Safety and patient response as indicated by biomarker changes to binding immunoglobulin protein in the phase I/IIA RAGULA clinical trial in rheumatoid arthritis

Bruce Kirkham; Khaldoun Chaabo; Christopher Hall; Toby Garrood; Timothy Mant; Elizabeth Allen; Alexandra Vincent; Joana C Vasconcelos; Andrew T Prevost; Gabriel S Panayi; Valerie M Corrigall

doi:10.1093/rheumatology/kew287

Safety and patient response as indicated by biomarker changes to binding immunoglobulin protein in the phase I/IIA RAGULA clinical trial in rheumatoid arthritis

Rheumatology (Oxford). 2016 Nov;55(11):1993-2000. doi: 10.1093/rheumatology/kew287. Epub 2016 Aug 7.

Authors

Affiliations

¹ Department of Rheumatology, Guys and St Thomas' NHS Foundation Trust Hospital.
² Academic Department of Rheumatology, Centre for Molecular and Cellular Biology of Inflammation, King's College London.
³ Quintiles Clinical Trials Unit.
⁴ Department of Primary Care and Public Health Sciences, King's College London, London, UK.
⁵ Department of Rheumatology, Guys and St Thomas' NHS Foundation Trust Hospital gabriel.panayi@kcl.ac.uk.

Abstract

Objectives: Binding immunoglobulin protein (BiP) is a human endoplasmic reticulum-resident stress protein. In pre-clinical studies it has anti-inflammatory properties due to the induction of regulatory cells. This randomized placebo-controlled, dose ascending double blind phase I/IIA trial of BiP in patients with active RA, who had failed accepted therapies, had the primary objective of safety. Potential efficacy was measured by DAS28-ESR and changes in biomarkers.

Methods: Twenty-four patients with active RA who had failed one or more DMARDs were sequentially assigned to three groups each of eight patients randomly allocated to receive placebo (two patients) or BiP (six patients), 1, 5 or 15 mg. Patients received a single i.v. infusion over 1 h and were observed as inpatients overnight. A 12-week follow-up for clinical, rheumatological and laboratory assessments for safety, efficacy (DAS28-ESR) and biomarker analysis was performed.

Results: No infusion reactions or serious adverse drug reactions were noted. Adverse events were evenly distributed between placebo and BiP groups with no BiP-related toxicities. Haematological, renal and metabolic parameters showed no drug-related toxicities. Remission was only achieved by patients in the 5 and 15 mg groups, and not patients who received placebo or 1 mg BiP. Good DAS28-ESR responses were achieved in all treatment groups. The BiP responding patients showed significantly lower serum concentrations of CRP, 2 weeks post-infusion compared with pre-infusion levels, and of VEGF and IL-8 from the placebo group.

Conclusion: BiP (⩽15 mg) is safe in patients with active RA. Some patients had clinical and biological improvements in RA activity. BiP merits further study.

Trial registration: ISRCTN registry, http://isrctn.com, ISRCTN22288225 and EudraCT, https://eudract.ema.europa.eu, 2011-005831-19.

Keywords: BiP; CRP; IL-8; VEGF; changes in biomarkers; efficacy; first-in-human trial; prolonged activity; regulatory cells; safety.

Publication types

Clinical Trial, Phase I
Clinical Trial, Phase II
Randomized Controlled Trial

MeSH terms

Adolescent
Adult
Aged
Antirheumatic Agents / administration & dosage*
Antirheumatic Agents / adverse effects
Arthritis, Rheumatoid / drug therapy*
Biological Products / therapeutic use
Biomarkers / metabolism
Double-Blind Method
Female
Humans
Infusions, Intravenous
Interleukin-8 / metabolism
Lymphokines / administration & dosage*
Lymphokines / adverse effects
Male
Middle Aged
Recombinant Proteins
Remission Induction
Treatment Outcome
Vascular Endothelial Growth Factor A / metabolism
Young Adult

Substances

Antirheumatic Agents
Biological Products
Biomarkers
Interleukin-8
Lymphokines
Recombinant Proteins
Vascular Endothelial Growth Factor A
immunoglobulin-binding factors