# A Phenome-Wide Mendelian Randomization and Colocalization Study Reveals Genetic Association Between PBC and Other Autoimmune Disorders

**Authors:** Shuyi Shi, Minghui Liu, Haonan Gao, Fang Liu, Yuhu Song

PMC · DOI: 10.1155/cjgh/1716853 · 2025-07-20

## TL;DR

This study finds a genetic link between primary biliary cholangitis and hypothyroidism, identifying two genes that could be drug targets.

## Contribution

The study reveals novel genetic associations and potential drug targets between PBC and autoimmune disorders using MR-PheWAS and colocalization.

## Key findings

- Genetic liability to PBC is linked to higher risk of 25 traits, including hypothyroidism.
- Two genes, CCDC88B and MMEL1, are identified as potential drug targets for hypothyroidism.
- Bidirectional Mendelian randomization confirms causal associations between PBC and hypothyroidism.

## Abstract

Background: Primary biliary cholangitis (PBC) is a chronic autoimmune liver disease that is commonly associated with various other autoimmune disorders. We conducted a phenome-wide association study Mendelian randomization (MR-PheWAS) to determine genetic association between PBC and other diseases, particularly autoimmune disorders.

Methods: We performed a PheWAS to investigate the causal associations between PBC and related traits by conducting enrichment analysis of 35 PBC risk loci identified by prior GWAS and their matched control SNP sets in UK Biobank database. MR-PheWAS and bidirectional two-sample Mendelian randomization analysis were conducted to determine causal association between PBC and hypothyroidism. Colocalization analysis was conducted to investigate common genetic variants with hypothyroidism.

Results: Genetic liability to PBC was associated with a higher risk of 25 traits (hypothyroidism, asthma, allergic rhinitis, psoriasis, ulcerative colitis, and multiple sclerosis). After false discovery rate (FDR) correction, there exist 9 traits significantly difference. MR-PheWAS analysis demonstrated causal association between PBC and hypothyroidism, and bidirectional two-sample Mendelian randomization analysis was performed to validate it. The OR of hypothyroidism on PBC was 113.61(p=9.30E − 05), and PBC was also causally associated with hypothyroidism (OR: 1.005; p=4.33E − 09). Among the genes identified, CCDC88B and MMEL1 were found to have positive associations with the risk of hypothyroidism (CCDC88B: OR = 1.004, p=4.69E − 07; MMEL1: OR = 1.004, p=6.65E − 06) and FinnGen cohorts (CCDC88B: OR = 1.044; MMEL1: OR = 1.038). The two genes may be the drug targets for hypothyroidism (CCDC88B: coloc.abf-PPH4 = 94.7%; MMEL1: coloc.abf-PPH4 = 91.8%).

Conclusions: Our study revealed genetic association between PBC and hypothyroidism through a phenome-wide Mendelian randomization, and then, colocalization identified two potential drug targets for hypothyroidism.

## Linked entities

- **Genes:** CCDC88B (coiled-coil and HOOK domain protein 88B) [NCBI Gene 283234], MMEL1 (membrane metalloendopeptidase like 1) [NCBI Gene 79258]
- **Diseases:** Primary biliary cholangitis (MONDO:0005388), hypothyroidism (MONDO:0005420), asthma (MONDO:0004979), allergic rhinitis (MONDO:0011786), psoriasis (MONDO:0005083), ulcerative colitis (MONDO:0005101), multiple sclerosis (MONDO:0005301)

## Full-text entities

- **Genes:** CCDC88B (coiled-coil and HOOK domain protein 88B) [NCBI Gene 283234] {aka BRLZ, CCDC88, HKRP3, gipie}, MMEL1 (membrane metalloendopeptidase like 1) [NCBI Gene 79258] {aka MMEL2, NEP2, NEPII, NL1, NL2, SEP}
- **Diseases:** hypothyroidism (MESH:D007037), autoimmune liver disease (MESH:D008107), multiple sclerosis (MESH:D009103), PBC (MESH:D008105), ulcerative colitis (MESH:D003093), psoriasis (MESH:D011565), asthma (MESH:D001249), allergic rhinitis (MESH:D065631), Autoimmune Disorders (MESH:D001327)
- **Chemicals:** PPH4 (-)

## Figures

3 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12301091/full.md

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Source: https://tomesphere.com/paper/PMC12301091