外周血基因表达作为复杂结节病的新型基因组生物标志物。

Peripheral blood gene expression as a novel genomic biomarker in complicated sarcoidosis.

机构信息

Institute for Personalized Respiratory Medicine, The University of Illinois at Chicago, Chicago, Illinois, United States of America.

出版信息

PLoS One. 2012;7(9):e44818. doi: 10.1371/journal.pone.0044818. Epub 2012 Sep 12.

DOI:10.1371/journal.pone.0044818

PMID:22984568

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3440319/

Abstract

Sarcoidosis, a systemic granulomatous syndrome invariably affecting the lung, typically spontaneously remits but in ~20% of cases progresses with severe lung dysfunction or cardiac and neurologic involvement (complicated sarcoidosis). Unfortunately, current biomarkers fail to distinguish patients with remitting (uncomplicated) sarcoidosis from other fibrotic lung disorders, and fail to identify individuals at risk for complicated sarcoidosis. We utilized genome-wide peripheral blood gene expression analysis to identify a 20-gene sarcoidosis biomarker signature distinguishing sarcoidosis (n = 39) from healthy controls (n = 35, 86% classification accuracy) and which served as a molecular signature for complicated sarcoidosis (n = 17). As aberrancies in T cell receptor (TCR) signaling, JAK-STAT (JS) signaling, and cytokine-cytokine receptor (CCR) signaling are implicated in sarcoidosis pathogenesis, a 31-gene signature comprised of T cell signaling pathway genes associated with sarcoidosis (TCR/JS/CCR) was compared to the unbiased 20-gene biomarker signature but proved inferior in prediction accuracy in distinguishing complicated from uncomplicated sarcoidosis. Additional validation strategies included significant association of single nucleotide polymorphisms (SNPs) in signature genes with sarcoidosis susceptibility and severity (unbiased signature genes - CX3CR1, FKBP1A, NOG, RBM12B, SENS3, TSHZ2; T cell/JAK-STAT pathway genes such as AKT3, CBLB, DLG1, IFNG, IL2RA, IL7R, ITK, JUN, MALT1, NFATC2, PLCG1, SPRED1). In summary, this validated peripheral blood molecular gene signature appears to be a valuable biomarker in identifying cases with sarcoidoisis and predicting risk for complicated sarcoidosis.

摘要

结节病是一种系统性肉芽肿综合征，通常会影响肺部，通常会自行缓解，但在约 20%的病例中，会出现严重的肺功能障碍或心脏和神经系统受累（复杂结节病）。不幸的是，目前的生物标志物无法区分缓解（单纯）结节病患者与其他纤维化肺疾病患者，也无法识别复杂结节病的风险个体。我们利用全基因组外周血基因表达分析来识别 20 个基因的结节病生物标志物特征，该特征可区分结节病（n=39）与健康对照者（n=35，86%的分类准确性），并作为复杂结节病的分子特征（n=17）。由于 T 细胞受体（TCR）信号、JAK-STAT（JS）信号和细胞因子-细胞因子受体（CCR）信号的异常与结节病发病机制有关，因此与结节病相关的 T 细胞信号通路基因组成的 31 个基因特征（TCR/JS/CCR）与无偏倚的 20 个基因生物标志物特征进行了比较，但在区分复杂和单纯结节病方面的预测准确性较差。其他验证策略包括鉴定与结节病易感性和严重程度相关的特征基因中的单核苷酸多态性（SNP），这些基因包括无偏倚特征基因（CX3CR1、FKBP1A、NOG、RBM12B、SENS3、TSHZ2；T 细胞/JAK-STAT 通路基因，如 AKT3、CBLB、DLG1、IFNG、IL2RA、IL7R、ITK、JUN、MALT1、NFATC2、PLCG1、SPRED1）。总之，这个经过验证的外周血分子基因特征似乎是识别结节病病例和预测复杂结节病风险的有价值的生物标志物。

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外周血基因表达作为复杂结节病的新型基因组生物标志物。

Peripheral blood gene expression as a novel genomic biomarker in complicated sarcoidosis.

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