What question did this study set out to answer?

This research aims to identify causal proteins and potential drug targets for asthma using mendelian randomization and other analyses.

March 2, 2026Open Access

Proteome-wide Mendelian randomization identifies therapeutic targets for asthma

Key Points

This research aims to identify causal proteins and potential drug targets for asthma using mendelian randomization and other analyses.
Conducted mendelian randomization analysis to assess causal relationships
Performed phenome-wide association analysis to identify associated proteins
Utilized colocalization analysis to confirm protein associations
Analyzed transcriptome and single-cell data for expression patterns
Examined protein interactions for therapeutic implications
NPNT and NEGR1 showed significant protective effects against asthma
TNFAIP3 indicated a suggestive association with asthma protection in MR analyses
COLOC analysis highlighted NPNT and NEGR1 as promising drug targets
NPNT was highly expressed in Type II pneumocytes, while NEGR1 was upregulated in key immune cells

Abstract

Objectives: Asthma is a prevalent chronic inflammatory disease that involves a complex interaction between various cells of the innate and adaptive immune systems and epithelial cells. Anti-inflammatory therapeutic approaches have proven superior in controlling asthma and reducing exacerbation rates and are receiving increasing attention. The treatment of asthma is a potentially actionable target pending further validation. This study presented integrative evidence that supports both previously reported and emerging causal proteins, as well as potential drug targets, for asthma. Methods: Mendelian randomization (MR) analysis, colocalization (COLOC) analysis, phenome-wide association (PWAS) analysis, transcriptome analysis, single-cell data analysis, protein–protein interaction medication targets analysis. Results: Nephronectin (NPNT) and neuronal growth regulator 1 (NEGR1) were found to be statistically significantly associated with a noticeable protective effect against asthma, tumor necrosis factor, alpha-induced protein 3 (TNFAIP3) showed a suggestive statistical association with a protective effect against asthma in MR analyses. COLOC indicated that NPNT and NEGR1 have greater potential as drug targets. Compared with normal tissues, NPNT exhibited a higher expression level in Type II pneumocytes; NEGR1 was upregulated in smooth muscle cells, regulatory T cells, plasmacytoid dendritic cells, helper T cells; TNFAIP3 expression was decreased in Cluster of differentiation 4 (CD4)-positive alpha-beta T cells, lung ciliated cell 1, smooth muscle cells, whereas it was elevated in CD8-positive alpha-beta T cell 1, helper T cells, and myelocytes in asthma lung tissues. The interaction between Integrin alpha-8 (ITGA8) and NPNT, as well as the interaction between melanocortin-4 receptor and NEGR1, might serve as potential therapeutic targets. Conclusion: NPNT and NEGR1 could be promising targets for current asthma medications. NEGR1 was first identified in MR of asthma, and we further performed across-omics validation to verify the roles of NPNT, NEGR1, and TNFAIP3.

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Proteome-wide Mendelian randomization identifies therapeutic targets for asthma

Key Points

Abstract

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