Identification of key biomolecules in rheumatoid arthritis through the reconstruction of comprehensive disease-specific biological networks.

In this study, several gene expression data including synovial tissue and macrophages from synovial tissues were integrated with a holistic perspective and the molecular targets and signatures in RA were determined. Differentially expressed genes (DEGs) were identified from each dataset by comparing diseased and healthy samples. Afterward, the RA-specific protein-protein interaction (PPI) and the transcriptional regulatory network were reconstructed by using several biomolecule interaction data. Key biomolecules were determined through a statistical test employing the hypergeometric probability density function by using the physical interactions of transcriptional regulators and PPI. The integrative analyses of DEGs indicated that there were 110 and 494 common genes between synovial tissues and macrophages related datasets, respectively. Common DEGs of all datasets were identified as 25 genes and these core genes which might be feasible to uncover the mutual biological mechanism insights behind the RA pathogenesis were used for disease specific biological networks reconstruction. It was determined the hub proteins, novel key biomolecules (i.e. receptor, transcription factors and miRNAs) and biomolecules interactions by using the core DEGs. It was identified STAT1, RAC2 and KYNU as hub proteins, PEPD as a receptor, NR4A1, MEOX2, KLF4, IRF1 and MYB as TFs, miR-299, miR-8078, miR-146a, miR-3659 and miR-6882 as key miRNAs. It was determined that biomolecule interaction scenarios ...
Source: Autoimmunity - Category: Allergy & Immunology Tags: Autoimmunity Source Type: research