心肌梗死和终末期肾病患者心肌肌钙蛋白 T 组成的差异:血管效应?

IF 1.8 Q3 MEDICAL LABORATORY TECHNOLOGY
Wim H M Vroemen, Ellen J S Denessen, William P T M van Doorn, Kelly E J M Pelzer, Tilman M Hackeng, Elisabeth J R Litjens, Yvonne M C Henskens, Frank M van der Sande, Will K W H Wodzig, Jeroen P Kooman, Otto Bekers, Douwe de Boer, Alma M A Mingels
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引用次数: 0

摘要

背景:心肌肌钙蛋白 T(cTnT)是诊断心肌梗死(MI)的关键,但在终末期肾病(ESRD)患者中也会升高。在心肌梗死急性期发现了特定的较大的 cTnT 蛋白形式,而在 ESRD 患者的血清中只发现了较小的 cTnT 片段。然而,其他人认为这是由于血清中大量凝血酶的产生导致的分析前效应。因此,我们研究了各种抗凝方法对 cTnT 组成和浓度的影响,并比较了 MI 和 ESRD 患者的 cTnT 组成:方法:使用高灵敏度(hs-)cTnT 免疫测定法研究了同时采集的血清、锂肝素(LH)血浆和乙二胺四乙酸(EDTA)血浆中 cTnT 浓度的一致性:结果:在所有血液基质中都观察到了良好的 hs-cTnT 浓度一致性(斜率大于 0.98;95% CI,0.96-1.04)。在 LH 血浆、EDTA 血浆和血清中发现了随时间变化的降解(40 kDa 完整片段:29 kDa 片段:15 至 18 kDa 片段),降解比例(%)分别为 90:10:0、0:5:95 和 0:0:100(采血 48 小时后)。此外,凝胶过滤层析(GFC)图谱显示,心肌梗死患者的 cTnT 蛋白形式主要较大,而 ESRD 患者在所有基质中主要发现 15 至 18 kDa 的片段:体外 cTnT 降解的程度取决于(抗)凝方法,但不会影响 hs-cTnT 的浓度。此外,在心肌梗死患者中主要存在较大的 cTnT 蛋白形式,而在 ESRD 患者中主要发现 15 至 18 kDa 的小 cTnT 片段。这些见解对于开发针对较大 cTnT 蛋白形式的新型 hs-cTnT 检测方法至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Differences in Cardiac Troponin T Composition in Myocardial Infarction and End-Stage Renal Disease Patients: A Blood Tube Effect?

Background: Cardiac troponin T (cTnT) is key in diagnosing myocardial infarction (MI) but is also elevated in end-stage renal disease (ESRD) patients. Specific larger cTnT proteoforms were identified for the acute phase of MI, while in serum of ESRD patients solely small cTnT fragments were found. However, others allocated this to a pre-analytic effect due to abundant thrombin generation in serum. Therefore, we investigated the effect of various anticoagulation methods on cTnT composition and concentration and compared the cTnT composition of MI and ESRD patients.

Methods: The agreement of cTnT concentrations between simultaneously collected serum, lithium-heparin (LH) plasma, and ethylenediaminetetraacetic acid (EDTA) plasma was studied using the high-sensitivity (hs-)cTnT immunoassay. cTnT proteoform composition was investigated in a standardized time-dependent manner through spike experiments and in simultaneously collected blood matrixes of MI and ESRD patients.

Results: Excellent hs-cTnT concentration agreements were observed across all blood matrixes (slopes > 0.98; 95% CI, 0.96-1.04). Time-dependent degradation (40 kDa intact:29 kDa fragment:15 to 18 kDa fragments) was found in LH plasma and EDTA plasma, and serum in ratios (%) of 90:10:0, 0:5:95, and 0:0:100, respectively (48 h after blood collection). Moreover, gel filtration chromatography (GFC) profiles illustrated mainly larger cTnT proteoforms in MI patients, while in ESRD patients mainly 15 to 18 kDa fragments were found for all matrices.

Conclusions: The extent of cTnT degradation in vitro is dependent on the (anti)coagulation method, without impacting hs-cTnT concentrations. Furthermore, mainly larger cTnT proteoforms were present in MI patients, while in ESRD patients mainly small 15 to 18 kDa cTnT fragments were found. These insights are essential when developing a novel hs-cTnT assay targeting larger cTnT proteoforms.

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来源期刊
Journal of Applied Laboratory Medicine
Journal of Applied Laboratory Medicine MEDICAL LABORATORY TECHNOLOGY-
CiteScore
3.70
自引率
5.00%
发文量
137
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