Department of Cardiology, Amsterdam UMC, University of Amsterdam, Meibergdreef 9, 1105, AZ, Amsterdam, the Netherlands; Netherlands Heart Institute, Moreelsepark 1, 3351, EP, Utrecht, the Netherlands.
Department of Cardiology, Amsterdam UMC, University of Amsterdam, Meibergdreef 9, 1105, AZ, Amsterdam, the Netherlands; Department of Cardiology, University Medical Center Utrecht, Heidelberglaan 100, 3584, CX, Utrecht, the Netherlands.
Int J Cardiol. 2020 May 1;306:56-60. doi: 10.1016/j.ijcard.2020.02.064. Epub 2020 Feb 27.
22q11.2 Deletion syndrome (22q11.2DS) is common in patients with tetralogy of Fallot (TOF) or pulmonary atresia with ventricular septal defect (PA/VSD) and is associated with worse outcomes in children. Whether this impaired prognosis is also translated into adulthood is unknown, as data in adult patients are limited. We aimed to compare long-term outcomes in adults with TOF or PA/VSD both with and without 22q11.2DS.
This study prospectively followed a nationwide multicenter cohort of TOF or PA/VSD patients with genetically confirmed presence or absence of 22q11.2DS, from inclusion in the Dutch national CONCOR registry for adults with congenital heart disease (CHD) onward. Outcome measures included all-cause mortality, cardiac mortality, need for pulmonary valve replacement (PVR), ventricular arrhythmias (VA), pacemaker implantation, and ICD implantation.
In total, 479 patients were included (277 (58%) male, median age 28 [IQR; 21-37] years, 62 (13%) with PA/VSD, 34 (7%) with 22q11.2DS). During a median follow-up of 11 [IQR; 6-13] years, 52 (11%) patients died (8 with 22q11.2DS and 44 without 22q11.2DS). Patients with 22q11.2DS had significant decreased survival after 12 years (76% [95% CI; 62-93]) compared to patients without 22q11.2DS (89% [95% CI; 86-92], p = 0.008). 22q11.2DS was associated with increased risk of all-cause mortality and cardiac-mortality, independent of age, sex, and PA/VSD. No association was found between 22q11.2DS and late complications i.e. PVR, VA, pacemaker, or ICD implantation.
Adults with TOF or PA/VSD with 22q11.2DS have a significantly worse survival than adults without this deletion. In patients with TOF or PA/VSD, genetic analysis for the presence of 22q11.2DS is important for risk stratification and genetic counseling.
22q11.2 缺失综合征(22q11.2DS)在四联症(TOF)或肺动脉闭锁伴室间隔缺损(PA/VSD)患者中较为常见,且与儿童患者的预后较差有关。但这种预后不良是否也会延续到成年期尚不清楚,因为目前有关成年患者的数据有限。我们旨在比较伴有和不伴有 22q11.2DS 的 TOF 或 PA/VSD 成年患者的长期预后。
本研究前瞻性地随访了荷兰全国先天性心脏病(CHD)成人 CONCOR 注册中心纳入的 TOF 或 PA/VSD 患者的全国多中心队列,这些患者的 22q11.2DS 存在或不存在经基因证实。主要终点包括全因死亡率、心源性死亡率、肺动脉瓣置换(PVR)、室性心律失常(VA)、起搏器植入和 ICD 植入的需要。
共纳入 479 例患者(277 例[58%]为男性,中位年龄 28[IQR; 21-37]岁,62 例[13%]为 PA/VSD,34 例[7%]为 22q11.2DS)。中位随访 11[IQR; 6-13]年后,52 例(11%)患者死亡(8 例伴有 22q11.2DS,44 例无 22q11.2DS)。伴有 22q11.2DS 的患者在 12 年后生存率显著降低(76%[95%CI; 62-93]),而无 22q11.2DS 的患者生存率为 89%[95%CI; 86-92%],两组间有统计学差异(p=0.008)。22q11.2DS 与全因死亡率和心源性死亡率增加相关,独立于年龄、性别和 PA/VSD。未发现 22q11.2DS 与晚期并发症(PVR、VA、起搏器或 ICD 植入)之间存在关联。
伴有 22q11.2DS 的 TOF 或 PA/VSD 成年患者的生存率显著低于不伴有该缺失的患者。对于 TOF 或 PA/VSD 患者,进行 22q11.2DS 基因分析对危险分层和遗传咨询很重要。
