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脑脊液的蛋白质组学分析可区分中枢神经系统的恶性和非恶性疾病,并识别特定的蛋白质标志物。

Proteomic analysis of cerebrospinal fluid discriminates malignant and nonmalignant disease of the central nervous system and identifies specific protein markers.

作者信息

Khwaja Fatima W, Nolen John David Larkin, Mendrinos Savaas E, Lewis Melinda M, Olson Jeffrey J, Pohl Jan, Van Meir Erwin G, Ritchie James C, Brat Daniel J

机构信息

Department of Neurosurgery, Emory University School of Medicine, Atlanta, GA 30322, USA.

出版信息

Proteomics. 2006 Dec;6(23):6277-87. doi: 10.1002/pmic.200600135.

DOI:10.1002/pmic.200600135
PMID:17078017
Abstract

CNS diseases are often accompanied by changes in the protein composition of cerebrospinal fluid (CSF). SELDI-TOF-MS provides an approach for identifying specific protein markers of disease in biological fluids. We compared the CSF proteomes from patients with neoplastic and reactive/inflammatory CNS diseases to identify potential biomarkers. SELDI-TOF-MS was performed on CSF derived from lumbar puncture of 32 patients, including 10 with CNS malignancies, 12 with inflammatory or reactive conditions, and 10 with unknown CNS disease. Using the SAX-2 (strong anionic exchange) chip, we uncovered three conserved protein peak ranges within each disease category. For neoplastic diseases, we identified conserved peaks at 7.5-8.0 kDa (9/10 samples), 15.1-15.9 kDa (8/10 samples), and 30.0-32.0 kDa (5/10 samples). In reactive/inflammatory diseases, conserved peaks were found at 6.7-7.1 kDa (10/12 samples), 11.5-11.9 kDa (12/12 samples), and 13.3-13.7 kDa (9/12 samples). A protein from the 30.0 to 32.0 kDa peak range found in neoplastic CSF was identified by MALDI analysis as carbonic anhydrase, a protein overexpressed in many malignancies including high-grade gliomas. Similarly, cystatin C was identified in the 13.3-13.7 kDa peak range in non-neoplastic CSF and was most prominent in inflammatory conditions. Our approach provides a rational basis for identifying biomarkers that could be used for detection, diagnosis, and monitoring of CNS diseases.

摘要

中枢神经系统(CNS)疾病常伴有脑脊液(CSF)蛋白质组成的变化。表面增强激光解吸电离飞行时间质谱(SELDI-TOF-MS)为识别生物体液中疾病的特定蛋白质标志物提供了一种方法。我们比较了患有肿瘤性和反应性/炎症性中枢神经系统疾病患者的脑脊液蛋白质组,以确定潜在的生物标志物。对32例患者腰椎穿刺获取的脑脊液进行了SELDI-TOF-MS检测,其中包括10例中枢神经系统恶性肿瘤患者、12例炎症或反应性疾病患者以及10例中枢神经系统疾病不明患者。使用SAX-2(强阴离子交换)芯片,我们在每个疾病类别中发现了三个保守的蛋白质峰范围。对于肿瘤性疾病,我们在7.5 - 8.0 kDa(9/10个样本)、15.1 - 15.9 kDa(8/10个样本)和30.0 - 32.0 kDa(5/10个样本)处鉴定出保守峰。在反应性/炎症性疾病中,在6.7 - 7.1 kDa(10/12个样本)、11.5 - 11.9 kDa(12/12个样本)和13.3 - 13.7 kDa(9/12个样本)处发现了保守峰。通过基质辅助激光解吸电离(MALDI)分析,在肿瘤性脑脊液中发现的30.0至32.0 kDa峰范围内的一种蛋白质被鉴定为碳酸酐酶,该蛋白在包括高级别胶质瘤在内的许多恶性肿瘤中过表达。同样,胱抑素C在非肿瘤性脑脊液的13.3 - 13.7 kDa峰范围内被鉴定出来,并且在炎症状态下最为突出。我们的方法为识别可用于中枢神经系统疾病检测、诊断和监测的生物标志物提供了合理依据。

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