleotides (73%) and flanking noncanonical positions (27%), and calculate the positive predictive value of pathogenicity for different classes of mutations. We identified 18 patients with likely diagnostic de novo mutations in dominant DD-associated genes at noncanonical positions in splice sites. We estimate 35%–40% of pathogenic variants in noncanonical splice site positions are missing from public databases. |
| format | Online Article Text |
| id | pubmed-6360807 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2019 |
| publisher | Cold Spring Harbor Laboratory Press |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-63608072019-02-25 Pathogenicity and selective constraint on variation near splice sites Lord, Jenny Gallone, Giuseppe Short, Patrick J. McRae, Jeremy F. Ironfield, Holly Wynn, Elizabeth H. Gerety, Sebastian S. He, Liu Kerr, Bronwyn Johnson, Diana S. McCann, Emma Kinning, Esther Flinter, Frances Temple, I. Karen Clayton-Smith, Jill McEntagart, Meriel Lynch, Sally Ann Joss, Shelagh Douzgou, Sofia Dabir, Tabib Clowes, Virginia McConnell, Vivienne P.M. Lam, Wayne Wright, Caroline F. FitzPatrick, David R. Firth, Helen V. Barrett, Jeffrey C. Hurles, Matthew E. Genome Res Research Mutations that perturb normal pre-mRNA splicing are significant contributors to human disease. We used exome sequencing data from 7833 probands with developmental disorders (DDs) and their unaffected parents, as well as more than 60,000 aggregated exomes from the Exome Aggregation Consortium, to investigate selection around the splice sites and quantify the contribution of splicing mutations to DDs. Patterns of purifying selection, a deficit of variants in highly constrained genes in healthy subjects, and excess de novo mutations in patients highlighted particular positions within and around the consensus splice site of greater functional relevance. By using mutational burden analyses in this large cohort of proband–parent trios, we could estimate in an unbiased manner the relative contributions of mutations at canonical dinucleotides (73%) and flanking noncanonical positions (27%), and calculate the positive predictive value of pathogenicity for different classes of mutations. We identified 18 patients with likely diagnostic de novo mutations in dominant DD-associated genes at noncanonical positions in splice sites. We estimate 35%–40% of pathogenic variants in noncanonical splice site positions are missing from public databases. Cold Spring Harbor Laboratory Press 2019-02 /pmc/articles/PMC6360807/ /pubmed/30587507 http://dx.doi.org/10.1101/gr.238444.118 Text en © 2019 Lord et al.; Published by Cold Spring Harbor Laboratory Press http://creativecommons.org/licenses/by/4.0/ This article, published in Genome Research, is available under a Creative Commons License (Attribution 4.0 International), as described at http://creativecommons.org/licenses/by/4.0/. |
| spellingShingle | Research Lord, Jenny Gallone, Giuseppe Short, Patrick J. McRae, Jeremy F. Ironfield, Holly Wynn, Elizabeth H. Gerety, Sebastian S. He, Liu Kerr, Bronwyn Johnson, Diana S. McCann, Emma Kinning, Esther Flinter, Frances Temple, I. Karen Clayton-Smith, Jill McEntagart, Meriel Lynch, Sally Ann Joss, Shelagh Douzgou, Sofia Dabir, Tabib Clowes, Virginia McConnell, Vivienne P.M. Lam, Wayne Wright, Caroline F. FitzPatrick, David R. Firth, Helen V. Barrett, Jeffrey C. Hurles, Matthew E. Pathogenicity and selective constraint on variation near splice sites |
| title | Pathogenicity and selective constraint on variation near splice sites |
| title_full | Pathogenicity and selective constraint on variation near splice sites |
| title_fullStr | Pathogenicity and selective constraint on variation near splice sites |
| title_full_unstemmed | Pathogenicity and selective constraint on variation near splice sites |
| title_short | Pathogenicity and selective constraint on variation near splice sites |
| title_sort | pathogenicity and selective constraint on variation near splice sites |
| topic | Research |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6360807/ https://www.ncbi.nlm.nih.gov/pubmed/30587507 http://dx.doi.org/10.1101/gr.238444.118 |
| work_keys_str_mv | AT lordjenny pathogenicityandselectiveconstraintonvariationnearsplicesites AT gallonegiuseppe pathogenicityandselectiveconstraintonvariationnearsplicesites AT shortpatrickj pathogenicityandselectiveconstraintonvariationnearsplicesites AT mcraejeremyf pathogenicityandselectiveconstraintonvariationnearsplicesites AT ironfieldholly pathogenicityandselectiveconstraintonvariationnearsplicesites AT wynnelizabethh pathogenicityandselectiveconstraintonvariationnearsplicesites AT geretysebastians pathogenicityandselectiveconstraintonvariationnearsplicesites AT heliu pathogenicityandselectiveconstraintonvariationnearsplicesites AT kerrbronwyn pathogenicityandselectiveconstraintonvariationnearsplicesites AT johnsondianas pathogenicityandselectiveconstraintonvariationnearsplicesites AT mccannemma pathogenicityandselectiveconstraintonvariationnearsplicesites AT kinningesther pathogenicityandselectiveconstraintonvariationnearsplicesites AT flinterfrances pathogenicityandselectiveconstraintonvariationnearsplicesites AT templeikaren pathogenicityandselectiveconstraintonvariationnearsplicesites AT claytonsmithjill pathogenicityandselectiveconstraintonvariationnearsplicesites AT mcentagartmeriel pathogenicityandselectiveconstraintonvariationnearsplicesites AT lynchsallyann pathogenicityandselectiveconstraintonvariationnearsplicesites AT jossshelagh pathogenicityandselectiveconstraintonvariationnearsplicesites AT douzgousofia pathogenicityandselectiveconstraintonvariationnearsplicesites AT dabirtabib pathogenicityandselectiveconstraintonvariationnearsplicesites AT clowesvirginia pathogenicityandselectiveconstraintonvariationnearsplicesites AT mcconnellviviennepm pathogenicityandselectiveconstraintonvariationnearsplicesites AT lamwayne pathogenicityandselectiveconstraintonvariationnearsplicesites AT wrightcarolinef pathogenicityandselectiveconstraintonvariationnearsplicesites AT fitzpatrickdavidr pathogenicityandselectiveconstraintonvariationnearsplicesites AT firthhelenv pathogenicityandselectiveconstraintonvariationnearsplicesites AT barrettjeffreyc pathogenicityandselectiveconstraintonvariationnearsplicesites AT hurlesmatthewe pathogenicityandselectiveconstraintonvariationnearsplicesites AT pathogenicityandselectiveconstraintonvariationnearsplicesites |