Boston type craniosynostosis: report of a second mutation in MSX2

Joyce M G Florisson; Annemieke J M H Verkerk; Daphne Huigh; A Jeannette M Hoogeboom; Sigrid Swagemakers; Andreas Kremer; Daphne Heijsman; Maarten H Lequin; Irene M J Mathijssen; Peter J van der Spek

doi:10.1002/ajmg.a.36126

Boston type craniosynostosis: report of a second mutation in MSX2

Joyce M G Florisson^*, Annemieke J M H Verkerk, Daphne Huigh, A Jeannette M Hoogeboom, Sigrid Swagemakers, Andreas Kremer, Daphne Heijsman, Maarten H Lequin, Irene M J Mathijssen, Peter J van der Spek

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

25 Citations (Scopus)

Abstract

We describe a family that segregated an autosomal dominant form of craniosynostosis characterized by variable expression and limited extra-cranial features. Linkage analysis and genome sequencing were performed to identify the underlying genetic mutation. A c.443C>T missense mutation in MSX2, which predicts p.Pro148Leu was identified and segregated with the disease in all affected family members. One other family with autosomal dominant craniosynostosis (Boston type) has been reported to have a missense mutation in MSX2. These data confirm that missense mutations altering the proline at codon 148 of MSX2 cause dominantly inherited craniosynostosis.

Original language	English
Pages (from-to)	2626-2633
Number of pages	8
Journal	American Journal of Medical Genetics Part A
Volume	161
Issue number	10
DOIs	https://doi.org/10.1002/ajmg.a.36126
Publication status	Published - Oct 2013

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title = "Boston type craniosynostosis: report of a second mutation in MSX2",

abstract = "We describe a family that segregated an autosomal dominant form of craniosynostosis characterized by variable expression and limited extra-cranial features. Linkage analysis and genome sequencing were performed to identify the underlying genetic mutation. A c.443C>T missense mutation in MSX2, which predicts p.Pro148Leu was identified and segregated with the disease in all affected family members. One other family with autosomal dominant craniosynostosis (Boston type) has been reported to have a missense mutation in MSX2. These data confirm that missense mutations altering the proline at codon 148 of MSX2 cause dominantly inherited craniosynostosis.",

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AU - Huigh, Daphne

AU - Hoogeboom, A Jeannette M

AU - Swagemakers, Sigrid

AU - Kremer, Andreas

AU - Heijsman, Daphne

AU - Lequin, Maarten H

AU - Mathijssen, Irene M J

AU - van der Spek, Peter J

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AB - We describe a family that segregated an autosomal dominant form of craniosynostosis characterized by variable expression and limited extra-cranial features. Linkage analysis and genome sequencing were performed to identify the underlying genetic mutation. A c.443C>T missense mutation in MSX2, which predicts p.Pro148Leu was identified and segregated with the disease in all affected family members. One other family with autosomal dominant craniosynostosis (Boston type) has been reported to have a missense mutation in MSX2. These data confirm that missense mutations altering the proline at codon 148 of MSX2 cause dominantly inherited craniosynostosis.

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Boston type craniosynostosis: report of a second mutation in MSX2

Abstract

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