Twenty patients including 7 probands with autosomal dominant cutis laxa confirm clinical and molecular homogeneity

Smail Hadj-Rabia; Bert L. Callewaert; Emmanuelle Bourrat; Marlies Kempers; Astrid S. Plomp; Valerie Layet; Deborah Bartholdi; Marjolijn Renard; Julie de Backer; Fransiska Malfait; Olivier M. Vanakker; Paul J. Coucke; Anne M. de Paepe; Christine Bodemer

doi:https://doi.org/10.1186/1750-1172-8-36

Twenty patients including 7 probands with autosomal dominant cutis laxa confirm clinical and molecular homogeneity

Smail Hadj-Rabia, Bert L. Callewaert, Emmanuelle Bourrat, Marlies Kempers, Astrid S. Plomp, Valerie Layet, Deborah Bartholdi, Marjolijn Renard, Julie de Backer, Fransiska Malfait, Olivier M. Vanakker, Paul J. Coucke, Anne M. de Paepe, Christine Bodemer

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

26 Citations (Scopus)

Abstract

Elastin gene mutations have been associated with a variety of phenotypes. Autosomal dominant cutis laxa (ADCL) is a rare disorder that presents with lax skin, typical facial characteristics, inguinal hernias, aortic root dilatation and pulmonary emphysema. In most patients, frameshift mutations are found in the 3' region of the elastin gene (exons 30-34) which result in a C-terminally extended protein, though exceptions have been reported. We clinically and molecularly characterized the thus far largest cohort of ADCL patients, consisting of 19 patients from six families and one sporadic patient. Molecular analysis showed C-terminal frameshift mutations in exon 30, 32, and 34 of the elastin gene and identified a mutational hotspot in exon 32 (c.2262delA). This cohort confirms the previously reported clinical constellation of skin laxity (100%), inguinal hernias (51%), aortic root dilatation (55%) and emphysema (37%). ADCL is a clinically and molecularly homogeneous disorder, but intra- and interfamilial variability in the severity of organ involvement needs to be taken into account. Regular cardiovascular and pulmonary evaluations are imperative in the clinical follow-up of these patients

Original language	English
Pages (from-to)	36
Journal	Orphanet Journal of Rare Diseases
Volume	8
Issue number	1
DOIs	https://doi.org/10.1186/1750-1172-8-36
Publication status	Published - 2013

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https://doi.org/10.1186/1750-1172-8-36

Cite this

Hadj-Rabia, S., Callewaert, B. L., Bourrat, E., Kempers, M., Plomp, A. S., Layet, V., Bartholdi, D., Renard, M., de Backer, J., Malfait, F., Vanakker, O. M., Coucke, P. J., de Paepe, A. M., & Bodemer, C. (2013). Twenty patients including 7 probands with autosomal dominant cutis laxa confirm clinical and molecular homogeneity. Orphanet Journal of Rare Diseases, 8(1), 36. https://doi.org/10.1186/1750-1172-8-36

@article{adf44005ca424774b18f3d4e2ec50848,

title = "Twenty patients including 7 probands with autosomal dominant cutis laxa confirm clinical and molecular homogeneity",

abstract = "Elastin gene mutations have been associated with a variety of phenotypes. Autosomal dominant cutis laxa (ADCL) is a rare disorder that presents with lax skin, typical facial characteristics, inguinal hernias, aortic root dilatation and pulmonary emphysema. In most patients, frameshift mutations are found in the 3' region of the elastin gene (exons 30-34) which result in a C-terminally extended protein, though exceptions have been reported. We clinically and molecularly characterized the thus far largest cohort of ADCL patients, consisting of 19 patients from six families and one sporadic patient. Molecular analysis showed C-terminal frameshift mutations in exon 30, 32, and 34 of the elastin gene and identified a mutational hotspot in exon 32 (c.2262delA). This cohort confirms the previously reported clinical constellation of skin laxity (100%), inguinal hernias (51%), aortic root dilatation (55%) and emphysema (37%). ADCL is a clinically and molecularly homogeneous disorder, but intra- and interfamilial variability in the severity of organ involvement needs to be taken into account. Regular cardiovascular and pulmonary evaluations are imperative in the clinical follow-up of these patients",

author = "Smail Hadj-Rabia and Callewaert, {Bert L.} and Emmanuelle Bourrat and Marlies Kempers and Plomp, {Astrid S.} and Valerie Layet and Deborah Bartholdi and Marjolijn Renard and {de Backer}, Julie and Fransiska Malfait and Vanakker, {Olivier M.} and Coucke, {Paul J.} and {de Paepe}, {Anne M.} and Christine Bodemer",

year = "2013",

doi = "https://doi.org/10.1186/1750-1172-8-36",

language = "English",

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journal = "Orphanet Journal of Rare Diseases",

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publisher = "BioMed Central",

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Hadj-Rabia, S, Callewaert, BL, Bourrat, E, Kempers, M, Plomp, AS, Layet, V, Bartholdi, D, Renard, M, de Backer, J, Malfait, F, Vanakker, OM, Coucke, PJ, de Paepe, AM & Bodemer, C 2013, 'Twenty patients including 7 probands with autosomal dominant cutis laxa confirm clinical and molecular homogeneity', Orphanet Journal of Rare Diseases, vol. 8, no. 1, pp. 36. https://doi.org/10.1186/1750-1172-8-36

TY - JOUR

T1 - Twenty patients including 7 probands with autosomal dominant cutis laxa confirm clinical and molecular homogeneity

AU - Hadj-Rabia, Smail

AU - Callewaert, Bert L.

AU - Bourrat, Emmanuelle

AU - Kempers, Marlies

AU - Plomp, Astrid S.

AU - Layet, Valerie

AU - Bartholdi, Deborah

AU - Renard, Marjolijn

AU - de Backer, Julie

AU - Malfait, Fransiska

AU - Vanakker, Olivier M.

AU - Coucke, Paul J.

AU - de Paepe, Anne M.

AU - Bodemer, Christine

PY - 2013

Y1 - 2013

N2 - Elastin gene mutations have been associated with a variety of phenotypes. Autosomal dominant cutis laxa (ADCL) is a rare disorder that presents with lax skin, typical facial characteristics, inguinal hernias, aortic root dilatation and pulmonary emphysema. In most patients, frameshift mutations are found in the 3' region of the elastin gene (exons 30-34) which result in a C-terminally extended protein, though exceptions have been reported. We clinically and molecularly characterized the thus far largest cohort of ADCL patients, consisting of 19 patients from six families and one sporadic patient. Molecular analysis showed C-terminal frameshift mutations in exon 30, 32, and 34 of the elastin gene and identified a mutational hotspot in exon 32 (c.2262delA). This cohort confirms the previously reported clinical constellation of skin laxity (100%), inguinal hernias (51%), aortic root dilatation (55%) and emphysema (37%). ADCL is a clinically and molecularly homogeneous disorder, but intra- and interfamilial variability in the severity of organ involvement needs to be taken into account. Regular cardiovascular and pulmonary evaluations are imperative in the clinical follow-up of these patients

AB - Elastin gene mutations have been associated with a variety of phenotypes. Autosomal dominant cutis laxa (ADCL) is a rare disorder that presents with lax skin, typical facial characteristics, inguinal hernias, aortic root dilatation and pulmonary emphysema. In most patients, frameshift mutations are found in the 3' region of the elastin gene (exons 30-34) which result in a C-terminally extended protein, though exceptions have been reported. We clinically and molecularly characterized the thus far largest cohort of ADCL patients, consisting of 19 patients from six families and one sporadic patient. Molecular analysis showed C-terminal frameshift mutations in exon 30, 32, and 34 of the elastin gene and identified a mutational hotspot in exon 32 (c.2262delA). This cohort confirms the previously reported clinical constellation of skin laxity (100%), inguinal hernias (51%), aortic root dilatation (55%) and emphysema (37%). ADCL is a clinically and molecularly homogeneous disorder, but intra- and interfamilial variability in the severity of organ involvement needs to be taken into account. Regular cardiovascular and pulmonary evaluations are imperative in the clinical follow-up of these patients

U2 - https://doi.org/10.1186/1750-1172-8-36

DO - https://doi.org/10.1186/1750-1172-8-36

M3 - Article

C2 - 23442826

SN - 1750-1172

VL - 8

SP - 36

JO - Orphanet Journal of Rare Diseases

JF - Orphanet Journal of Rare Diseases

IS - 1

ER -