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IgA 肾病相关自身抗体分析:整合抗微生物组学方法。

Profiling of autoantibodies in IgA nephropathy, an integrative antibiomics approach.

机构信息

Departments of Pediatrics-Nephrology, Stanford University School of Medicine, Stanford, CA 94304, USA.

出版信息

Clin J Am Soc Nephrol. 2011 Dec;6(12):2775-84. doi: 10.2215/CJN.04600511.

Abstract

BACKGROUND AND OBJECTIVES

IgG commonly co-exists with IgA in the glomerular mesangium of patients with IgA nephropathy (IgAN) with unclear clinical relevance. Autoantibody (autoAb) biomarkers to detect and track progression of IgAN are an unmet clinical need. The objective of the study was to identify IgA-specific autoAbs specific to IgAN.

DESIGN, SETTING, PARTICIPANTS, & MEASUREMENTS: High-density protein microarrays were evaluated IgG autoAbs in the serum of IgAN patients (n = 22) and controls (n = 10). Clinical parameters, including annual GFR and urine protein measurements, were collected on all patients over 5 years. Bioinformatic data analysis was performed to select targets for further validation by immunohistochemistry (IHC).

RESULTS

One hundred seventeen (1.4%) specific antibodies were increased in IgAN. Among the most significant were the autoAb to the Ig family of proteins. IgAN-specific autoAbs (approximately 50%) were mounted against proteins predominantly expressed in glomeruli and tubules, and selected candidates were verified by IHC. Receiver operating characteristic analysis of our study demonstrated that IgG autoAb levels (matriline 2, ubiquitin-conjugating enzyme E2W, DEAD box protein, and protein kinase D1) might be used in combination with 24-hour proteinuria to improve prediction of the progression of IgAN (area under the curve = 0.86, P = 0.02).

CONCLUSIONS

IgAN is associated with elevated IgG autoAbs to multiple proteins in the kidney. This first analysis of the repertoire of autoAbs in IgAN identifies novel, immunogenic protein targets that are highly expressed in the kidney glomerulus and tubules that may bear relevance in the pathogenesis and progression of IgAN.

摘要

背景和目的

IgA 肾病(IgAN)患者肾小球系膜中 IgG 常与 IgA 共存,但临床相关性尚不清楚。用于检测和跟踪 IgAN 进展的自身抗体(autoAb)生物标志物是临床尚未满足的需求。本研究的目的是鉴定针对 IgAN 的 IgA 特异性自身抗体。

设计、设置、参与者和测量:使用高密度蛋白质微阵列评估了 22 例 IgAN 患者(n = 22)和 10 例对照者(n = 10)血清中的 IgG 自身抗体。对所有患者进行了 5 年以上的临床参数(包括每年的肾小球滤过率和尿蛋白测量)收集。通过免疫组织化学(IHC)进一步验证,进行了生物信息数据分析以选择目标。

结果

IgAN 患者的 IgG 自身抗体增加了 117 种(1.4%)。其中最显著的是 Ig 家族蛋白的自身抗体。针对主要在肾小球和肾小管中表达的蛋白产生的 IgAN 特异性自身抗体(约 50%),通过 IHC 进行了验证。本研究的接收者操作特征分析表明,IgG 自身抗体水平(谱系 2、泛素结合酶 E2W、DEAD 框蛋白和蛋白激酶 D1)可能与 24 小时蛋白尿联合使用,以提高 IgAN 进展的预测(曲线下面积 = 0.86,P = 0.02)。

结论

IgAN 与肾脏中多种蛋白质的 IgG 自身抗体升高有关。对 IgAN 自身抗体谱的首次分析确定了新型免疫原性肾肾小球和肾小管高表达的蛋白靶标,这些靶标可能与 IgAN 的发病机制和进展有关。

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