Sadasivan Chandu, Gagnon Luke R, Hazra Deepan, Wang Kaiming, Youngson Erik, Thomas Jissy, Chan Anita Y M, Paterson D Ian, McAlister Finlay A, Dzwiniel Tara, Tymchak Wayne, Christian Susan, Oudit Gavin Y
Division of Cardiology, Department of Medicine, Mazankowski Alberta Heart Institute, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, AB, Canada.
The Alberta Strategy for Patient Oriented Research Support Unit (AbSPORU), Edmonton, AB, Canada.
ESC Heart Fail. 2025 Jun;12(3):1942-1955. doi: 10.1002/ehf2.15202. Epub 2024 Dec 30.
Patients with cardiomyopathies are a heterogeneous group of patients who experience high morbidity and mortality. Early cardiac assessment and intervention with access to genetic counselling in a multidisciplinary Cardiomyopathy Clinic may improve outcomes and prevent progression to advanced heart failure.
Our prospective cohort study was conducted at a multidisciplinary Cardiomyopathy Clinic with 421 patients enrolled (42.5% female, median age 58 years), including 224 patients with dilated cardiomyopathy (DCM, 42.9% female, median age 57 years), 72 with hypertrophic cardiomyopathy (HCM, 43.1% female, median age 60 years), 79 with infiltrative cardiomyopathy (65.8% female, median age 70 years) and 46 who were stage A/at risk for genetic cardiomyopathy (54.3% female, median age 36 years). Patients were seen in follow-up at a median of 18 months. A pathogenic/likely pathogenic variant was identified in 28.5% of the total cohort, including 33.3% of the DCM cohort (28% TTN mutations) and 34.1% of the HCM cohort (60% MYBPC3 and 20% MYH7) who underwent genetic testing. The use of angiotensin-converting enzyme inhibitors/angiotensin receptor blockers/angiotensin receptor neprilysin inhibitor (48.3-69.5% of total cohort, P < 0.001), β-blockers (58.4-72.4%, P < 0.001), mineralocorticoid receptor antagonists (33.9-41.4%, P = 0.0014) and sodium/glucose cotransporter-2 inhibitors (5.3-27.9%, P < 0.001) all increased at follow-up. Precision-based therapies were also implemented, including tafamidis for transthyretin amyloidosis (n = 21), enzyme replacement therapy for Fabry disease (n = 14) and mavacamten (n = 4) for HCM. Optimization of medications and devices resulted in improvements in left ventricular ejection fraction (LVEF) from 27% to 43% at follow-up for DCM patients with reduced LVEF at baseline (P < 0.001) and reduction in left ventricular mass index (LVMI) from 156 g/m to 128 g/m at follow-up for HCM patients with abnormal LVMI at baseline (P = 0.009). Optimization of therapies was associated with stable plasma biomarkers in stage B patients while lowering levels of BNP (619-517.5 pg/mL, P = 0.048), NT-proBNP (777.5-356 ng/L, P < 0.001) and hsTropT (31-22 ng/L, P = 0.005) at follow-up relative to baseline values for stage C patients. Despite stage B patients having overt cardiomyopathy at baseline, stage A and B patients had a similarly high probability of survival (χ2 = 0.204, P = 0.652). The overall cardiovascular mortality rate was low at 1.7% for the cohort (0.5% for stage B and 3.3% for stage C) over a median of 34-month follow-up.
Our study demonstrates that a multidisciplinary cardiomyopathy clinic can improve the clinical profiles of patients with diverse genetic cardiomyopathies.
心肌病患者是一组异质性患者,其发病率和死亡率都很高。在多学科心肌病诊所进行早期心脏评估并提供基因咨询,可能会改善治疗效果并预防进展为晚期心力衰竭。
我们在一家多学科心肌病诊所进行了前瞻性队列研究,纳入421例患者(42.5%为女性,中位年龄58岁),其中包括224例扩张型心肌病(DCM)患者(42.9%为女性,中位年龄57岁)、72例肥厚型心肌病(HCM)患者(43.1%为女性,中位年龄60岁)、79例浸润性心肌病患者(65.8%为女性,中位年龄70岁)以及46例处于A期/有遗传性心肌病风险的患者(54.3%为女性,中位年龄36岁)。患者随访的中位时间为18个月。在整个队列中,28.5%的患者鉴定出致病/可能致病的变异,其中接受基因检测的DCM队列中有33.3%(28%为TTN突变),HCM队列中有34.1%(60%为MYBPC3突变,20%为MYH7突变)。血管紧张素转换酶抑制剂/血管紧张素受体阻滞剂/血管紧张素受体脑啡肽酶抑制剂(占整个队列的48.3 - 69.5%,P < 0.001)、β受体阻滞剂(58.4 - 72.4%,P < 0.001)、盐皮质激素受体拮抗剂(33.9 - 41.4%,P = 0.0014)和钠/葡萄糖协同转运蛋白2抑制剂(5.3 - 27.9%,P < 0.001)在随访时的使用均增加。还实施了精准治疗,包括用于转甲状腺素蛋白淀粉样变性的tafamidis(n = 21)、用于法布里病的酶替代疗法(n = 14)以及用于HCM的mavacamten(n = 4)。药物和器械的优化使基线时左心室射血分数(LVEF)降低的DCM患者在随访时LVEF从27%提高到43%(P < 0.001),使基线时左心室质量指数(LVMI)异常的HCM患者在随访时LVMI从156 g/m²降至128 g/m²(P = 0.009)。治疗的优化与B期患者血浆生物标志物稳定相关,而相对于C期患者的基线值,随访时B型利钠肽(BNP)(619 - 517.5 pg/mL,P = 0.048)、N末端B型利钠肽原(NT - proBNP)(777.5 - 356 ng/L,P < 0.001)和高敏肌钙蛋白T(hsTropT)(31 - 22 ng/L,P = 0.005)水平降低。尽管B期患者在基线时已有明显心肌病,但A期和B期患者的生存概率相似(χ² = 0.204,P = 0.652)。在中位34个月的随访中,整个队列的总体心血管死亡率较低,为1.7%(B期为0.5%,C期为3.3%)。
我们的研究表明,多学科心肌病诊所可以改善不同遗传性心肌病患者的临床状况。
