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Cover of Plasma exchange and glucocorticoids to delay death or end-stage renal disease in anti-neutrophil cytoplasm antibody-associated vasculitis: PEXIVAS non-inferiority factorial RCT

Plasma exchange and glucocorticoids to delay death or end-stage renal disease in anti-neutrophil cytoplasm antibody-associated vasculitis: PEXIVAS non-inferiority factorial RCT

Health Technology Assessment, No. 26.38

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Author Information and Affiliations
Southampton (UK): National Institute for Health and Care Research; .

Headline

This trial showed that plasma exchange did not delay onset of end-stage renal disease or death and reduced oral steroid dosing was no less effective than the standard dose.

Abstract

Background:

Anti-neutrophil cytoplasm antibody-associated vasculitis is a multisystem, autoimmune disease that causes organ failure and death. Physical removal of pathogenic autoantibodies by plasma exchange is recommended for severe presentations, along with high-dose glucocorticoids, but glucocorticoid toxicity contributes to morbidity and mortality. The lack of a robust evidence base to guide the use of plasma exchange and glucocorticoid dosing contributes to variation in practice and suboptimal outcomes.

Objectives:

We aimed to determine the clinical efficacy of plasma exchange in addition to immunosuppressive therapy and glucocorticoids with respect to death and end-stage renal disease in patients with severe anti-neutrophil cytoplasm antibody-associated vasculitis. We also aimed to determine whether or not a reduced-dose glucocorticoid regimen was non-inferior to a standard-dose regimen with respect to death and end-stage renal disease.

Design:

This was an international, multicentre, open-label, randomised controlled trial. Patients were randomised in a two-by-two factorial design to receive either adjunctive plasma exchange or no plasma exchange, and either a reduced or a standard glucocorticoid dosing regimen. All patients received immunosuppressive induction therapy with cyclophosphamide or rituximab.

Setting:

Ninety-five hospitals in Europe, North America, Australia/New Zealand and Japan participated.

Participants:

Participants were aged ≥ 16 years with a diagnosis of granulomatosis with polyangiitis or microscopic polyangiitis, and either proteinase 3 anti-neutrophil cytoplasm antibody or myeloperoxidase anti-neutrophil cytoplasm antibody positivity, and a glomerular filtration rate of < 50 ml/minute/1.73 m2 or diffuse alveolar haemorrhage attributable to active anti-neutrophil cytoplasm antibody-associated vasculitis.

Interventions:

Participants received seven sessions of plasma exchange within 14 days or no plasma exchange. Oral glucocorticoids commenced with prednisolone 1 mg/kg/day and were reduced over different lengths of time to 5 mg/kg/day, such that cumulative oral glucocorticoid exposure in the first 6 months was 50% lower in patients allocated to the reduced-dose regimen than in those allocated to the standard-dose regimen. All patients received the same glucocorticoid dosing from 6 to 12 months. Subsequent dosing was at the discretion of the treating physician.

Primary outcome:

The primary outcome was a composite of all-cause mortality and end-stage renal disease at a common close-out when the last patient had completed 10 months in the trial.

Results:

The study recruited 704 patients from June 2010 to September 2016. Ninety-nine patients died and 138 developed end-stage renal disease, with the primary end point occurring in 209 out of 704 (29.7%) patients: 100 out of 352 (28%) in the plasma exchange group and 109 out of 352 (31%) in the no plasma exchange group (adjusted hazard ratio 0.86, 95% confidence interval 0.65 to 1.13; p = 0.3). In the per-protocol analysis for the non-inferiority glucocorticoid comparison, the primary end point occurred in 92 out of 330 (28%) patients in the reduced-dose group and 83 out of 325 (26%) patients in the standard-dose group (partial-adjusted risk difference 0.023, 95% confidence interval 0.034 to 0.08; p = 0.5), thus meeting our non-inferiority hypothesis. Serious infections in the first year occurred in 96 out of 353 (27%) patients in the reduced-dose group and in 116 out of 351 (33%) patients in the standard-dose group. The rate of serious infections at 1 year was lower in the reduced-dose group than in the standard-dose group (incidence rate ratio 0.69, 95% confidence interval 0.52 to 0.93; p = 0.016).

Conclusions:

Plasma exchange did not prolong the time to death and/or end-stage renal disease in patients with anti-neutrophil cytoplasm antibody-associated vasculitis with severe renal or pulmonary involvement. A reduced-dose glucocorticoid regimen was non-inferior to a standard-dose regimen and was associated with fewer serious infections.

Future work:

A meta-analysis examining the effects of plasma exchange on kidney outcomes in anti-neutrophil cytoplasm antibody-associated vasculitis is planned. A health-economic analysis of data collected in this study to examine the impact of both plasma exchange and reduced glucocorticoid dosing is planned to address the utility of plasma exchange for reducing early end-stage renal disease rates. Blood and tissue samples collected in the study will be examined to identify predictors of response to plasma exchange in anti-neutrophil cytoplasm in antibody-associated vasculitis. The benefits associated with reduced glucocorticoid dosing will inform future studies of newer therapies to permit further reduction in glucocorticoid exposure. Data from this study will contribute to updated management recommendations for anti-neutrophil cytoplasm antibody-associated vasculitis.

Limitations:

This study had an open-label design which may have permitted observer bias; however, the nature of the end points, end-stage renal disease and death, would have minimised this risk. Despite being, to our knowledge, the largest ever trial in anti-neutrophil cytoplasm antibody-associated vasculitis, there was an insufficient sample size to assess clinically useful benefits on the separate components of the primary end-point: end-stage renal disease and death. Use of a fixed-dose plasma exchange regimen determined by consensus rather than data-driven dose ranging meant that some patients may have been underdosed, thus reducing the therapeutic impact. In particular, no biomarkers have been identified to help determine dosing in a particular patient, although this is one of the goals of the biomarker plan of this study.

Trial registration:

This trial is registered as ISRCTN07757494, EudraCT 2009-013220-24 and Clinicaltrials.gov NCT00987389.

Funding:

This project was funded by the National Institute for Health and Care Research (NIHR) Health Technology Assessment programme and will be published in full in Health Technology Assessment; Vol. 26, No. 38. See the NIHR Journals Library website for further project information.

Contents

About the Series

Health Technology Assessment
ISSN (Print): 1366-5278
ISSN (Electronic): 2046-4924

Declared competing interests of authors: David Jayne has received research grants from Chemocentryx Inc. (San Carlos, CA, USA), GlaxoSmithKline (Brentford, UK), Roche Holding AG (Basel, Switzerland)/Genentech (South San Francisco, CA, USA) and Sanofi (Paris, France)/Genzyme (Cambridge, MA, USA); has received consultancy fees from AstraZeneca (Cambridge, UK), Boehringer Ingelheim (Ingelheim am Rhein, Germany), Chemocentryx Inc., GlaxoSmithKline, InflaRx (Jena, Germany), Insmed Inc. (Bridgewater Township, NJ, USA), Roche Holding AG/Genentech and Vifor Pharma (Opfikon, Switzerland); and was a member of the Efficacy and Mechanism Evaluation (EME) Prioritisation Group (2012–16) and EME Strategy Group (2015–18). Michael Walsh was supported by a New Investigator Award from the Canadian Institutes of Health Research, and reports other funding from Bayer HealthCare (Leverkusen, Germany) and Ionis Pharmaceuticals (Carlsbad, CA, USA) outside the submitted work. Peter A Merkel reports receiving consulting fees from AbbVie (Lake Bluff, IL, USA), Biogen Inc. (Cambridge, MA, USA), CSL Behring (King of Prussia, PA, USA), Genzyme, Insmed Inc. (Bridgewater Township, NJ, USA), Janssen Pharmaceuticals (Beerse, Belgium), Kiniksa Pharmaceuticals (Bermuda) and Sparrow (Portland, OR, USA); grant support and consulting fees from AstraZeneca, Boehringer Ingelheim, Bristol-Myers Squibb (New York, NY, USA), Celgene (Summit, NJ, USA), Chemocentryx Inc., Genentech/Roche Holding AG, GlaxoSmithKline (Brentford, UK) and InflaRx; grant support from Kypha Inc. (St. Louis, MO, USA); and supplies from Terumo BCT, Inc. (Lakewood, CO, USA). Xavier Puéchal reports personal fees and non-financial support from Roche Holding AG, personal fees from Pfizer Inc. (New York, NY, USA) and LFB (Paris, France) and non-financial support from Sanofi outside the submitted work. Shouichi Fujimoto reports receiving equipment related to plasma exchange from Asahi Kasei Medical Co., Ltd (Tokyo, Japan). Carmel Hawley reports consumables from Terumo BCT (Lakewood, CO, USA), Fresenius (Bad Homburg, Germany) and Gambro (Deerfield, IL, USA); and grants from The National Health and Medical Research Council (NHMRC) Australia (26939, 2010–13, and 1086192, 2014–17), Shire (Lexington, MA, USA) and Amgen (Thousand Oaks, CA, USA) during the conduct of the study. Nader Khalidi reports advisory board fees and study drugs from Roche Holding AG and study drugs from Bristol-Myers Squibb outside the submitted work. Rachel Jones reports personal fees from Chemocentryx Inc. and grants from GlaxoSmithKline outside the submitted work. Christian Pagnoux reports grants and personal fees from Roche Holding AG, personal fees from Sanofi and Chemocentryx Inc. outside the submitted work. Toshiko Ito-Ihara reports receiving equipment related to plasma exchange from Asahi Kasei Medical Co., Ltd. Donna Reidlinger reports consumables from Terumo BCT, Inc., Fresenius (Bad Homburg, Germany) and Gambro, and grants from NHMRC (Canberra, ACT, Australia) (626939, 2010–13, and 1086192, 2014–17) during the conduct of the study. Keith Wheatley reports membership of the Health Technology Assessment (HTA) Clinical Trials Committee (2012–17).

Article history

The research reported in this issue of the journal was funded by the HTA programme as project number 08/56/04. The contractual start date was in June 2009. The draft report began editorial review in December 2018 and was accepted for publication in August 2021. The authors have been wholly responsible for all data collection, analysis and interpretation, and for writing up their work. The HTA editors and publisher have tried to ensure the accuracy of the authors’ report and would like to thank the reviewers for their constructive comments on the draft document. However, they do not accept liability for damages or losses arising from material published in this report.

Last reviewed: December 2018; Accepted: August 2021.

Copyright © 2022 Jayne et al. This work was produced by Jayne et al. under the terms of a commissioning contract issued by the Secretary of State for Health and Social Care. This is an Open Access publication distributed under the terms of the Creative Commons Attribution CC BY 4.0 licence, which permits unrestricted use, distribution, reproduction and adaption in any medium and for any purpose provided that it is properly attributed. See: https://creativecommons.org/licenses/by/4.0/. For attribution the title, original author(s), the publication source – NIHR Journals Library, and the DOI of the publication must be cited.
Bookshelf ID: NBK584491DOI: 10.3310/PNXB5040

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