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Identifying Novel Osteoarthritis-Associated Genes in Human Cartilage Using a Systematic Meta-Analysis and a Multi-Source Integrated Network. | LitMetric

AI Article Synopsis

  • Osteoarthritis is the most common joint disorder, marked by the breakdown of articular cartilage, but effective treatments remain elusive.
  • This study aimed to identify key genes and micro-RNAs linked to osteoarthritis through a systematic meta-analysis of gene expression in affected cartilage.
  • The research identified an enriched pathway related to cellular senescence and constructed a comprehensive network of 1,689 genes, leading to the discovery of five new proteins associated with osteoarthritis that could be potential targets for future treatments.

Article Abstract

Osteoarthritis, the most common joint disorder, is characterised by deterioration of the articular cartilage. Many studies have identified potential therapeutic targets, yet no effective treatment has been determined. The aim of this study was to identify and rank osteoarthritis-associated genes and micro-RNAs to prioritise those most integral to the disease. A systematic meta-analysis of differentially expressed mRNA and micro-RNAs in human osteoarthritic cartilage was conducted. Ingenuity pathway analysis identified cellular senescence as an enriched pathway, confirmed by a significant overlap (p < 0.01) with cellular senescence drivers (CellAge Database). A co-expression network was built using genes from the meta-analysis as seed nodes and combined with micro-RNA targets and SNP datasets to construct a multi-source information network. This accumulated and connected 1689 genes which were ranked based on node and edge aggregated scores. These bioinformatic analyses were confirmed at the protein level by mass spectrometry of the different zones of human osteoarthritic cartilage (superficial, middle, and deep) compared to normal controls. This analysis, and subsequent experimental confirmation, revealed five novel osteoarthritis-associated proteins (PPIB, ASS1, LHDB, TPI1, and ARPC4-TTLL3). Focusing future studies on these novel targets may lead to new therapies for osteoarthritis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9030814PMC
http://dx.doi.org/10.3390/ijms23084395DOI Listing

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