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A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE

OBJECTIVES: SLE is a severe autoimmune disease characterized by autoreactive B cells and IC formation, which causes systemic inflammation. B cell–targeted therapy could be a promising treatment strategy in SLE patients; nevertheless, randomized clinical trials have not always been successful. Howeve...

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Autores principales: van Dam, Laura S, Osmani, Zgjim, Kamerling, Sylvia W A, Kraaij, Tineke, Bakker, Jaap A  , Scherer, Hans U, Rabelink, Ton J, Voll, Reinhard E, Alexander, Tobias, Isenberg, David A, van Kooten, Cees, Teng, Y K Onno
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7516125/
https://www.ncbi.nlm.nih.gov/pubmed/31951278
http://dx.doi.org/10.1093/rheumatology/kez623
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author van Dam, Laura S
Osmani, Zgjim
Kamerling, Sylvia W A
Kraaij, Tineke
Bakker, Jaap A  
Scherer, Hans U
Rabelink, Ton J
Voll, Reinhard E
Alexander, Tobias
Isenberg, David A
van Kooten, Cees
Teng, Y K Onno
author_facet van Dam, Laura S
Osmani, Zgjim
Kamerling, Sylvia W A
Kraaij, Tineke
Bakker, Jaap A  
Scherer, Hans U
Rabelink, Ton J
Voll, Reinhard E
Alexander, Tobias
Isenberg, David A
van Kooten, Cees
Teng, Y K Onno
author_sort van Dam, Laura S
collection PubMed
description OBJECTIVES: SLE is a severe autoimmune disease characterized by autoreactive B cells and IC formation, which causes systemic inflammation. B cell–targeted therapy could be a promising treatment strategy in SLE patients; nevertheless, randomized clinical trials have not always been successful. However, some groups have demonstrated beneficial effects in severe SLE patients with off-label rituximab (RTX) with belimumab (BLM), or bortezomib (BTZ), which targeted different B cells subsets. This study assembled sera from SLE cohorts treated with RTX+BLM (n = 15), BTZ (n = 11) and RTX (n = 16) to get an in-depth insight into the immunological effects of these therapies on autoantibodies and IC formation. METHODS: Autoantibodies relevant for IC formation and the avidity of anti-dsDNA were determined by ELISA. IC-mediated inflammation was studied by complement levels and ex vivo serum-induced neutrophil extracellular trap formation. RESULTS: Reductions in autoantibodies were observed after all approaches, but the spectrum differed depending upon the treatment. Specifically, only RTX+BLM significantly decreased anti-C1q. Achieving seronegativity of ≥1 autoantibody, specifically anti-C1q, was associated with lower disease activity. In all SLE patients, the majority of anti-dsDNA autoantibodies had low avidity. RTX+BLM significantly reduced low-, medium- and high-avidity anti-dsDNA, while RTX and BTZ only significantly reduced medium avidity. IC-mediated inflammation, measured by C3 levels and neutrophil extracellular trap formation, improved after RTX+BLM and RTX but less after BTZ. CONCLUSION: This study demonstrated the impact of different B cell–targeted strategies on autoantibodies and IC formation and their potential clinical relevance in SLE.
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spelling pubmed-75161252020-09-30 A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE van Dam, Laura S Osmani, Zgjim Kamerling, Sylvia W A Kraaij, Tineke Bakker, Jaap A   Scherer, Hans U Rabelink, Ton J Voll, Reinhard E Alexander, Tobias Isenberg, David A van Kooten, Cees Teng, Y K Onno Rheumatology (Oxford) Clinical Science OBJECTIVES: SLE is a severe autoimmune disease characterized by autoreactive B cells and IC formation, which causes systemic inflammation. B cell–targeted therapy could be a promising treatment strategy in SLE patients; nevertheless, randomized clinical trials have not always been successful. However, some groups have demonstrated beneficial effects in severe SLE patients with off-label rituximab (RTX) with belimumab (BLM), or bortezomib (BTZ), which targeted different B cells subsets. This study assembled sera from SLE cohorts treated with RTX+BLM (n = 15), BTZ (n = 11) and RTX (n = 16) to get an in-depth insight into the immunological effects of these therapies on autoantibodies and IC formation. METHODS: Autoantibodies relevant for IC formation and the avidity of anti-dsDNA were determined by ELISA. IC-mediated inflammation was studied by complement levels and ex vivo serum-induced neutrophil extracellular trap formation. RESULTS: Reductions in autoantibodies were observed after all approaches, but the spectrum differed depending upon the treatment. Specifically, only RTX+BLM significantly decreased anti-C1q. Achieving seronegativity of ≥1 autoantibody, specifically anti-C1q, was associated with lower disease activity. In all SLE patients, the majority of anti-dsDNA autoantibodies had low avidity. RTX+BLM significantly reduced low-, medium- and high-avidity anti-dsDNA, while RTX and BTZ only significantly reduced medium avidity. IC-mediated inflammation, measured by C3 levels and neutrophil extracellular trap formation, improved after RTX+BLM and RTX but less after BTZ. CONCLUSION: This study demonstrated the impact of different B cell–targeted strategies on autoantibodies and IC formation and their potential clinical relevance in SLE. Oxford University Press 2020-01-17 /pmc/articles/PMC7516125/ /pubmed/31951278 http://dx.doi.org/10.1093/rheumatology/kez623 Text en © The Author(s) 2020. Published by Oxford University Press on behalf of the British Society for Rheumatology. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Clinical Science
van Dam, Laura S
Osmani, Zgjim
Kamerling, Sylvia W A
Kraaij, Tineke
Bakker, Jaap A  
Scherer, Hans U
Rabelink, Ton J
Voll, Reinhard E
Alexander, Tobias
Isenberg, David A
van Kooten, Cees
Teng, Y K Onno
A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE
title A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE
title_full A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE
title_fullStr A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE
title_full_unstemmed A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE
title_short A reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in SLE
title_sort reverse translational study on the effect of rituximab, rituximab plus belimumab, or bortezomib on the humoral autoimmune response in sle
topic Clinical Science
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7516125/
https://www.ncbi.nlm.nih.gov/pubmed/31951278
http://dx.doi.org/10.1093/rheumatology/kez623
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