TY - JOUR
T1 - Clinical history and management recommendations of the smooth muscle dysfunction syndrome due to ACTA2 arginine 179 alterations
AU - Montalcino Aortic Consortium
AU - Regalado, Ellen S.
AU - Mellor-Crummey, Lauren
AU - De Backer, Julie
AU - Braverman, Alan C.
AU - Ades, Lesley
AU - Benedict, Susan
AU - Bradley, Timothy J.
AU - Brickner, M. Elizabeth
AU - Chatfield, Kathryn C.
AU - Child, Anne
AU - Feist, Cori
AU - Holmes, Kathryn W.
AU - Iannucci, Glen
AU - Lorenz, Birgit
AU - Mark, Paul
AU - Morisaki, Takayuki
AU - Morisaki, Hiroko
AU - Morris, Shaine A.
AU - Mitchell, Anna L.
AU - Ostergaard, John R.
AU - Richer, Julie
AU - Sallee, Denver
AU - Shalhub, Sherene
AU - Tekin, Mustafa
AU - Estrera, Anthony
AU - Musolino, Patricia
AU - Yetman, Anji
AU - Pyeritz, Reed
AU - Milewicz, Dianna M.
N1 - Publisher Copyright:
© 2018, American College of Medical Genetics and Genomics.
PY - 2018/10/1
Y1 - 2018/10/1
N2 - Purpose: Smooth muscle dysfunction syndrome (SMDS) due to heterozygous ACTA2 arginine 179 alterations is characterized by patent ductus arteriosus, vasculopathy (aneurysm and occlusive lesions), pulmonary arterial hypertension, and other complications in smooth muscle–dependent organs. We sought to define the clinical history of SMDS to develop recommendations for evaluation and management. Methods: Medical records of 33 patients with SMDS (median age 12 years) were abstracted and analyzed. Results: All patients had congenital mydriasis and related pupillary abnormalities at birth and presented in infancy with a patent ductus arteriosus or aortopulmonary window. Patients had cerebrovascular disease characterized by small vessel disease (hyperintense periventricular white matter lesions; 95%), intracranial artery stenosis (77%), ischemic strokes (27%), and seizures (18%). Twelve (36%) patients had thoracic aortic aneurysm repair or dissection at median age of 14 years and aortic disease was fully penetrant by the age of 25 years. Three (9%) patients had axillary artery aneurysms complicated by thromboembolic episodes. Nine patients died between the ages of 0.5 and 32 years due to aortic, pulmonary, or stroke complications, or unknown causes. Conclusion: Based on these data, recommendations are provided for the surveillance and management of SMDS to help prevent early-onset life-threatening complications.
AB - Purpose: Smooth muscle dysfunction syndrome (SMDS) due to heterozygous ACTA2 arginine 179 alterations is characterized by patent ductus arteriosus, vasculopathy (aneurysm and occlusive lesions), pulmonary arterial hypertension, and other complications in smooth muscle–dependent organs. We sought to define the clinical history of SMDS to develop recommendations for evaluation and management. Methods: Medical records of 33 patients with SMDS (median age 12 years) were abstracted and analyzed. Results: All patients had congenital mydriasis and related pupillary abnormalities at birth and presented in infancy with a patent ductus arteriosus or aortopulmonary window. Patients had cerebrovascular disease characterized by small vessel disease (hyperintense periventricular white matter lesions; 95%), intracranial artery stenosis (77%), ischemic strokes (27%), and seizures (18%). Twelve (36%) patients had thoracic aortic aneurysm repair or dissection at median age of 14 years and aortic disease was fully penetrant by the age of 25 years. Three (9%) patients had axillary artery aneurysms complicated by thromboembolic episodes. Nine patients died between the ages of 0.5 and 32 years due to aortic, pulmonary, or stroke complications, or unknown causes. Conclusion: Based on these data, recommendations are provided for the surveillance and management of SMDS to help prevent early-onset life-threatening complications.
KW - ACTA2
KW - congenital mydriasis
KW - patent ductus arteriosus
KW - smooth muscle dysfunction syndrome
KW - thoracic aortic aneurysm
UR - http://www.scopus.com/inward/record.url?scp=85054126014&partnerID=8YFLogxK
U2 - 10.1038/gim.2017.245
DO - 10.1038/gim.2017.245
M3 - Article
C2 - 29300374
AN - SCOPUS:85054126014
SN - 1098-3600
VL - 20
SP - 1206
EP - 1215
JO - Genetics in Medicine
JF - Genetics in Medicine
IS - 10
ER -