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Cardiac features of Noonan syndrome in Japanese patients

Authors :
Yasuhiro Ichikawa
Hiroyuki Kuroda
Takeshi Ikegawa
Shun Kawai
Shin Ono
Ki-Sung Kim
Sadamitsu Yanagi
Kenji Kurosawa
Yoko Aoki
Hideaki Ueda
Source :
Cardiology in the Young. 33:564-569
Publication Year :
2022
Publisher :
Cambridge University Press (CUP), 2022.

Abstract

Background:Cardiovascular disease is one of the most important problems in long-term follow-up for Noonan syndrome. We examined cardiovascular issues and clinical manifestations, with a focus on the cardiovascular disease and prognosis of patients with Noonan syndrome.Methods:This single-centre study evaluated patients who were clinically and genetically diagnosed with Noonan syndrome.Results:Forty-three patients diagnosed with Noonan syndrome were analysed. The most prevalent responsible mutation was found in PTPN11 (25/43). The second and third most prevalent causative genes were SOS1 (6/43) and RIT1 (5/43), respectively, and 67.4% of genetically diagnosed patients with Noonan syndrome had structural cardiovascular abnormalities. Pulmonary valve stenosis was prevalent in patients with mutations in PTPN11 (8/25), SOS1 (4/6), and RIT1 (4/5). Hypertrophic cardiomyopathy was found in two of three patients with mutations in RAF1. There was no difference in the cardiovascular events or cardiovascular disease prevalence in patients with or without PTPN11 mutations. The proportion of RIT1 mutation-positive patients who underwent intervention due to cardiovascular disease was significantly higher than that of patients with PTPN11 mutations. Patients who underwent any intervention for pulmonary valve stenosis exhibited significantly higher pulmonary flow velocity than patients who did not undergo intervention, when they visited our hospital for the first time. All patients who underwent intervention for pulmonary valve stenosis had a pulmonary flow velocity of more than 3.0 m/s at first visit.Conclusions:These findings suggest that genetic information can provide a clinical prognosis for cardiovascular disease and may be part of genotype-based follow-up in Noonan syndrome.

Details

ISSN :
14671107 and 10479511
Volume :
33
Database :
OpenAIRE
Journal :
Cardiology in the Young
Accession number :
edsair.doi.dedup.....f4ad669896e1925125f73441183e5db2
Full Text :
https://doi.org/10.1017/s104795112200124x