Pos0193 evaluation of Cress in the Phase 2 Randomised Placebo-Controlled Study of Sequential Belimumab/Rituximab Administration in Patients With Primary Sjögren’s Syndrome

Bootsma, H.P.R.; Arends, S.; Wolff, Liseth de; Clark, Kenneth L.; Maurik, André van; Mistry, Prafull; Shukla, P.; Nihtyanova, S.; Fox, Norma Lynn; Roth, D.

doi:10.1136/annrheumdis-2022-eular.1336

Cited by 3 publications

(2 citation statements)

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“…As such, the novel cellular and molecular pathology biomarkers reported in this study will require further validation. Such work is currently being implemented as part of the IMI2‐NECESSITY consortium (https://www.imi.europa.eu/projects-results/project-factsheets/necessity), which will provide access to longitudinal labial and parotid biopsies from recently completed clinical trials, including ones in which patients received abatacept 43 and a most recent trial in which patients received rituximab in combination with anti‐BAFF monoclonal antibody (belimumab) 44,45 …”

Section: Discussionmentioning

confidence: 99%

Serum and Tissue Biomarkers Associated With Composite of Relevant Endpoints for Sjögren Syndrome (CRESS) and Sjögren Tool for Assessing Response (STAR) to B Cell–Targeted Therapy in the Trial of Anti–B Cell Therapy in Patients With Primary Sjögren Syndrome (TRACTISS)

Pontarini,

Sciacca,

Chowdhury

et al. 2024

Arthritis & Rheumatology

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ObjectivesTo identify peripheral and salivary gland (SG) biomarkers of response/resistance to B‐cell depletion based on the novel concise CRESS (cCRESS) and candidate STAR composite endpoints.MethodsLongitudinal analysis of peripheral blood and SG biopsies pre‐ and post‐treatment from the TRACTISS trial combining FACS immunophenotyping, serum cytokines and SG bulk‐RNA‐sequencing.ResultsRituximab prevented the worsening of SG inflammation observed in the placebo arm, by inhibiting the accumulation of class‐switched memory‐B‐cells within the SG. Furthermore, rituximab significantly downregulated genes involved in immune‐cell recruitment, lymphoid organization alongside antigen presentation, and T‐cell co‐stimulatory pathways. In the peripheral compartment, rituximab downregulated immunoglobulins and autoantibodies together with proinflammatory cytokines and chemokines. Interestingly, STAR responders displayed significantly higher baseline levels of CXCL13, IL‐22, IL‐17A, IL‐17F and TNFα while a longitudinal analysis of serum T‐cell‐related cytokines showed selective reduction in both STAR and cCRESS responders. Conversely, cCRESS response was better associated with biomarkers of SG immunopathology, with responders showing significant decrease in SG B‐cell infiltration and reduced expression of transcriptional gene modules related to T‐cell costimulation, complement activation and FcγR engagement. Finally, cCRESS and STAR response was associated with a significant improvement in SG exocrine function, linked to transcriptional evidence of SG epithelial and metabolic restoration.ConclusionsRituximab modulates both peripheral and SG inflammation, preventing the deterioration of exocrine function linked with functional and metabolic restoration of the glandular epithelium. Response assessed by newly developed cCRESS and STAR criteria was associated with differential modulation of peripheral and SG biomarkers, emerging as novel tools for patient stratification.image

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Section: Discussionmentioning

confidence: 99%

Serum and Tissue Biomarkers Associated With Composite of Relevant Endpoints for Sjögren Syndrome (CRESS) and Sjögren Tool for Assessing Response (STAR) to B Cell–Targeted Therapy in the Trial of Anti–B Cell Therapy in Patients With Primary Sjögren Syndrome (TRACTISS)

Pontarini,

Sciacca,

Chowdhury

et al. 2024

Arthritis & Rheumatology

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“…Such new endpoints may prove useful in future studies aimed at developing new treatments for patients with pSS. A recent post hoc analysis of the current study assessed CRESS outcomes, and treatment with belimumab + rituximab was generally associated with a numerically higher concise CRESS response rate compared with monotherapies at week 24 (52.9% belimumab + rituximab, 36.8% belimumab, 31.3% rituximab), week 52 (58.8% belimumab + rituximab, 42.1% belimumab, 25.0% rituximab), and week 68 (35.3% belimumab + rituximab, 36.8% belimumab, 18.8% rituximab) (75). However, the placebo response for CRESS was notable (week 24, 50.0%; week 52, 50.0%; week 68, 12.5%) and similar to the placebo response for ClinESSDAI.…”

Section: Discussionmentioning

confidence: 99%

A randomized, phase II study of sequential belimumab and rituximab in primary Sjögren’s syndrome

Mariette¹,

Barone²,

Baldini³

et al. 2022

JCI Insight

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BACKGROUND Primary Sjögren’s syndrome (pSS) is characterized by B cell hyperactivity and elevated B-lymphocyte stimulator (BLyS). Anti-BLyS treatment (e.g., belimumab) increases peripheral memory B cells; decreases naive, activated, and plasma B cell subsets; and increases stringency on B cell selection during reconstitution. Anti-CD20 therapeutics (e.g., rituximab) bind and deplete CD20-expressing B cells in circulation but are less effective in depleting tissue-resident CD20 + B cells. Combined, these 2 mechanisms may achieve synergistic effects. METHODS This 68-week, phase II, double-blind study (GSK study 201842) randomized 86 adult patients with active pSS to 1 of 4 arms: placebo, s.c. belimumab, i.v. rituximab, or sequential belimumab + rituximab. RESULTS Overall, 60 patients completed treatment and follow-up until week 68. The incidence of adverse events (AEs) and drug-related AEs was similar across groups. Infections/infestations were the most common AEs, and no serious infections of special interest occurred. Near-complete depletion of minor salivary gland CD20 + B cells and a greater and more sustained depletion of peripheral CD19 + B cells were observed with belimumab + rituximab versus monotherapies. With belimumab + rituximab, reconstitution of peripheral B cells occurred, but it was delayed compared with rituximab. At week 68, mean (± standard error) total EULAR Sjögren’s syndrome disease activity index scores decreased from 11.0 (1.17) at baseline to 5.0 (1.27) for belimumab + rituximab and 10.4 (1.36) to 8.6 (1.57) for placebo. CONCLUSION The safety profile of belimumab + rituximab in pSS was consistent with the monotherapies. Belimumab + rituximab induced enhanced salivary gland B cell depletion relative to the monotherapies, potentially leading to improved clinical outcomes. TRIAL REGISTRATION ClinicalTrials.gov NCT02631538. FUNDING Funding was provided by GSK.

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Emerging treatment for Sjögren’s disease: a review of recent phase II and III trials

Fox

McCoy

2023

Expert Opinion on Emerging Drugs

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Pos0193 evaluation of Cress in the Phase 2 Randomised Placebo-Controlled Study of Sequential Belimumab/Rituximab Administration in Patients With Primary Sjögren’s Syndrome

Cited by 3 publications

References 0 publications

Serum and Tissue Biomarkers Associated With Composite of Relevant Endpoints for Sjögren Syndrome (CRESS) and Sjögren Tool for Assessing Response (STAR) to B Cell–Targeted Therapy in the Trial of Anti–B Cell Therapy in Patients With Primary Sjögren Syndrome (TRACTISS)

Serum and Tissue Biomarkers Associated With Composite of Relevant Endpoints for Sjögren Syndrome (CRESS) and Sjögren Tool for Assessing Response (STAR) to B Cell–Targeted Therapy in the Trial of Anti–B Cell Therapy in Patients With Primary Sjögren Syndrome (TRACTISS)

A randomized, phase II study of sequential belimumab and rituximab in primary Sjögren’s syndrome

Emerging treatment for Sjögren’s disease: a review of recent phase II and III trials

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