机构地区:[1]Shenzhen Key Laboratory of Synthetic Genomics,Guangdong Provincial Key Laboratory of Synthetic Genomics,CAS Key Laboratory of Quantitative Engineering Biology,Shenzhen Institute of Synthetic Biology,Shenzhen Institutes of Advanced Technology,Chinese Academy of Sciences,Shenzhen 518055,China [2]Department of Urology,Shenzhen Second People’s Hospital,the First Affiliated Hospital of Shenzhen University,International Cancer Center,Shenzhen University School of Medicine,Shenzhen 518039,China [3]State Key Laboratory of Chemical Biology and Drug Discovery,Food Safety and Technology Research Centre and Department of Applied Biology and Chemical Technology,The Hong Kong Polytechnic University,Hong Kong 999077,China [4]Department of Medicinal Chemistry,Shantou University Medical College,Shantou 515041,China
出 处:《Acta Biochimica et Biophysica Sinica》2022年第12期1909-1916,共8页生物化学与生物物理学报(英文版)
基 金:supported by the grants from the National Key R&D Program of China(No.2019YFA0906000);the Guangdong Basic and Applied Basic Research Foundation(No.2020A1515110032);Guangdong Provincial Key Laboratory of Synthetic Genomics(No.2019B030301006);Shenzhen Key Laboratory of Synthetic Genomics(No.ZDSYS201802061806209);Shenzhen Institute of Synthetic Biology Scientific Research Program(Nos.HSY899011058,HSE199011345,and HSE199011058).
摘 要:The autoantibody in patients’serum can act as a biomarker for diagnosing cancer,and the differences in autoantibodies are significantly correlated with the changes in their target proteins.In this study,16 renal cancer(RC)patients were assigned to the disease group,and 16 healthy people were assigned to the healthy control(HC)group.The human proteome microarray consisting of>19,500 proteins was used to examine the differences in IgG and IgM autoantibodies in sera between RC and HC.The comparative analysis of the microarray results shows that 101 types of IgG and 25 types of IgM autoantibodies are significantly higher in RC than in HC.Highly responsive autoantibodies can be candidate biomarkers(e.g.,anti-KCNAB2 IgG and anti-RCN1 IgM).Extensive enzyme-linked immunosorbent assay(ELISA)was performed to screen sera in 72 RC patients and 66 healthy volunteers to verify the effectiveness of the new autoantibodies.The AUCs of anti-KCNAB2 IgG and anti-GAPDH IgG were 0.833 and 0.753,respectively.KCNAB2 achieves high protein expression,and its high mRNA level is confirmed to be an unfavorable prognostic marker in clear cell renal cell carcinoma(ccRCC)tissues.This study suggests that the highthroughput human proteome microarray can effectively screen autoantibodies in serum as candidate biomarkers,and their corresponding target proteins can lay a basis for the in-depth investigation into renal cancer.
关 键 词:renal cancer AUTOANTIBODY BIOMARKER human proteome microarray
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