Abstract Background Chronic rhinosinusitis with nasal polyps (CRSwNP) is a persistent inflammatory airway disease characterized by high recurrence rates despite medical therapy and surgery. The molecular mechanisms underlying disease progression and treatment failure remain incompletely understood, limiting the development of targeted therapies. Transcriptomic studies provide an opportunity to systematically uncover dysregulated genes and pathways involved in CRSwNP pathogenesis. Methods A systematic review was conducted according to PRISMA guidelines across PubMed, Scopus, EMBASE, ScienceDirect, and Web of Science to identify transcriptomics-based case–control studies investigating gene expression in human CRSwNP tissues. Differentially expressed genes (DEGs) reported in eligible studies were compiled and subjected to functional enrichment analysis using Gene Ontology tools. Gene–disease associations with asthma were explored using DisGeNET, and potential drug–gene interactions were identified through DGIdb. Results Fourteen studies comprising 577 samples met the inclusion criteria, yielding 1495 DEGs, of which 70 were experimentally validated. Functional enrichment analysis identified ten significantly dysregulated biological processes, including blood vessel morphogenesis, calcium ion transport, ERK1/ERK2 cascade, intracellular cation homeostasis, regulation of angiogenesis, regulation of actin cytoskeleton organization, and MAPK cascade signaling. Comparative analysis with asthma-associated genes identified 43 shared genes with high confidence. Several genes, including IL4R, IL6R, CSF3, ICAM1, MBL2, SOD1, SCGB1A1, and TSLP, demonstrated interactions with approved or investigational drugs, highlighting potential repurposing opportunities. Conclusions This systematic transcriptomic integration identifies key biological pathways and druggable targets involved in CRSwNP pathogenesis. These findings provide a molecular framework for understanding disease mechanisms and support the development of pathway-oriented and personalized therapeutic strategies in CRSwNP.
Khayer et al. (Wed,) studied this question.