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首页> 外文期刊>Advances in Experimental Medicine and Biology >Proteomic and Genomic Biomarkers for Age-Related Macular Degeneration.
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Proteomic and Genomic Biomarkers for Age-Related Macular Degeneration.

机译:蛋白质组学和基因组生物标志物,用于年龄相关性黄斑变性。

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Toward early detection of susceptibility to age-related macular degeneration (AMD), we quantified plasma carboxyethylpyrrole (CEP) oxidative protein modifications and CEP autoantibodies by ELISA in 916 AMD and 488 control donors. Mean CEP adduct and autoantibody levels were elevated in AMD plasma by approximately 60 and approximately 30%, respectively, and the odds ratio for both CEP markers elevated was approximately 3-fold greater in AMD than in control patients. Genotyping was performed for AMD risk polymorphisms associated with age-related maculopathy susceptibility 2 (ARMS2), high-temperature requirement factor A1 (HTRA1), complement factor H (CFH), and complement C3. The AMD risk predicted for those exhibiting elevated CEP markers and risk genotypes was 2- to 3-fold greater than the risk based on genotype alone. AMD donors carrying the ARMS2 and HTRA1 risk alleles were the most likely to exhibit elevated CEP markers. Receiver operating characteristic curves suggest that CEP markers alone can discriminate between AMD and control plasma donors with approximately 76% accuracy and in combination with genomic markers, provide up to approximately 80% discrimination accuracy. CEP plasma biomarkers, particularly in combination with genomic markers, offer a potential early warning system for predicting susceptibility to this blinding disease.
机译:为了早期检测与年龄相关的黄斑变性(AMD)的易感性,我们通过ELISA在916 AMD和488个对照供体中对血浆羧乙基吡咯(CEP)氧化蛋白修饰和CEP自身抗体进行了定量。在AMD血浆中,平均CEP加合物和自身抗体水平分别升高了约60%和约30%,并且在AMD中,两种CEP标记升高的比值比在对照患者中高了约3倍。对与年龄相关的黄斑病易感性2(ARMS2),高温需求因子A1(HTRA1),补体因子H(CFH)和补体C3相关的AMD风险多态性进行基因分型。那些表现出高CEP标记和高风险基因型的人预测的AMD风险比仅基于基因型的风险高2至3倍。携带ARMS2和HTRA1风险等位基因的AMD供体最有可能表现出升高的CEP标记。接收器工作特征曲线表明,仅CEP标记就能以约76%的准确度区分AMD和对照血浆供体,并与基因组标记结合使用,可提供高达约80%的识别准确度。 CEP血浆生物标志物,特别是与基因组标志物的组合,为预测这种致盲性疾病的易感性提供了潜在的预警系统。

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