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Heterozygous mutations of FREM1 are associated with an increased risk of isolated metopic craniosynostosis in humans and mice
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نویسنده
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vissers l.e.l.m. ,cox t.c. ,maga a.m. ,short k.m. ,wiradjaja f. ,janssen i.m. ,jehee f. ,bertola d. ,liu j. ,yagnik g. ,sekiguchi k. ,kiyozumi d. ,van bokhoven h. ,marcelis c. ,cunningham m.l. ,anderson p.j. ,boyadjiev s.a. ,passos-bueno m.r. ,veltman j.a. ,smyth i. ,buckley m.f. ,roscioli t.
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منبع
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plos genetics - 2011 - دوره : 7 - شماره : 9
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چکیده
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The premature fusion of the paired frontal bones results in metopic craniosynostosis (mc) and gives rise to the clinical phenotype of trigonocephaly. deletions of chromosome 9p22.3 are well described as a cause of mc with variably penetrant midface hypoplasia. in order to identify the gene responsible for the trigonocephaly component of the 9p22.3 syndrome,a cohort of 109 patients were assessed by high-resolution arrays and mlpa for copy number variations (cnvs) involving 9p22. five cnvs involving frem1,all of which were de novo variants,were identified by array-based analyses. the remaining 104 patients with mc were then subjected to targeted frem1 gene re-sequencing,which identified 3 further mutant alleles,one of which was de novo. consistent with a pathogenic role,mouse frem1 mrna and protein expression was demonstrated in the metopic suture as well as in the pericranium and dura mater. micro-computed tomography based analyses of the mouse posterior frontal (pf) suture,the human metopic suture equivalent,revealed advanced fusion in all mice homozygous for either of two different frem1 mutant alleles,while heterozygotes exhibited variably penetrant pf suture anomalies. gene dosage-related penetrance of midfacial hypoplasia was also evident in the frem1 mutants. these data suggest that cnvs and mutations involving frem1 can be identified in a significant percentage of people with mc with or without midface hypoplasia. furthermore,we present frem1 mutant mice as the first bona fide mouse model of human metopic craniosynostosis and a new model for midfacial hypoplasia. © 2011 vissers et al.
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آدرس
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department of human genetics,nijmegen centre for molecular life sciences,radboud university nijmegen medical centre,nijmegen, Netherlands, division of craniofacial medicine,department of pediatrics,university of washington,seattle,wa,united states,department of anatomy and developmental biology,monash university,clayton, Australia, division of craniofacial medicine,department of pediatrics,university of washington,seattle,wa, United States, department of biochemistry and molecular biology,monash university,clayton, Australia, department of biochemistry and molecular biology,monash university,clayton, Australia, department of human genetics,nijmegen centre for molecular life sciences,radboud university nijmegen medical centre,nijmegen, Netherlands, centro de estudos do genoma humano,instituto de biociências,universidade de são paulo,são paulo, Brazil, centro de estudos do genoma humano,instituto de biociências,universidade de são paulo,são paulo, Brazil, section of genetics,department of pediatrics,university of california davis,sacramento,ca, United States, section of genetics,department of pediatrics,university of california davis,sacramento,ca, United States, institute for protein research,osaka university,osaka, Japan, institute for protein research,osaka university,osaka, Japan, department of human genetics,nijmegen centre for molecular life sciences,radboud university nijmegen medical centre,nijmegen,netherlands,donders institute for brain,imaging,and cognition,nijmegen, Netherlands, department of human genetics,nijmegen centre for molecular life sciences,radboud university nijmegen medical centre,nijmegen, Netherlands, division of craniofacial medicine,department of pediatrics,university of washington,seattle,wa, United States, australian craniofacial unit,women and children's hospital,adelaide, Australia, section of genetics,department of pediatrics,university of california davis,sacramento,ca, United States, centro de estudos do genoma humano,instituto de biociências,universidade de são paulo,são paulo, Brazil, department of human genetics,nijmegen centre for molecular life sciences,radboud university nijmegen medical centre,nijmegen, Netherlands, department of anatomy and developmental biology,monash university,clayton,australia,department of biochemistry and molecular biology,monash university,clayton, Australia, department of human genetics,nijmegen centre for molecular life sciences,radboud university nijmegen medical centre,nijmegen,netherlands,department of haematology and genetics,south-eastern area laboratory services,prince of wales and sydney children's hospitals,randwick, Australia, department of human genetics,nijmegen centre for molecular life sciences,radboud university nijmegen medical centre,nijmegen,netherlands,sydney south west genetic service,royal prince alfred hospital,sydney university,sydney, Australia
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Authors
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