Max Yates1, Louise E Hamilton1, Frances Elender1, Loretta Dean1, Helen Doll1, Alex J MacGregor1, Joegi Thomas1, Karl Gaffney2. 1. From the Department of Rheumatology, Norfolk and Norwich University Hospital National Health Service (NHS) Foundation Trust; Norwich Medical School, University of East Anglia, Norwich; ICON Commercialisation and Outcomes, Oxford; James Paget University Hospital, Gorleston, UK.M. Yates, BSc(Hons), MBBS, MSc, MRCP, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust, and Norwich Medical School, University of East Anglia; L.E. Hamilton, BM BCh, MD, MRCP; F. Elender, BSc, PhD; L. Dean, PGDip, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust; H. Doll, MSc, DPhil, Norwich Medical School, University of East Anglia, and ICON Commercialisation and Outcomes; A.J. MacGregor, MBBS, MD, PhD, FRCP, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust, and Norwich Medical School, University of East Anglia; J. Thomas, MBBS, MD, FRCP, James Paget University Hospital; K. Gaffney, MB ChB, BAO(Hons), FEGEMS, FRCPI, FRCP, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust. 2. From the Department of Rheumatology, Norfolk and Norwich University Hospital National Health Service (NHS) Foundation Trust; Norwich Medical School, University of East Anglia, Norwich; ICON Commercialisation and Outcomes, Oxford; James Paget University Hospital, Gorleston, UK.M. Yates, BSc(Hons), MBBS, MSc, MRCP, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust, and Norwich Medical School, University of East Anglia; L.E. Hamilton, BM BCh, MD, MRCP; F. Elender, BSc, PhD; L. Dean, PGDip, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust; H. Doll, MSc, DPhil, Norwich Medical School, University of East Anglia, and ICON Commercialisation and Outcomes; A.J. MacGregor, MBBS, MD, PhD, FRCP, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust, and Norwich Medical School, University of East Anglia; J. Thomas, MBBS, MD, FRCP, James Paget University Hospital; K. Gaffney, MB ChB, BAO(Hons), FEGEMS, FRCPI, FRCP, Rheumatology, Norfolk and Norwich University Hospital NHS Foundation Trust. karl.gaffney@nnuh.nhs.uk.
Abstract
OBJECTIVE: To investigate, in a pilot randomized controlled trial, whether etanercept (ETN) 25 mg once weekly is effective at maintaining a clinical response in patients with ankylosing spondylitis (AS) who have responded to the standard 50 mg dose. METHODS:Adults with AS not responding to conventional therapies were prescribed ETN 50 mg once weekly for 6 months. Responders as defined by the Bath Ankylosing Spondylitis Disease Activity Index (BASDAI) were randomly assigned to taper to 25 mg once weekly or continue on 50 mg and followed for a further 6 months. The primary outcome measure was maintenance of a 50% reduction in the BASDAI or fall in BASDAI by ≥ 2 units and a ≥ 2-unit reduction in BASDAI spinal pain as measured on a 10-point visual analog scale at 6 months postrandomization. RESULTS: Of 89 patients assessed for eligibility, 59 were enrolled; 47 (80%) had sufficient clinical response and were eligible for randomization, 24 were assigned to continue receiving ETN 50 mg, and 23 to taper to 25 mg. After 6 months, 20 (83%) of the 50 mg arm maintained clinical response compared with 12 (52%) of the 25 mg arm (a difference of -31%, 95% CI -58% - -5%). CONCLUSION: Although this pilot study demonstrates that treatment with ETN 25 mg was less effective at maintaining treatment response in the stepdown phase, 52% of participants maintained treatment response. Future research should address which patients are suitable for tapering.
RCT Entities:
OBJECTIVE: To investigate, in a pilot randomized controlled trial, whether etanercept (ETN) 25 mg once weekly is effective at maintaining a clinical response in patients with ankylosing spondylitis (AS) who have responded to the standard 50 mg dose. METHODS: Adults with AS not responding to conventional therapies were prescribed ETN 50 mg once weekly for 6 months. Responders as defined by the Bath Ankylosing Spondylitis Disease Activity Index (BASDAI) were randomly assigned to taper to 25 mg once weekly or continue on 50 mg and followed for a further 6 months. The primary outcome measure was maintenance of a 50% reduction in the BASDAI or fall in BASDAI by ≥ 2 units and a ≥ 2-unit reduction in BASDAI spinal painas measured on a 10-point visual analog scale at 6 months postrandomization. RESULTS: Of 89 patients assessed for eligibility, 59 were enrolled; 47 (80%) had sufficient clinical response and were eligible for randomization, 24 were assigned to continue receiving ETN 50 mg, and 23 to taper to 25 mg. After 6 months, 20 (83%) of the 50 mg arm maintained clinical response compared with 12 (52%) of the 25 mg arm (a difference of -31%, 95% CI -58% - -5%). CONCLUSION: Although this pilot study demonstrates that treatment with ETN 25 mg was less effective at maintaining treatment response in the stepdown phase, 52% of participants maintained treatment response. Future research should address which patients are suitable for tapering.
Authors: Michael M Ward; Atul Deodhar; Lianne S Gensler; Maureen Dubreuil; David Yu; Muhammad Asim Khan; Nigil Haroon; David Borenstein; Runsheng Wang; Ann Biehl; Meika A Fang; Grant Louie; Vikas Majithia; Bernard Ng; Rosemary Bigham; Michael Pianin; Amit Aakash Shah; Nancy Sullivan; Marat Turgunbaev; Jeff Oristaglio; Amy Turner; Walter P Maksymowych; Liron Caplan Journal: Arthritis Care Res (Hoboken) Date: 2019-08-21 Impact factor: 4.794
Authors: Michael M Ward; Atul Deodhar; Lianne S Gensler; Maureen Dubreuil; David Yu; Muhammad Asim Khan; Nigil Haroon; David Borenstein; Runsheng Wang; Ann Biehl; Meika A Fang; Grant Louie; Vikas Majithia; Bernard Ng; Rosemary Bigham; Michael Pianin; Amit Aakash Shah; Nancy Sullivan; Marat Turgunbaev; Jeff Oristaglio; Amy Turner; Walter P Maksymowych; Liron Caplan Journal: Arthritis Rheumatol Date: 2019-08-22 Impact factor: 15.483
Authors: Celia A J Michielsens; Nathan den Broeder; Michelle L M Mulder; Frank H J van den Hoogen; Lise M Verhoef; Alfons A den Broeder Journal: Rheumatology (Oxford) Date: 2022-05-30 Impact factor: 7.046
Authors: Alexandre Sepriano; Andrea Regel; Désirée van der Heijde; Jürgen Braun; Xenofon Baraliakos; Robert Landewé; Filip Van den Bosch; Louise Falzon; Sofia Ramiro Journal: RMD Open Date: 2017-01-27