自身抗体
噬菌体展示
生物
微阵列
单克隆抗体
DNA微阵列
抗体
蛋白质组学
免疫学
分子生物学
基因
遗传学
基因表达
作者
Pablo San Segundo‐Acosta,Ana Montero‐Calle,Manuel Fuentes,Alberto Rábano,Mayte Villalba,Rodrigo Barderas
标识
DOI:10.1021/acs.jproteome.9b00258
摘要
The characterization of the humoral response in Alzheimer’s disease (AD) patients might aid in detecting the disease at early stages. We have combined phage display and protein microarrays to identify AD autoantibodies and their target biomarkers. After enrichment of the T7 phage display libraries from AD and healthy brain tissue mRNA in AD-specific phages, 1536 monoclonal phages were printed on microarrays to probe them with 8 AD and 8 healthy control sera. A total of 57 phages showed higher seroreactivity in AD. In total, 13 out of the 44 unique sequences displayed on the phages were selected for validation using 68 AD and 52 healthy control sera. Peptides from Anthrax toxin receptor 1, Nuclear protein 1, Glycogen phosphorylase, and Olfactory receptor 8J1 expressed in bacteria as HaloTag fusion proteins showed a statistically significant ability to discriminate between AD patients and controls. The identified panel of AD autoantibodies might provide new insights into the blood-based diagnosis of the disease.
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