Sarcomere gene variants did not improve cardiac function in pediatric patients with dilated cardiomyopathy from Japanese cohorts
Author:
Hirono KeiichiORCID, Hata Yukiko, Ichimata Shojiro, Nishida NaokiORCID, Imamura TeruhikoORCID, Asano Yoshihiro, Kuramoto YukiORCID, Tsuboi Kaori, Takarada Shinya, Okabe Mako, Nakaoka Hideyuki, Ibuki Keijiro, Ozawa Sayaka, Muneuchi JunORCID, Yasuda KazushiORCID, Urayama Kotaro, Oka HideharuORCID, Miyamoto Tomoyuki, Baba Kenji, Kato Akio, Saiki Hirofumi, Kuwahara Naoki, Harada Masako, Baba ShiroORCID, Morikawa Mari, Iwasaki Hidenori, Hirata Yuichiro, Ito Yuki, Sakaguchi Heima, Urata Susumu, Toda Koichi, Kittaka Emi, Okagda Seigo, Hasebe Yohei, Hoshino ShinsukeORCID, Fujii Takanari, Mitsushita Norie, Nii MasakiORCID, Ogino Kayo, Fujino Mitsuhiro, Yoshida Yoko, Fukuda Yutaka, Iwashima SatoruORCID, Takigiku Kiyohiro, Sakata Yasushi, Inuzuka RyoORCID, Maeda JunORCID, Hayabuchi YasunobuORCID, Fujioka Tao, Namiki Hidemasa, Fujita ShuheiORCID, Nishida Koichi, Kuraoka Ayako, Kan Nobuhiko, Kido Sachiko, Watanabe Ken, Ichida FukikoORCID
Abstract
AbstractBackgroundDilated cardiomyopathy (DCM) is a progressive myocardial disorder characterized by impaired cardiac contraction and ventricular dilation. Some patients with DCM could manifest improvement in these abnormalities called left ventricular reverse remodeling (LVRR). However, the detailed association between genotypes and clinical outcomes, including LVRR, particularly among pediatric patients, remains uncertain.MethodsWe prospectively enrolled pediatric patients with DCM from Japanese multi-institutional centers between 2014 and 2023. We identified DCM-related genes and explored the association between gene variants and clinical outcomes, including LVRR, which was defined as any increase in left ventricular ejection fraction during the observation period.ResultsA total of 123 pediatric patients (62 males; mean age of 8 months [range, 1–51 months]) were retrospectively enrolled. There were 50 pathogenic variants in 45 patients (35.0%). The most identified gene wasMYH7(14.0%), followed byRYR2(12.0%), andTPM1(8.0%). A novel variant in theCASZ1gene (NM_001079843.2 c.3356G>A, p. Trp1119Ter) was identified. LVRR was achieved in 47.5% of patients. In patients with sarcomere gene variants, the left ventricular ejection fraction remained unchanged (31.4% to 39.8%,P= 0.1913), whereas it significantly increased in patients with non-sarcomere gene variants (33.4% to 47.8%,P= 0.0466) and in patients without gene variants (33.6% to 54.1%,P= 0.003).ConclusionsPediatric patients with DCM exhibited a marked genetic heterogeneity with a different landscape from adults with DCM. LVRR was not uniform across functional gene groups, opening the door to tailor-made gene-guided prediction in pediatric patients with DCM.Clinical perspectiveWhat is new?Younger patients had predominance for DCM and risk factors for survival.LVRR occurrence was lower in the sarcomere gene group, and cardiac function failed to improve.What are the clinical implications?LVRR was not uniform across functional gene groups, which opens the door to the adoption of an individualized prediction approach in DCM according to the genetic features.
Publisher
Cold Spring Harbor Laboratory
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