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Absence of Cardiovascular Manifestations in a Haploinsufficient Tgfbr1 Mouse Model

Authors :
Renard, M
Trachet, B
Casteleyn, C
Campens, L
Cornillie, P
Callewaert, B
Deleye, S
Vandeghinste, B
Heijningen, Paula
Dietz, H
Vos, F
Essers, J.
Staelens, S
Segers, P
Loeys, B
Coucke, P
de Paepe, A
Backer, J
Renard, M
Trachet, B
Casteleyn, C
Campens, L
Cornillie, P
Callewaert, B
Deleye, S
Vandeghinste, B
Heijningen, Paula
Dietz, H
Vos, F
Essers, J.
Staelens, S
Segers, P
Loeys, B
Coucke, P
de Paepe, A
Backer, J
Source :
Renard , M , Trachet , B , Casteleyn , C , Campens , L , Cornillie , P , Callewaert , B , Deleye , S , Vandeghinste , B , Heijningen , P , Dietz , H , Vos , F , Essers , J , Staelens , S , Segers , P , Loeys , B , Coucke , P , de Paepe , A & Backer , J 2014 , ' Absence of Cardiovascular Manifestations in a Haploinsufficient Tgfbr1 Mouse Model ' , PLoS One (print) , vol. 9 , no. 2 .
Publication Year :
2014

Abstract

Loeys-Dietz syndrome (LDS) is an autosomal dominant arterial aneurysm disease belonging to the spectrum of transforming growth factor beta (TGF beta)-associated vasculopathies. In its most typical form it is characterized by the presence of hypertelorism, bifid uvula/cleft palate and aortic aneurysm and/or arterial tortuosity. LDS is caused by heterozygous loss of function mutations in the genes encoding TGF beta receptor 1 and 2 (TGFBR1 and -2), which lead to a paradoxical increase in TGF beta signaling. To address this apparent paradox and to gain more insight into the pathophysiology of aneurysmal disease, we characterized a new Tgfbr1 mouse model carrying a p.Y378* nonsense mutation. Study of the natural history in this model showed that homozygous mutant mice die during embryonic development due to defective vascularization. Heterozygous mutant mice aged 6 and 12 months were morphologically and (immuno) histochemically indistinguishable from wild-type mice. We show that the mutant allele is degraded by nonsense mediated mRNA decay, expected to result in haploinsufficiency of the mutant allele. Since this haploinsufficiency model does not result in cardiovascular malformations, it does not allow further study of the process of aneurysm formation. In addition to providing a comprehensive method for cardiovascular phenotyping in mice, the results of this study confirm that haploinsuffciency is not the underlying genetic mechanism in human LDS.

Details

Database :
OAIster
Journal :
Renard , M , Trachet , B , Casteleyn , C , Campens , L , Cornillie , P , Callewaert , B , Deleye , S , Vandeghinste , B , Heijningen , P , Dietz , H , Vos , F , Essers , J , Staelens , S , Segers , P , Loeys , B , Coucke , P , de Paepe , A & Backer , J 2014 , ' Absence of Cardiovascular Manifestations in a Haploinsufficient Tgfbr1 Mouse Model ' , PLoS One (print) , vol. 9 , no. 2 .
Notes :
application/pdf, und
Publication Type :
Electronic Resource
Accession number :
edsoai.on1313618331
Document Type :
Electronic Resource