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基于血液中基因表达的早期帕金森病分子标志物

Molecular markers of early Parkinson's disease based on gene expression in blood.

作者信息

Scherzer Clemens R, Eklund Aron C, Morse Lee J, Liao Zhixiang, Locascio Joseph J, Fefer Daniel, Schwarzschild Michael A, Schlossmacher Michael G, Hauser Michael A, Vance Jeffery M, Sudarsky Lewis R, Standaert David G, Growdon John H, Jensen Roderick V, Gullans Steven R

机构信息

Center for Neurologic Diseases, Brigham and Women's Hospital and Harvard Medical School, 65 Landsdowne Street, Cambridge, MA 02139, USA.

出版信息

Proc Natl Acad Sci U S A. 2007 Jan 16;104(3):955-60. doi: 10.1073/pnas.0610204104. Epub 2007 Jan 10.

Abstract

Parkinson's disease (PD) progresses relentlessly and affects five million people worldwide. Laboratory tests for PD are critically needed for developing treatments designed to slow or prevent progression of the disease. We performed a transcriptome-wide scan in 105 individuals to interrogate the molecular processes perturbed in cellular blood of patients with early-stage PD. The molecular multigene marker here identified is associated with risk of PD in 66 samples of the training set comprising healthy and disease controls [third tertile cross-validated odds ratio of 5.7 (P for trend 0.005)]. It is further validated in 39 independent test samples [third tertile odds ratio of 5.1 (P for trend 0.04)]. Insights into disease-linked processes detectable in peripheral blood are offered by 22 unique genes differentially expressed in patients with PD versus healthy individuals. These include the co-chaperone ST13, which stabilizes heat-shock protein 70, a modifier of alpha-synuclein misfolding and toxicity. ST13 messenger RNA copies are lower in patients with PD (mean +/- SE 0.59 +/- 0.05) than in controls (0.96 +/- 0.09) (P = 0.002) in two independent populations. Thus, gene expression signals measured in blood can facilitate the development of biomarkers for PD.

摘要

帕金森病(PD)会持续进展,全球有500万人受其影响。开发旨在减缓或预防该病进展的治疗方法急需PD的实验室检测。我们对105名个体进行了全转录组扫描,以探究早期PD患者外周血中受到干扰的分子过程。此处鉴定出的分子多基因标志物与包括健康对照和疾病对照的训练集中66个样本的PD风险相关[三分位数交叉验证的优势比为5.7(趋势P值为0.005)]。它在39个独立测试样本中得到进一步验证[三分位数优势比为5.1(趋势P值为0.04)]。PD患者与健康个体中22个差异表达的独特基因揭示了在外周血中可检测到的与疾病相关的过程。其中包括共伴侣蛋白ST13,它可稳定热休克蛋白70,而热休克蛋白70是α-突触核蛋白错误折叠和毒性的调节剂。在两个独立人群中,PD患者的ST13信使RNA拷贝数(均值±标准误0.59±0.05)低于对照组(0.96±0.09)(P = 0.002)。因此,血液中测得的基因表达信号有助于开发PD的生物标志物。

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