The relationship between disease activity and UDCA response criteria in primary biliary cholangitis: A cohort study
David E.J. Jones,
Aaron Wetten,
Ben Barron-Millar,
Laura Ogle,
George Mells,
Steven Flack,
Richard Sandford,
John Kirby,
Jeremy Palmer,
Sophie Brotherston,
Laura Jopson,
John Brain,
Graham R. Smith,
Steve Rushton,
Rebecca Jones,
Simon Rushbrook,
Douglas Thorburn,
Stephen D. Ryder,
Gideon Hirschfield,
Jessica K. Dyson
Affiliations
David E.J. Jones
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom; Corresponding author at: Translational and Clinical Research Institute, Medical School, Framlington Place, Newcastle-upon-Tyne, NE24HH United Kingdom.
Aaron Wetten
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom; Freeman Hospital, Newcastle-upon-Tyne, United Kingdom
Ben Barron-Millar
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom
Laura Ogle
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom
George Mells
Dept of Human Genetics, University of Cambridge, Cambridge, United Kingdom
Steven Flack
Dept of Human Genetics, University of Cambridge, Cambridge, United Kingdom
Richard Sandford
Dept of Human Genetics, University of Cambridge, Cambridge, United Kingdom
John Kirby
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom
Jeremy Palmer
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom
Sophie Brotherston
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom
Laura Jopson
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom
John Brain
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom
Graham R. Smith
Bioinformatics Support Unit (BSU), Newcastle University, Newcastle-upon-Tyne, United Kingdom
Steve Rushton
School of Natural and Environmental Science, Newcastle University, Newcastle-upon-Tyne, United Kingdom
Rebecca Jones
Liver Unit, St James’ Hospital, Leeds, United Kingdom
Simon Rushbrook
University Department of Hepatology, UEA Medical School, Norwich, United Kingdom
Douglas Thorburn
Liver Unit, Royal Free Hospital, London, United Kingdom
Stephen D. Ryder
NIHR Nottingham Biomedical Research centre at Nottingham University Hospitals NHS Trust, Nottingham, United Kingdom
Gideon Hirschfield
Queen Elizabeth Hospital, Birmingham, United Kingdom; Toronto Centre for Liver Disease, University of Toronto, Toronto, Canada
Jessica K. Dyson
Translational and Clinical Research Institute, Newcastle University, Newcastle-upon-Tyne, United Kingdom; Freeman Hospital, Newcastle-upon-Tyne, United Kingdom
Summary: Background: Uncertainty exists about how best to identify primary biliary cholangitis (PBC) patients who would benefit from second-line therapy. Existing, purely clinical, ursodeoxycholic acid (UDCA) response criteria accept degrees of liver biochemistry abnormality in responding patients, emerging data, however, suggest that any degree of ongoing abnormality may, in fact, be associated with an increased risk of adverse outcomes. This cohort study explores the link between response status, the biology of high-risk disease and its implications for clinical practice. Methods: Proteomics, exploring 19 markers previously identified as remaining elevated in PBC following UDCA therapy, were performed on 400 serum samples, from participants previously recruited to the UK-PBC Nested Cohort between 2014 and 2019. All participants had an established diagnosis of PBC and were taking therapeutic doses of UDCA for greater than 12 months. UDCA response status was assessed using Paris 1, Paris 2 and the POISE criteria, with additional analyses using normal liver blood tests stratified by bilirubin level. Statistical analysis using parametric t tests and 1-way ANOVA. Findings: Disease markers were statistically significantly higher in UDCA non-responders than in responders for all the UDCA response criteria, suggesting a meaningful link between biochemical disease status and disease mechanism. For each of the criteria, however, marker levels were also statistically significantly higher in responders with ongoing liver function test abnormality compared to those who had normalised their liver biochemistry. IL-4RA, IL-18-R1, CXCL11, 9 and 10, CD163 and ACE2 were consistently elevated across all responder groups with ongoing LFT abnormality. No statistically significant differences occurred between markers in normal LFT groups stratified by bilirubin level. Interpretation: This study provides evidence that any ongoing elevation in alkaline phosphatase levels in PBC after UDCA therapy is associated with some degree of ongoing disease activity. There was no difference in activity between patients with normal LFT when stratified by bilirubin. These findings suggest that if our goal is to completely control disease activity in PBC, then normalisation of alkaline phosphatase and bilirubin should be the treatment target. This would also simplify messaging around goals of therapy in PBC, benefiting both patients and clinicians. Funding: Funding by the UK Medical Research Council (Stratified Medicine Programme) and an independent research grant by Pfizer. The study funders played no role in the study design, data collection, data analyses, data interpretation or manuscript writing.
