Two Patients with the Heterozygous R189H Mutation in <i>ACTA2</i> and Complex Congenital Heart Defects Expands the Cardiac Phenotype of Multisystemic Smooth Muscle Dysfunction Syndrome - Forschungsportal der Justus-Liebig-Universität Gießen:

Journalartikel

Two Patients with the Heterozygous R189H Mutation in ACTA2 and Complex Congenital Heart Defects Expands the Cardiac Phenotype of Multisystemic Smooth Muscle Dysfunction Syndrome

Autorenliste: Logeswaran, Thushiha; Friedburg, Christoph; Hofmann, Karoline; Akintuerk, Hakan; Biskup, Saskia; Graef, Michael; Rad, Ali; Weber, Axel; Neubauer, Bernd A.; Schranz, Dietmar; Bouvagnet, Patrice; Lorenz, Birgit; Hahn, Andreas

Jahr der Veröffentlichung: 2017

Seiten: 959-965

Zeitschrift: The American Journal of Medical Genetics - Part A

Bandnummer: 173

Heftnummer: 4

ISSN: 1552-4825

eISSN: 1552-4833

DOI Link: https://doi.org/10.1002/ajmg.a.38102

Verlag: Wiley

Abstract:
De novo heterozygous mutations changing R179 to histidine, leucine, or cysteine in the ACTA2 gene are associated with Multisystemic Smooth Muscle Dysfunction Syndrome (MSMDS). Characteristic hallmarks of this condition, caused only by these specific ACTA2 mutations, are congenital mydriasis (mid-dilated, non-reactive pupils), a large persistent ductus arteriosus (PDA), aortic aneurysms evolving during childhood, and cerebrovascular anomalies. We describe two patients, a 3-day-old newborn and a 26-year-old woman, with this unique mutation in association with a huge PDA and an aorto-pulmonary window. In addition, one showed a coarctation of the aortic arch and the other a complete interruption of the aortic arch type A; thereby expanding the spectrum of cardiac congenital heart defect of this syndrome. Each patient displayed a huge PDA and an extra-cardiovascular phenotype consistent with MSMDS. These observations exemplify that a functional alpha 2 smooth muscle actin is necessary for proper cardiovascular organ development, and demonstrate that a very exceptional congenital heart defect (aortopulmonary window) can be caused by a mutation in a gene encoding a contractile protein of vascular smooth muscle cells. (C) 2017 Wiley Periodicals, Inc.

Zitierstile

Harvard-Zitierstil: Logeswaran, T., Friedburg, C., Hofmann, K., Akintuerk, H., Biskup, S., Graef, M., et al. (2017) Two Patients with the Heterozygous R189H Mutation in ACTA2 and Complex Congenital Heart Defects Expands the Cardiac Phenotype of Multisystemic Smooth Muscle Dysfunction Syndrome, The American Journal of Medical Genetics - Part A, 173(4), pp. 959-965. https://doi.org/10.1002/ajmg.a.38102

APA-Zitierstil: Logeswaran, T., Friedburg, C., Hofmann, K., Akintuerk, H., Biskup, S., Graef, M., Rad, A., Weber, A., Neubauer, B., Schranz, D., Bouvagnet, P., Lorenz, B., & Hahn, A. (2017). Two Patients with the Heterozygous R189H Mutation in ACTA2 and Complex Congenital Heart Defects Expands the Cardiac Phenotype of Multisystemic Smooth Muscle Dysfunction Syndrome. The American Journal of Medical Genetics - Part A. 173(4), 959-965. https://doi.org/10.1002/ajmg.a.38102

Schlagwörter

ACTA2; aortic arch coarctation; AORTOPULMONARY SEPTAL-DEFECT; aortopulmonary window; congenital mydriasis; DISSECTIONS; interrupted aortic arch; pupil dysfunction; R179H; syndrome of generalized smooth muscle dysfunction; THORACIC AORTIC-ANEURYSMS

Nachhaltigkeitsbezüge

3 Gesundheit und Wohlergehen