Citations to this article
Citation Information: J Clin Invest. 2004;114(2):172-181. https://doi.org/10.1172/JCI20641.
Abstract
Marfan syndrome is a connective tissue disorder caused by mutations in the gene encoding fibrillin-1 (FBN1). A dominant-negative mechanism has been inferred based upon dominant inheritance, mulitimerization of monomers to form microfibrils, and the dramatic paucity of matrix-incorporated fibrillin-1 seen in heterozygous patient samples. Yeast artificial chromosome–based transgenesis was used to overexpress a disease-associated mutant form of human fibrillin-1 (C1663R) on a normal mouse background. Remarkably, these mice failed to show any abnormalities of cellular or clinical phenotype despite regulated overexpression of mutant protein in relevant tissues and developmental stages and direct evidence that mouse and human fibrillin-1 interact with high efficiency. Immunostaining with a human-specific mAb provides what we believe to be the first demonstration that mutant fibrillin-1 can participate in productive microfibrillar assembly. Informatively, use of homologous recombination to generate mice heterozygous for a comparable missense mutation (C1039G) revealed impaired microfibrillar deposition, skeletal deformity, and progressive deterioration of aortic wall architecture, comparable to characteristics of the human condition. These data are consistent with a model that invokes haploinsufficiency for WT fibrillin-1, rather than production of mutant protein, as the primary determinant of failed microfibrillar assembly. In keeping with this model, introduction of a WT FBN1 transgene on a heterozygous C1039G background rescues aortic phenotype.
Authors
Daniel P. Judge, Nancy J. Biery, Douglas R. Keene, Jessica Geubtner, Loretha Myers, David L. Huso, Lynn Y. Sakai, Harry C. Dietz
Total citations by year
Citations to this article in year 2017 (13)
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Nature Medicine | 2017 |
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Aortic Aneurysms
H Lu, A Daugherty |
Arteriosclerosis, thrombosis, and vascular biology | 2017 |
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Premature aortic smooth muscle cell differentiation contributes to matrix dysregulation in Marfan Syndrome
M Dale, MP Fitzgerald, Z Liu, T Meisinger, A Karpisek, LN Purcell, JS Carson, P Harding, H Lang, P Koutakis, R Batra, CJ Mietus, G Casale, I Pipinos, BT Baxter, W Xiong, LV Pereira |
PloS one | 2017 |
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A Novel Murine Model of Marfan Syndrome Accelerates Aortopathy and Cardiomyopathy
NB Cavanaugh, L Qian, NM Westergaard, WJ Kutschke, EJ Born, JW Turek |
The Annals of Thoracic Surgery | 2017 |
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Establishment of DNA methylation patterns of the Fibrillin1 (FBN1) gene in porcine embryos and tissues
Y ARAI, K UMEYAMA, K TAKEUCHI, N OKAZAKI, N HICHIWA, S YASHIMA, K NAKANO, H NAGASHIMA, J OHGANE |
Journal of Reproduction and Development | 2017 |
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High-Resolution Morphological Approach to Analyse Elastic Laminae Injuries of the Ascending Aorta in a Murine Model of Marfan Syndrome
J López-Guimet, J Andilla, P Loza-Alvarez, G Egea |
Scientific Reports | 2017 |
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Sex, pregnancy and aortic disease in Marfan syndrome
M Renard, L Muiño-Mosquera, EC Manalo, S Tufa, EJ Carlson, DR Keene, JD Backer, LY Sakai, M Bader |
PloS one | 2017 |
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Aortopathy in a Mouse Model of Marfan Syndrome Is Not Mediated by Altered Transforming Growth Factor β Signaling
H Wei, JH Hu, SN Angelov, K Fox, J Yan, R Enstrom, A Smith, DA Dichek |
Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease | 2017 |
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Cardiovascular Benefits of Moderate Exercise Training in Marfan Syndrome: Insights From an Animal Model
A MasStachurska, AM Siegert, M Batlle, DG Blanco, T Meirelles, C Rubies, F Bonorino, C SerraPeinado, B Bijnens, J Baudin, M Sitges, L Mont, E Guasch, G Egea |
Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease | 2017 |
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Moderately Elevated Homocysteine Does Not Contribute to Thoracic Aortic Aneurysm in Mice
J Roohi, B Kang, D Bernard, D Bedja, HC Dietz, LC Brody |
The Journal of nutrition | 2017 |
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Differences in the Thoracic Aorta by Region and Sex in a Murine Model of Marfan Syndrome
F Jiménez-Altayó, AM Siegert, F Bonorino, T Meirelles, L Barberà, AP Dantas, E Vila, G Egea |
Frontiers in physiology | 2017 |
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