Proteome-scale autoantibody profiling in PSC: Associations with clinical phenotypes and evidence for neuroendocrine deregulations
Martin Cornillet, Aiva Lundberg Båve, Dan Sun, Ghada Nouairia, Christina Villard, Aristeidis Grigoriadis, Erik von Seth, Hannes Jansson, María Bueno Álvez, Sofia Bergström, Peter Nilsson, Mathias Uhlén, Fredrik Edfors, Per Stål, Mårten Werner, Mårten Werner, Nils Nyhlin

TL;DR
This study identifies autoantibodies linked to disease progression and immune-related tissues in primary sclerosing cholangitis, suggesting a role for neuroendocrine dysregulation.
Contribution
The study provides proteome-scale autoantibody profiling in PSC, revealing associations with clinical traits and evidence of neuroendocrine deregulation.
Findings
Autoantibodies are associated with clinical severity, comorbidities, and disease progression in PSC.
Autoantigen targets are enriched in immune-privileged tissues like the brain, testis, and retina.
Neuroendocrine dysregulation is supported by multiomics analysis and PSC risk variant data.
Abstract
Primary sclerosing cholangitis (PSC) is a rare cholestatic liver disease with heterogeneous phenotypes and progression. Autoimmune traits, such as the presence of autoantibodies, are suspected to drive its heterogeneity. We performed a proteome-scale autoantibody screen of IgG and IgA isotypes using >42,100 protein fragments. This was followed by a validation of 1,153 selected autoantibodies, in serum samples from 466 patients with PSC in a longitudinal setting using the SUPRIM cohort and 214 controls. We identified autoantibodies associated with clinical phenotypes, biochemical and clinical severity, comorbidities, and disease progression (e.g. alkaline phosphatase and albumin level p <e-10, presence of hepatobiliary malignancies p <0.001, seroconversion before transplantation p <0.001). Rather than a single universal autoantibody marker, small patient subgroups were positive for…
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Taxonomy
TopicsLiver Diseases and Immunity · Systemic Lupus Erythematosus Research · IgG4-Related and Inflammatory Diseases
