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通过表面增强激光解吸/电离飞行时间质谱法定量戈谢病血样中生物标志物CCL18的局限性。

Limitations in quantitation of the biomarker CCL18 in Gaucher disease blood samples by surface-enhanced laser desorption/ionization time-of-flight mass spectrometry.

作者信息

van Breemen Mariëlle J, Bleijlevens Boris, de Koster Chris G, Aerts Johannes M F G

机构信息

Clinical Proteomics Facility, Department of Medical Biochemistry, Academic Medical Center, University of Amsterdam, Meibergdreef 15, 1105AZ Amsterdam, The Netherlands.

出版信息

Biochim Biophys Acta. 2006 Oct;1764(10):1626-32. doi: 10.1016/j.bbapap.2006.08.004. Epub 2006 Aug 22.

DOI:10.1016/j.bbapap.2006.08.004
PMID:17010683
Abstract

SELDI-TOF MS assisted the discovery of the chemokine CCL18/PARC as plasma biomarker for pathological storage cells in Gaucher disease patients. Prognostic elevation of CCL18 in blood of Gaucher patients has been confirmed by ELISA. Given its low molecular mass, positive charge, and relatively high abundance, CCL18 seems a particular attractive protein for SELDI-TOF based quantitation. Therefore, we determined CCL18 levels in plasma using SELDI-TOF MS and ELISA, in parallel. CCL18 levels in some blood samples were significantly underestimated when determined by SELDI-TOF MS. Spiking of recombinant CCL18 indicated that its detection by SELDI-TOF MS is strongly determined by the nature of the sample, even markedly varying between samples obtained from one donor at different time points. Independent of the total CCL18 concentration in blood only 1-10% of the chemokine bound to the ProteinChip Array. Even when comparable amounts of CCL18 from distinct samples were bound to the ProteinChip Array, diverse peak intensities could be observed. Thus, limited binding capacity and sample-dependent suppression of CCL18 ionization contribute significantly to the final peak intensity. In conclusion, SELDI-TOF MS offers no reliable procedure to quantitatively monitor CCL18 levels in blood and thus cannot be applied in evaluation of disease status of Gaucher patients.

摘要

表面增强激光解吸/电离飞行时间质谱(SELDI-TOF MS)助力发现趋化因子CCL18/PARC作为戈谢病患者病理性储存细胞的血浆生物标志物。酶联免疫吸附测定(ELISA)已证实戈谢病患者血液中CCL18的预后性升高。鉴于其低分子量、正电荷以及相对较高的丰度,CCL18似乎是基于SELDI-TOF进行定量分析的特别有吸引力的蛋白质。因此,我们同时使用SELDI-TOF MS和ELISA测定血浆中的CCL18水平。用SELDI-TOF MS测定时,一些血样中的CCL18水平被显著低估。重组CCL18的加样表明,SELDI-TOF MS对其检测强烈取决于样品的性质,甚至在从同一供体在不同时间点采集的样品之间也有显著差异。与血液中CCL18的总浓度无关,只有1%至10%的趋化因子与蛋白质芯片阵列结合。即使来自不同样品的相当数量的CCL18与蛋白质芯片阵列结合,也能观察到不同的峰强度。因此,有限的结合能力和样品依赖性的CCL18电离抑制对最终的峰强度有显著贡献。总之,SELDI-TOF MS无法提供可靠的程序来定量监测血液中的CCL18水平,因此不能用于评估戈谢病患者的疾病状态。

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