# Hemidesmosome Mutations Contribute to the Onset and Severity of Acquired Autoimmune Bullous Diseases

**Authors:** Shan Cao, Tianyu Wang, Chen Lv, Shanshan Ma, Gongqi Yu, Qianqian Xia, Tingting Liu, Yueqian Yu, Lele Sun, Xiaoyan Pei, Qing Zhao, Zhenzhen Wang, Chuan Wang, Yongxia Liu, Shengli Chen, Jianwen Wang, Guizhi Zhou, Hong Liu, Yonghu Sun, Furen Zhang

PMC · DOI: 10.1002/mco2.70627 · 2026-02-15

## TL;DR

This study shows that mutations in hemidesmosome-related genes contribute to the development and severity of acquired autoimmune bullous diseases like pemphigoid.

## Contribution

The study identifies novel hemidesmosome gene variants and demonstrates their functional impact in autoimmune bullous diseases using genetic, proteomic, and model organism approaches.

## Key findings

- ITGA6, LAMC2, and EPPK1 mutations significantly affect hemidesmosome-related protein expression.
- ITGA6 mutations disrupt hemidesmosome assembly in C. elegans models, altering structural components.
- ITGA6 mutations activate NOD-like receptor–NF-κB–TNF–pyroptosis signaling pathways, affecting disease progression.

## Abstract

Hemidesmosomes are structures that anchor junctions between basal epithelial cells and the basement membrane, essential for skin integrity. Genetic mutation of hemidesmosomes was well documented for the inherited bullous disorder, but is rarely investigated for acquired bullous disorders. We designed a 16‐gene targeted capture panel and sequenced 202 patients with hemidesmosomes‐related acquired disorders and 123 healthy controls, identifying 114 pathogenic variants in 15 genes, including 20.2% novel variants. Clinical relevance (disease severity and outcome) and immunohistochemistry results demonstrated that ITGA6, LAMC2, and EPPK1 mutations significantly affected the expression of hemidesmosome‐related proteins, compared with controls with non‐carriers. Functional studies in Caenorhabditis elegans models with transmission electron microscopy and confocal microscopy demonstrated that ITGA6 (ina‐1) mutation can disrupt the hemidesmosomes assembly network, such as cytolinker (vab‐10a) and apical (mup‐4) and basal (let‐805), thereby disrupting the hemidesmosome structure. This represents a quantitative to qualitative change in pemphigoid disease. Transcriptomic and serum proteomic analyses further revealed that ITGA6 mutations perturb epithelial development and hemidesmosome integrity, with both missense/loss‐of‐function variants leading to activation of  NOD‐like receptor–NF‐κB–TNF–pyroptosis signaling pathways. These findings highlight the critical role of hemidesmosome genetic variants in the development of not only inherited but also acquired autoimmune bullous disorders.

This study examined hemidesmosome assembly‐related genes in pemphigoid diseases, revealing variants linked to disease onset and severity. Functional analyses, including Caenorhabditis elegans models, Ker‐CT transcriptomics, human proteomics, etc., demonstrated that ITGA6 mutations destabilize hemidesmosomes, disrupt dermal–epidermal adhesion, and increase susceptibility in patients, providing mechanistic insight into autoimmune targeting in pemphigoid disorders.

## Linked entities

- **Genes:** ITGA6 (integrin subunit alpha 6) [NCBI Gene 3655], LAMC2 (laminin subunit gamma 2) [NCBI Gene 3918], EPPK1 (epiplakin 1) [NCBI Gene 83481], Mup4 (major urinary protein 4) [NCBI Gene 17843], let-805 (Fibronectin type-III domain-containing protein;SHOCT domain-containing protein) [NCBI Gene 175384]
- **Proteins:** NFKB1 (nuclear factor kappa B subunit 1), TNF (tumor necrosis factor)
- **Species:** Caenorhabditis elegans (taxon 6239), Mus musculus (taxon 10090)

## Full-text entities

- **Genes:** ITGA6 (integrin subunit alpha 6) [NCBI Gene 3655] {aka CD49f, ITGA6A, ITGA6B, JEB6, VLA-6}, NFKB1 (nuclear factor kappa B subunit 1) [NCBI Gene 4790] {aka CVID12, EBP-1, KBF1, NF-kB, NF-kB1, NF-kappa-B1}, LAMC2 (laminin subunit gamma 2) [NCBI Gene 3918] {aka B2T, BM600, CSF, EBR2, EBR2A, JEB3A}, EPPK1 (epiplakin 1) [NCBI Gene 83481] {aka EPIPL, EPIPL1}, TNF (tumor necrosis factor) [NCBI Gene 7124] {aka DIF, IMD127, TNF-alpha, TNFA, TNFSF2, TNLG1F}
- **Diseases:** bullous disorder (MESH:D012872), -related acquired (MESH:D000163), Acquired Autoimmune Bullous Diseases (MESH:D001327), pemphigoid disease (MESH:D010391)
- **Species:** Caenorhabditis elegans (species) [taxon 6239], Homo sapiens (human, species) [taxon 9606]

## Figures

8 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12906664/full.md

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Source: https://tomesphere.com/paper/PMC12906664