From the Department of Medicine, and the Casey Eye Institute, and the OHSU-PSU (Portland State University) School of Public Health, Oregon Health & Science University (OHSU), Portland, Oregon, USA; Graduate School of Dentistry, Kyung Hee University, Seoul, Korea; Devers Eye Institute, Legacy Health Systems, Portland, Oregon, USA.
M.A. Friedman, MD, Instructor of Medicine, Department of Medicine, OHSU; D. Choi, PhD, Professor, Department of Medicine, and the Casey Eye Institute, and the OHSU-PSU School of Public Health, and the Graduate School of Dentistry, Kyung Hee University; S.R. Planck, PhD, Professor of Ophthalmology, Department of Medicine, and Casey Eye Institute, OHSU; J.T. Rosenbaum, MD, Professor of Ophthalmology, Department of Medicine, and Casey Eye Institute, OHSU, and Devers Eye Institute, Legacy Health Systems; C.H. Sibley, MD, Assistant Professor of Medicine, Department of Medicine, OHSU.
J Rheumatol. 2019 Jun;46(6):609-615. doi: 10.3899/jrheum.180455. Epub 2019 Jan 15.
To identify commonalities in gene expression data across all antineutrophil cytoplasmic antibody (ANCA)-associated vasculitis (AAV) tissues thus far characterized.
Gene expression data were collected from the 3 AAV tissues thus far characterized (orbit, peripheral leukocytes, and sinus brushings). These data were analyzed to identify commonly expressed genes and disease pathways. The pathways data were adjusted for multiple comparisons using a combined local false discovery rate, which estimates the probability of a false discovery of a given pathway in all 3 tissues analyzed.
Only 4 genes were upregulated in all 3 tissues - , , and . After multiple comparison adjustments, the network pathway analysis revealed 28 pathways associated with all 3 tissues. The most strongly associated pathway for all 3 tissues was the neutrophil degranulation pathway [multidimensional local false discovery (md-locfdr) = 1.05 × 10], followed by the osteoclast differentiation (md-locfdr = 3.8 × 10), cell surface interactions at the vascular wall (md-locfdr = 4.2 × 10), signaling by interleukins (md-locfdr = 6.1 × 10), and phagosome (md-locfdr = 0.003) pathways. There were no downregulated genes or pathways common to all 3 tissues.
This analysis identified individual genes and pathways of disease common to all AAV tissues thus far characterized. The use of a network pathway analysis allowed us to identify pathologic mechanisms that were not readily apparent in the commonly expressed genes alone. Many of these pathways are consistent with current theories about infectious drivers and the crossroads of innate and adaptive immune mechanisms. In addition, this analysis highlights novel pathways, such as vessel wall interactions and platelet activation, which require further investigation.
确定迄今为止所有抗中性粒细胞胞浆抗体(ANCA)相关性血管炎(AAV)组织中基因表达数据的共性。
收集迄今为止已鉴定的 3 种 AAV 组织(眼眶、外周白细胞和窦刷)的基因表达数据。对这些数据进行分析以确定共同表达的基因和疾病途径。使用联合局部假发现率(local false discovery rate,lfdr)对途径数据进行多重比较调整,该概率估计了在分析的所有 3 种组织中给定途径的假发现概率。
仅有 4 个基因在所有 3 种组织中上调——、、和。在多重比较调整后,网络途径分析显示与所有 3 种组织相关的 28 种途径。与所有 3 种组织最相关的途径是中性粒细胞脱颗粒途径[多维局部假发现率(multidimensional local false discovery rate,md-locfdr)= 1.05×10],其次是破骨细胞分化途径(md-locfdr= 3.8×10)、血管壁细胞表面相互作用途径(md-locfdr= 4.2×10)、白细胞介素信号转导途径(md-locfdr= 6.1×10)和吞噬体途径(md-locfdr= 0.003)。没有下调的基因或途径在所有 3 种组织中共同存在。
该分析确定了迄今为止所有 AAV 组织中共同存在的个体疾病基因和途径。网络途径分析的使用使我们能够识别单独的基因表达途径中不易察觉的病理机制。其中许多途径与当前关于感染驱动因素以及固有和适应性免疫机制交叉的理论一致。此外,该分析突出了新的途径,如血管壁相互作用和血小板激活,需要进一步研究。
