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The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa

BACKGROUND: Orofacial clefts are congenital malformations of the orofacial region, with a global incidence of one per 700 live births. Interferon Regulatory Factor 6 (IRF6) (OMIM:607199) gene has been associated with the etiology of both syndromic and nonsyndromic orofacial clefts. The aim of this s...

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Autores principales: Gowans, Lord Jephthah Joojo, Busch, Tamara D., Mossey, Peter A., Eshete, Mekonen A., Adeyemo, Wasiu L., Aregbesola, Babatunde, Donkor, Peter, Arthur, Fareed K. N., Agbenorku, Pius, Olutayo, James, Twumasi, Peter, Braimah, Rahman, Oti, Alexander A., Plange‐Rhule, Gyikua, Obiri‐Yeboah, Solomon, Abate, Fikre, Hoyte‐Williams, Paa E., Hailu, Taye, Murray, Jeffrey C., Butali, Azeez
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5370218/
https://www.ncbi.nlm.nih.gov/pubmed/28361103
http://dx.doi.org/10.1002/mgg3.273
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author Gowans, Lord Jephthah Joojo
Busch, Tamara D.
Mossey, Peter A.
Eshete, Mekonen A.
Adeyemo, Wasiu L.
Aregbesola, Babatunde
Donkor, Peter
Arthur, Fareed K. N.
Agbenorku, Pius
Olutayo, James
Twumasi, Peter
Braimah, Rahman
Oti, Alexander A.
Plange‐Rhule, Gyikua
Obiri‐Yeboah, Solomon
Abate, Fikre
Hoyte‐Williams, Paa E.
Hailu, Taye
Murray, Jeffrey C.
Butali, Azeez
author_facet Gowans, Lord Jephthah Joojo
Busch, Tamara D.
Mossey, Peter A.
Eshete, Mekonen A.
Adeyemo, Wasiu L.
Aregbesola, Babatunde
Donkor, Peter
Arthur, Fareed K. N.
Agbenorku, Pius
Olutayo, James
Twumasi, Peter
Braimah, Rahman
Oti, Alexander A.
Plange‐Rhule, Gyikua
Obiri‐Yeboah, Solomon
Abate, Fikre
Hoyte‐Williams, Paa E.
Hailu, Taye
Murray, Jeffrey C.
Butali, Azeez
author_sort Gowans, Lord Jephthah Joojo
collection PubMed
description BACKGROUND: Orofacial clefts are congenital malformations of the orofacial region, with a global incidence of one per 700 live births. Interferon Regulatory Factor 6 (IRF6) (OMIM:607199) gene has been associated with the etiology of both syndromic and nonsyndromic orofacial clefts. The aim of this study was to show evidence of potentially pathogenic variants in IRF6 in orofacial clefts cohorts from Africa. METHODS: We carried out Sanger Sequencing on DNA from 184 patients with nonsyndromic orofacial clefts and 80 individuals with multiple congenital anomalies that presented with orofacial clefts. We sequenced all the nine exons of IRF6 as well as the 5′ and 3′ untranslated regions. In our analyses pipeline, we used various bioinformatics tools to detect and describe the potentially etiologic variants. RESULTS: We observed that potentially etiologic exonic and splice site variants were nonrandomly distributed among the nine exons of IRF6, with 92% of these variants occurring in exons 4 and 7. Novel variants were also observed in both nonsyndromic orofacial clefts (p.Glu69Lys, p.Asn185Thr, c.175‐2A>C and c.1060+26C>T) and multiple congenital anomalies (p.Gly65Val, p.Lys320Asn and c.379+1G>T) patients. Our data also show evidence of compound heterozygotes that may modify phenotypes that emanate from IRF6 variants. CONCLUSIONS: This study demonstrates that exons 4 and 7 of IRF6 are mutational ‘hotspots’ in our cohort and that IRF6 mutants‐induced orofacial clefts may be prevalent in the Africa population, however, with variable penetrance and expressivity. These observations are relevant for detection of high‐risk families as well as genetic counseling. In conclusion, we have shown that there may be a need to combine both molecular and clinical evidence in the grouping of orofacial clefts into syndromic and nonsyndromic forms.
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spelling pubmed-53702182017-03-30 The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa Gowans, Lord Jephthah Joojo Busch, Tamara D. Mossey, Peter A. Eshete, Mekonen A. Adeyemo, Wasiu L. Aregbesola, Babatunde Donkor, Peter Arthur, Fareed K. N. Agbenorku, Pius Olutayo, James Twumasi, Peter Braimah, Rahman Oti, Alexander A. Plange‐Rhule, Gyikua Obiri‐Yeboah, Solomon Abate, Fikre Hoyte‐Williams, Paa E. Hailu, Taye Murray, Jeffrey C. Butali, Azeez Mol Genet Genomic Med Original Articles BACKGROUND: Orofacial clefts are congenital malformations of the orofacial region, with a global incidence of one per 700 live births. Interferon Regulatory Factor 6 (IRF6) (OMIM:607199) gene has been associated with the etiology of both syndromic and nonsyndromic orofacial clefts. The aim of this study was to show evidence of potentially pathogenic variants in IRF6 in orofacial clefts cohorts from Africa. METHODS: We carried out Sanger Sequencing on DNA from 184 patients with nonsyndromic orofacial clefts and 80 individuals with multiple congenital anomalies that presented with orofacial clefts. We sequenced all the nine exons of IRF6 as well as the 5′ and 3′ untranslated regions. In our analyses pipeline, we used various bioinformatics tools to detect and describe the potentially etiologic variants. RESULTS: We observed that potentially etiologic exonic and splice site variants were nonrandomly distributed among the nine exons of IRF6, with 92% of these variants occurring in exons 4 and 7. Novel variants were also observed in both nonsyndromic orofacial clefts (p.Glu69Lys, p.Asn185Thr, c.175‐2A>C and c.1060+26C>T) and multiple congenital anomalies (p.Gly65Val, p.Lys320Asn and c.379+1G>T) patients. Our data also show evidence of compound heterozygotes that may modify phenotypes that emanate from IRF6 variants. CONCLUSIONS: This study demonstrates that exons 4 and 7 of IRF6 are mutational ‘hotspots’ in our cohort and that IRF6 mutants‐induced orofacial clefts may be prevalent in the Africa population, however, with variable penetrance and expressivity. These observations are relevant for detection of high‐risk families as well as genetic counseling. In conclusion, we have shown that there may be a need to combine both molecular and clinical evidence in the grouping of orofacial clefts into syndromic and nonsyndromic forms. John Wiley and Sons Inc. 2017-01-12 /pmc/articles/PMC5370218/ /pubmed/28361103 http://dx.doi.org/10.1002/mgg3.273 Text en © 2017 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc. This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Gowans, Lord Jephthah Joojo
Busch, Tamara D.
Mossey, Peter A.
Eshete, Mekonen A.
Adeyemo, Wasiu L.
Aregbesola, Babatunde
Donkor, Peter
Arthur, Fareed K. N.
Agbenorku, Pius
Olutayo, James
Twumasi, Peter
Braimah, Rahman
Oti, Alexander A.
Plange‐Rhule, Gyikua
Obiri‐Yeboah, Solomon
Abate, Fikre
Hoyte‐Williams, Paa E.
Hailu, Taye
Murray, Jeffrey C.
Butali, Azeez
The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa
title The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa
title_full The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa
title_fullStr The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa
title_full_unstemmed The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa
title_short The prevalence, penetrance, and expressivity of etiologic IRF6 variants in orofacial clefts patients from sub‐Saharan Africa
title_sort prevalence, penetrance, and expressivity of etiologic irf6 variants in orofacial clefts patients from sub‐saharan africa
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5370218/
https://www.ncbi.nlm.nih.gov/pubmed/28361103
http://dx.doi.org/10.1002/mgg3.273
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