利用广义加法模型调整多中心试验中肌酸激酶 MB 活性和质量数据的可行性。

0 CARDIAC & CARDIOVASCULAR SYSTEMS
Markus Hoenicka, Arbresha Vokshi, Shaoxia Zhou, Andreas Liebold, Benjamin Mayer
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引用次数: 0

摘要

目的:血清肌酸激酶同工酶MB(CK-MB)水平升高预示着治疗心脏病期间心肌缺血和围手术期心肌损伤。我们在一项前瞻性试验研究的基础上,建立了一种从活动数据预测 CK-MB 质量的方法,以简化多中心试验。方法:我们招募了 38 名没有急性心肌缺血和终末肾衰竭的择期心脏手术患者。对术前、术后、术后 6 小时和术后 12 小时抽取的静脉血样本进行 CK-MB 质量和活性测定。采用线性回归和广义相加模型(GAMs)来描述质量和活性之间的关系。评估了人口统计学和围手术期因素对 GAMs 拟合的影响。通过Bland-Altman分析评估了预测和测量的CK-MB质量的一致性:结果:线性回归提供了可接受的总体拟合度(r2=0.834),但在 CK-MB 水平较低时出现了偏差。加入年龄、体重指数和手术时间后,GAMs 并未受益。通过活动、性别和取样时间预测 CK-MB 质量的最小适当模型的 r2 为 0.981。Bland-Altman分析证实了一致性范围较窄(差值:8.87 µg/L),且不存在固定偏差(p = 0.41)和比例偏差(p = 0.21):结论:对具有代表性的患者队列中的 CK-MB 数据进行基于 GAM 的建模,可根据活动、性别和采样时间预测 CK-MB 质量。这种方法简化了将CK-MB数据不一致的研究中心纳入多中心试验的过程,以便于将CK-MB水平纳入统计模型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Feasibility of aligning creatine kinase MB activity and mass data in multicentre trials using generalized additive modelling.

Objectives: Elevated serum creatine kinase isoenzyme MB (CK-MB) levels indicate myocardial ischaemia and periprocedural myocardial injury during treatment of heart diseases. We established a method to predict CK-MB mass from activity data based on a prospective pilot study in order to simplify multicentre trials.

Methods: 38 elective cardiac surgery patients without acute myocardial ischaemia and terminal renal failure were recruited. CK-MB mass and activity were determined in venous blood samples drawn preoperatively, postoperatively, 6 h post-op, and 12 h post-op. Linear regression and generalized additive models (GAMs) were applied to describe the relationship of mass and activity. Influences of demographic and perioperative factors on the fit of GAMs was evaluated. The agreement of predicted and measured CK-MB masses was assessed by Bland-Altman analyses.

Results: Linear regression provided an acceptable overall fit (r2 = 0.834) but showed deviances at low CK-MB levels. GAMs did not benefit from the inclusion of age, body mass index and surgical times. The minimal adequate model predicted CK-MB masses from activities, sex and sampling time with an r2 of 0.981. Bland-Altman analyses confirmed narrow limits of agreement (spread: 8.87 µg/l) and the absence of fixed (P = 0.41) and proportional (P = 0.21) biases.

Conclusions: GAM-based modelling of CK-MB data in a representative patient cohort allowed to predict CK-MB masses from activities, sex and sampling time. This approach simplifies the integration of study centres with incompatible CK-MB data into multicentre trials in order to facilitate inclusion of CK-MB levels in statistical models.

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