Shahi Karan, Miller Robert J H, Dykstra Steven, Feng Yuanchao, Howlett Jonathan G, Jimenez-Zepeda Victor, Veenhuyzen Jan, White James A, Fine Nowell M
Division of Cardiology, Department of Cardiac Sciences, Libin Cardiovascular Institute, University of Calgary, Calgary, AB T2N 1N4, Canada.
Division of Hematology, Department of Internal Medicine, Cumming School of Medicine, University of Calgary, Calgary, AB T2N 1N4, Canada.
J Clin Med. 2024 Sep 16;13(18):5490. doi: 10.3390/jcm13185490.
Tafamidis is a costly therapy that improves outcomes for patients with transthyretin amyloidosis cardiomyopathy (ATTR-CM), although significant knowledge gaps exist for predicting longer-term response to treatment. The purpose of this study was to examine baseline predictors of adverse outcomes and their association with tafamidis treatment in comparison with those untreated in a clinical cohort from a Canadian ATTR-CM referral center. Patients with a confirmed diagnosis of ATTR-CM were included. Multivariable modeling was used to identify baseline variables associated with the primary outcome of all-cause mortality and secondary outcomes of cardiovascular mortality or hospitalization. Cox proportional hazard and competing risk analyses were used, with tafamidis modeled as a time-varying covariate. In total, 139 ATTR-CM patients were included, with a median age of 80.9 years [74.3-86.6 years], from 2011 to 2022. The mean follow-up was 2.9 ± 1.8 years. Eighty (55%) patients were treated with tafamidis. All-cause mortality and cardiovascular mortality alone were associated with the following baseline variables: age, clinical frailty scale, systolic blood pressure, renal function, and right ventricular size and function (all < 0.05), with no identified interactions with tafamidis treatment. Only baseline renal function was associated with cardiovascular hospitalization ( < 0.05). Important baseline variables associated with adverse ATTR-CM disease outcomes included renal function, systolic blood pressure, frailty, and right ventricular size and function. The risk factors were independent of treatment with tafamidis. These findings may help improve risk stratification for determining eligibility for ATTR-CM therapies.
塔法米迪斯是一种昂贵的疗法,可改善转甲状腺素蛋白淀粉样变心肌病(ATTR-CM)患者的预后,尽管在预测长期治疗反应方面存在重大知识空白。本研究的目的是在加拿大ATTR-CM转诊中心的一个临床队列中,检查不良结局的基线预测因素及其与塔法米迪斯治疗的关联,并与未接受治疗的患者进行比较。纳入确诊为ATTR-CM的患者。采用多变量建模来确定与全因死亡率这一主要结局以及心血管死亡率或住院这一次要结局相关的基线变量。使用Cox比例风险分析和竞争风险分析,将塔法米迪斯建模为一个随时间变化的协变量。2011年至2022年期间,共纳入139例ATTR-CM患者,中位年龄为80.9岁[74.3 - 86.6岁]。平均随访时间为2.9±1.8年。80例(55%)患者接受了塔法米迪斯治疗。全因死亡率和单独的心血管死亡率与以下基线变量相关:年龄、临床衰弱量表、收缩压、肾功能以及右心室大小和功能(均P<0.05),未发现与塔法米迪斯治疗有相互作用。只有基线肾功能与心血管住院相关(P<0.05)。与ATTR-CM疾病不良结局相关的重要基线变量包括肾功能、收缩压、衰弱以及右心室大小和功能。这些风险因素与塔法米迪斯治疗无关。这些发现可能有助于改善风险分层,以确定ATTR-CM治疗的 eligibility。 (注:原文中“eligibility”未准确翻译,可能需要结合上下文进一步确定其准确含义。)
