N末端B型利钠肽原(NTproBNP)和ST2作为提示心力衰竭症状老年患者全因死亡率和心血管死亡率的预测指标。
NTproBNP and ST2 as predictors for all-cause and cardiovascular mortality in elderly patients with symptoms suggestive for heart failure.
作者信息
Boman Kurt, Thormark Fröst Finn, Bergman Ann-Charlotte R, Olofsson Mona
机构信息
a Research Unit, Department of Medicine , Skellefteå Hospital , Skellefteå , Sweden.
b Department of Public Health and Clinical Medicine , Umeå University , Umeå , Sweden.
出版信息
Biomarkers. 2018 May-Jun;23(4):373-379. doi: 10.1080/1354750X.2018.1431692. Epub 2018 Feb 6.
BACKGROUND
A new biomarker, suppression of tumorigenicity 2 (ST2) has been introduced as a marker for fibrosis and hypertrophy. Its clinical value in comparison with N-terminal pro-hormone of brain natriuretic peptide /Amino-terminal pro-B-type natriuretic peptide (NTproBNP) in predicting mortality in elderly patients with symptoms of heart failure (HF) is still unclear.
AIM
To evaluate the prognostic value for all-cause- and cardiovascular mortality of ST2 or NTproBNP and the combination of these biomarkers.
PATIENTS AND METHODS
One hundred seventy patients patients with clinical symptoms of HF (77 (45%) were with verified HF) were recruited from one selected primary health care center (PHC) in Sweden and echocardiography was performed in all patients. Blood samples were obtained from 159 patients and stored frozen at -70 °C. NTproBNP was analyzed at a central core laboratory using a clinically available immunoassay.ST2 was analyzed with Critical Diagnostics Presage ST2 ELISA immunoassay.
RESULTS
We studied 159 patients (mean age 77 ± 8.3 years, 70% women). During ten years of follow up 78 patients had died, out of which 50 deaths were for cardiovascular reasons. Continuous NTproBNP and ST2 were both significantly associated with all-cause mortality (1.0001; 1.00001-1.0002, p = 0.04 and 1.03; 1.003-1.06, p = 0.03), NTproBNP but not ST2 remained significant for cardiovascular mortality after adjustments (1.0001; 1.00001-1.0002, p = 0.03 and 1.01; 0.77-1.06, p = 0.53), respectively. NTproBNP above median (>328 ng/L) compared to below median was significantly associated with all-cause mortality(HR: 4.0; CI :2.46-6.61; p < 0.001) and cardiovascular mortality (HR: 6.1; CI: 3.11-11.95; p < 0.001). Corresponding analysis for ST2 above median (25.6 ng/L) was not significantly associated neither with all-cause mortality (HR; 1.4; CI: 0.89-2.77) nor cardiovascular mortality (HR: 1.3; CI: 0.73-2.23) and no significant interaction of NTproBNP and ST2 (OR: 1.1; CI: 0.42-3.12) was found.
CONCLUSION
In elderly patients with symptoms of heart failure ST2 was not superior to NTproBNP to predict all cause or cardiovascular mortality. Furthermore, it is unclear if the combination of ST2 and NTproBNP will improve long-term prognostication beyond what is achieved by NTproBNP alone.
背景
一种新的生物标志物——致瘤性2抑制因子(ST2)已被作为纤维化和肥大的标志物引入。在预测老年心力衰竭(HF)症状患者的死亡率方面,其与脑钠肽N端前体/氨基末端B型利钠肽原(NTproBNP)相比的临床价值仍不明确。
目的
评估ST2或NTproBNP以及这些生物标志物组合对全因死亡率和心血管死亡率的预后价值。
患者与方法
从瑞典一个选定的初级卫生保健中心招募了170例有HF临床症状的患者(77例(45%)经证实患有HF),并对所有患者进行了超声心动图检查。从159例患者中采集血样并在-70°C下冷冻保存。NTproBNP在中央核心实验室使用临床可用的免疫测定法进行分析。ST2使用Critical Diagnostics Presage ST2 ELISA免疫测定法进行分析。
结果
我们研究了159例患者(平均年龄77±8.3岁,70%为女性)。在十年的随访期间,78例患者死亡,其中50例死于心血管原因。连续变量NTproBNP和ST2均与全因死亡率显著相关(1.0001;1.00001 - 1.0002,p = 0.04和1.03;1.003 - 1.06,p = 0.03),调整后NTproBNP对心血管死亡率仍有显著意义(1.0001;1.00001 - 1.0002,p = 0.03),而ST2无显著意义(1.01;0.77 - 1.06,p = 0.53)。与中位数以下相比,NTproBNP高于中位数(>328 ng/L)与全因死亡率(HR:4.0;CI:2.46 - 6.61;p < 0.001)和心血管死亡率(HR:6.1;CI:3.11 - 11.95;p < 0.001)显著相关。对ST2高于中位数(25.6 ng/L)的相应分析,与全因死亡率(HR;1.4;CI:0.89 - 2.77)和心血管死亡率(HR:1.3;CI:0.73 - 2.23)均无显著相关性,且未发现NTproBNP和ST2有显著交互作用(OR:1.1;CI:0.42 - 3.12)。
结论
在有心力衰竭症状的老年患者中,ST2在预测全因或心血管死亡率方面并不优于NTproBNP。此外,尚不清楚ST2和NTproBNP的组合是否能比单独使用NTproBNP更好地改善长期预后。
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