Autoimmune fibroinflammation in IgG4-related ophthalmic disease: TLR8-dependent signaling pathways and fibrotic remodeling revealed by proteomic profiling
Yingxue Ma, Dejuan Song, Chuanjie Xu, GuangYu Li

TL;DR
This study identifies TLR8-dependent pathways and fibrosis markers in IgG4-related ophthalmic disease using proteomic analysis of lacrimal gland tissue.
Contribution
Novel proteomic profiling reveals TLR8 signaling and fibrotic markers in IgG4-ROD, offering potential diagnostic and therapeutic targets.
Findings
Patients with suspected IgG4-ROD share proteomic profiles with diagnosed cases, suggesting a common disease population.
Diagnosed IgG4-ROD cases show severe fibrosis and reduced lacrimal secretion function compared to controls.
TLR8-related proteins are upregulated, implicating TLR signaling in disease pathogenesis.
Abstract
Immunoglobulin G4-related ophthalmic disease (IgG4-ROD) is an immune-mediated ocular condition characterized by tumefactive lesions with IgG4+ plasma cell infiltration, and commonly affecting the lacrimal gland, extraocular muscles, and trigeminal nerves.The precise pathogenesis of IgG4-ROD remains unclear. Elucidating its molecular mechanisms is crucial for the development of targeted molecular therapies. To investigate the molecular pathogenesis of IgG4-ROD, we conducted a case-controlled study involving 15 patients who presented at the Second Hospital of Jilin University between 2021 and 2022. In accordance with the comprehensive diagnostic criteria for IgG4-related disease (IgG4-RD) established in 2011, participants were stratified into three distinct cohorts based on lacrimal gland histopathological findings: confirmed IgG4-ROD, suspected IgG4-ROD, and a control group. We then…
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Taxonomy
TopicsIgG4-Related and Inflammatory Diseases · Nasolacrimal Duct Obstruction Treatments · Sinusitis and nasal conditions
