多发性骨髓瘤化疗期间心肌功能障碍和损伤生物标志物的变化:实验室数据解读的难点

IF 0.3 Q4 CARDIAC & CARDIOVASCULAR SYSTEMS Rational Pharmacotherapy in Cardiology Pub Date : 2023-11-07 DOI:10.20996/1819-6446-2023-2955
E. V. Fomina, S. A. Kardovskaya, D. A. Budanova, P. Markin, S. Appolonova, A. S. Lishuta, Y. Belenkov, I. Ilgisonis
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All patients underwent standard laboratory (complete blood count, biochemical tests, serum protein electrophoresis), electrocardiography, echocardiography, as well as the level of specific laboratory markers of myocardial dysfunction (NT-proBNP) and injury (hsTnI) was determined immediately before treatment, after 3 and 6 cycles of chemotherapy.Results. The mean age was 63,8±10 years with a slight predominance of men (56,7%, n=17). The patients initially had an increased level of NT-proBNP (316 [75,9; 602,6] pg/mL) with its decrease to 144,0 [102,3; 294,0] pg/ml after 3 cycles and to 109,2 [59,9; 344,5] pg/ml after 6 cycles of chemotherapy. At the MM onset, the mean hsTnI values were 0,06 [0,03; 0,49] ng/mL, whereas after 3 and 6 chemotherapy cycles it accounted for 0,02 [0,01-0,68] and 0,65 [0,02; 1,51] ng/ml, respectively, with the normal range of less than 0,1 ng/ml. Despite this, no statistical significance has been obtained. 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引用次数: 0

摘要

目的研究新诊断的多发性骨髓瘤(MM)患者在接受硼替佐米(VCd方案)方案治疗期间心脏生物标志物(N-端前脑钠肽(NT-proBNP)和高敏肌钙蛋白I(hsTnI))水平的变化。这项前瞻性试验研究纳入了新确诊的多发性骨髓瘤患者(30 人),这些患者计划接受包括蛋白酶体抑制剂(硼替佐米)在内的化疗周期。所有患者均接受了标准实验室检查(全血细胞计数、生化检验、血清蛋白电泳)、心电图检查、超声心动图检查,并在治疗前、化疗 3 个周期和 6 个周期后测定了心肌功能障碍(NT-proBNP)和心肌损伤(hsTnI)的特定实验室标志物水平。患者平均年龄为(63.8±10)岁,男性略占多数(56.7%,n=17)。患者最初的 NT-proBNP 水平升高(316 [75,9; 602,6] pg/ml),化疗 3 个周期后降至 144,0 [102,3; 294,0] pg/ml,化疗 6 个周期后降至 109,2 [59,9; 344,5] pg/ml。在 MM 发病时,hsTnI 的平均值为 0,06 [0,03; 0,49] 纳克/毫升,而在 3 个和 6 个化疗周期后,hsTnI 的平均值分别为 0,02 [0,01-0,68] 纳克/毫升和 0,65 [0,02; 1,51] 纳克/毫升,正常范围小于 0,1 纳克/毫升。尽管如此,统计结果并不显著。该队列中没有心衰、缺血或其他非心脏原因导致 NT-proBNP 水平升高的临床和/或实验室迹象。多变量回归分析显示以下因素对初始 hsTnI 水平有显著影响:副蛋白、血红蛋白和红细胞沉降率(ESR)。由此得出的回归模型具有很强的相关性(r=0,702,p<0,001)。MM及其致病特征(如副蛋白血症)可能对治疗前相关人群的NT-proBNP和hsTnI水平评估带来挑战。化疗前对这些指标的不可靠评估可能会导致不正确的心血管风险基线分层,并使心脏病专家/心血管肿瘤专家难以选择适当的管理策略。
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Changes of myocardial dysfunction and injury biomarkers over chemotherapy for multiple myeloma: difficulties in laboratory data interpretation
Aim. To study the changes of the levels of cardiac biomarkers (N-terminal pro-brain natriuretic peptide (NT-proBNP) and high-sensitivity troponin I (hsTnI)) in patients with newly diagnosed multiple myeloma (MM) during programmatic treatment with bortezomib (VCd regimen).Material and methods. This prospective pilot study included patients with a newly diagnosed MM (n=30), who were scheduled for a cycle of chemotherapy including a proteasome inhibitor (bortezomib). All patients underwent standard laboratory (complete blood count, biochemical tests, serum protein electrophoresis), electrocardiography, echocardiography, as well as the level of specific laboratory markers of myocardial dysfunction (NT-proBNP) and injury (hsTnI) was determined immediately before treatment, after 3 and 6 cycles of chemotherapy.Results. The mean age was 63,8±10 years with a slight predominance of men (56,7%, n=17). The patients initially had an increased level of NT-proBNP (316 [75,9; 602,6] pg/mL) with its decrease to 144,0 [102,3; 294,0] pg/ml after 3 cycles and to 109,2 [59,9; 344,5] pg/ml after 6 cycles of chemotherapy. At the MM onset, the mean hsTnI values were 0,06 [0,03; 0,49] ng/mL, whereas after 3 and 6 chemotherapy cycles it accounted for 0,02 [0,01-0,68] and 0,65 [0,02; 1,51] ng/ml, respectively, with the normal range of less than 0,1 ng/ml. Despite this, no statistical significance has been obtained. There were no clinical and/or laboratory signs of heart failure, ischemia, or other non-cardiac causes of elevated NT-proBNP levels in this cohort. Multivariate regression analysis revealed the following significant factors influencing the initial hsTnI level: paraprotein, hemoglobin and erythrocyte sedimentation rate (ESR). The resulting regression model was characterized by a strong correlation (r=0,702, p<0,001).Conclusion. MM and its pathogenetic features such as paraproteinemia may be challenging for NT-proBNP and hsTnI levels assessment in group of interest before treatment. An unreliable assessment of these markers before chemotherapy may lead to incorrect baseline cardiovascular risk stratification and make it difficult for a cardiologist/cardio-oncologist to choose proper management strategy.
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来源期刊
Rational Pharmacotherapy in Cardiology
Rational Pharmacotherapy in Cardiology CARDIAC & CARDIOVASCULAR SYSTEMS-
CiteScore
1.00
自引率
50.00%
发文量
79
审稿时长
6 weeks
期刊介绍: The primary goals of the Journal are consolidation of information on scientific and practical achievements in pharmacotherapy and prevention of cardiovascular diseases and continuing education of cardiologists and internists. The scientific concept of the edition suggests the publication of information on current achievements in cardiology, the results of national and international clinical trials. The Journal publishes original articles on the results of clinical trials designed to study the effectiveness and safety of drugs, analysis of clinical practice and its compliance with national and international recommendations, expert s’ opinions on a wide range of cardiology issues, associated conditions and clinical pharmacology. There is a heading “Preventive cardiology and public health” in the Journal to stimulate research interest in this highly demanded area. Memories of the outstanding people in medicine including cardiology, which are of great interest to historians of medicine, are published in "Our Mentors” heading.
期刊最新文献
Patients with atrial fibrillation in outpatient practice: clinical characteristics and outcomes over a 10-year observation period (data from the REQUAZA AF registrу — Yaroslavl) Prognostic Significance of Echocardiographic Characteristics in Patients with Type 2 Myocardial Infarction: comparison with Type 1 Myocardial Infarction Efficacy of azilsartan medoxomil in patients with hypertension and stable coronary artery disease in combination with type 2 diabetes Pharmacogenetics and pharmacokinetics of rivaroxaban in patients with atrial fibrillation and chronic kidney disease Changes of myocardial dysfunction and injury biomarkers over chemotherapy for multiple myeloma: difficulties in laboratory data interpretation
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