
AbstractThe genetic contribution of protein-coding variants to immune-mediated diseases (IMDs) remains underexplored. Through whole exome sequencing of 40 IMDs in 350,770 UK Biobank participants, we identified 162 unique genes in 35 IMDs, among which 124 were novel genes. Several genes, including FLG which is associated with atopic dermatitis and asthma, showed converging evidence from both rare and common variants. 91 genes exerted significant effects on longitudinal outcomes (interquartile range of Hazard Ratio: 1.12-5.89). Mendelian randomization identified five causal genes, of which four were approved drug targets (CDSN, DDR1, LTA, and IL18BP). Proteomic analysis indicated that mutations associated with specific IMDs might also affect protein expression in other IMDs. For example, DXO (celiac disease-related gene) and PSMB9 (alopecia areata-related gene) could modulate CDSN (autoimmune hypothyroidism-, psoriasis-, asthma-, and Graves’ disease-related gene) expression. Identified genes predominantly impact immune and biochemical processes, and can be clustered into pathways of immune-related, urate metabolism, and antigen processing. Our findings identified protein-coding variants which are the key to IMDs pathogenesis and provided new insights into tailored innovative therapies.
Male, Adult, Proteomics, Science, Q, Genetic Variation, Filaggrin Proteins, Middle Aged, Mendelian Randomization Analysis, Article, Asthma, Dermatitis, Atopic, Immune System Diseases, Exome Sequencing, Mutation, Humans, Female, Genetic Predisposition to Disease, Aged
Male, Adult, Proteomics, Science, Q, Genetic Variation, Filaggrin Proteins, Middle Aged, Mendelian Randomization Analysis, Article, Asthma, Dermatitis, Atopic, Immune System Diseases, Exome Sequencing, Mutation, Humans, Female, Genetic Predisposition to Disease, Aged
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