Abstract
Objective. The Outcome Measures in Rheumatology (OMERACT) synovial tissue biopsy (STB) working group initiated an international effort to standardize STB analyses, define consensual items to inform treatment choices, and predict responses in rheumatoid arthritis (RA).
Methods. (1) A Delphi survey to determine items for STB analyses. (2) A multicenter retrospective study of STB data in patients with RA posttreatment with biological disease-modifying antirheumatic drugs.
Results. The Delphi survey identified 18 STB analyses items. Consensus on histological markers was achieved in the OMERACT 2018 SIG.
Conclusion. Six markers were identified for examination in a multicenter study designed to define an OMERACT-endorsed set of STB markers to predict responses to treatment.
Despite current therapeutic advances in rheumatoid arthritis (RA), predicting and achieving adequate treatment responses and remission remains elusive for a substantial proportion of patients. Indeed, even with biological disease-modifying antirheumatic drugs (bDMARD), rates of remission and improvement in function are suboptimal1,2. RA is a heterogeneous disease clinically and pathologically3,4, so one explanation for low response rates may be the current nontargeted, “trial and error” use of conventional DMARD (cDMARD) and bDMARD. Although there have been several attempts to identify biomarkers in peripheral blood to guide therapeutic choices for individual patients5,6,7, they have generally proven inconclusive and inconsistent.
Because the synovium is the major target of disease and a robust measure of treatment response in RA8, it is probable that the search for biomarker(s) to guide therapy and predict response to treatment may best be addressed by synovial tissue biopsy (STB) analyses9,10,11,12. Indeed, despite current therapeutic approaches, 30–40% of patients are resistant to therapy, having persistent synovitis and erosion progression11. An alternative “pathobiological” approach13 basing treatment selection upon individual patient factors such as STB analyses could provide a better rationale for the selection of appropriate bDMARD, resulting in better individual patient responses.
STB are not currently considered standard of care in randomized controlled trials or for choice of therapy for a variety of reasons14,15, including relative lack of access and technical expertise in their performance and evaluation16. An important step advancing their use occurred at the OMERACT 2016 STB SIG, establishing the feasibility, reliability, and validity of minimally invasive ultrasound (US)-guided synovial biopsy techniques according to the OMERACT Filter 2.014,17,18.
Regarding evaluation and interpretation of STB, considerable heterogeneity remains across centers. Before addressing more advanced techniques to interpret STB, such as RNA sequencing and transcriptomics19, standardization of standard histologic and immunohistochemistry (IHC) analysis is critical. Given the relative ease of performing histological semiquantitative analysis (SQA), it is likely to be the most feasible technique to direct treatment choices, facilitating rapid decision making from the bench to the bedside.
However, before proposing routine use of standardized STB histologic and IHC techniques to guide therapy, several factors must be satisfied, including (1) uniformity of biopsy handling and analyses across centers, (2) creation of a uniform quality score, (3) validation of the score to identify the relationship between immunopathology and therapeutic responses, and (4) identification of novel STB markers of disease phenotype and outcomes and to match these with circulating biomarkers and imaging techniques. Hence, the strategic aims and objectives of the OMERACT STB SIG were to initially conduct a Delphi survey regarding STB handling and analytic procedures, followed by analysis of STB histological markers to assess whether they can (1) guide choices of appropriate therapeutic agents, (2) predict responses to treatment, and thereby (3) define a consensual set of histological items to be used for prediction of therapeutic responses in RA.
MATERIALS AND METHODS
The initial Delphi survey (Table 1 and Supplementary Data, available with the online version of this article) invited participation from relevant experts in performance and analysis of STB. The survey was conducted in 3 stages. The first stage included 44 items in 2 distinct clinical parts: clinical practice and translational research. Each participant rated each item on a scale of 1 to 5 (1 = strongly disagree, 2 = disagree, 3 = neutral, 4 = agree, 5 = strongly agree). The second round constituted iterative refinements from the earlier round.
Based on the consensual set of items that emerged from this Delphi, the OMERACT STB SIG decided to perform a study to determine whether STB histological markers can be used to guide treatment choices, predict responses, and define a consensual set of histological items for future use.
This analysis of STB histological markers will be performed retrospectively on collected STB at baseline and followup ≥ 6 months in biologic treatment–naive patients with RA [fulfilling the American College of Rheumatology (ACR)/European League Against Rheumatism (EULAR) 2010 criteria for diagnosis] following initiation of treatment with bDMARD. Synovial biopsies will be stained for H&E, CD68+, CD3+, CD19+, or CD20+, presence of lymphoid aggregates, and staining of blood vessels.
Following initial quality control, all slides will be independently scored (using SQA) by 2 observers at each center who are blinded to the design of the study and responses to the treatment. Each observer will be asked for a percent likelihood of response to each of the following bDMARD: interleukin 6 blockade, T cell costimulation inhibition, tumor necrosis factor-α (TNF-α) blockade, and anti-CD20, depending on histological features.
Statistical analyses will include descriptive analyses, logistic regression, and κ coefficients for each histological marker.
RESULTS
Delphi exercise: first round
Twenty-seven experts from 19 centers were contacted by e-mail. Twenty participants (85%) from 18 centers responded; of these, 19 (95%) were rheumatologists, and 1 (5%) was a pathologist. Twenty-three out of 44 items (52.3%) from the clinical practice portion of the first questionnaire were selected for the second round based on their score and percentage of agreement. Of these, 5 remained unchanged, 16 were modified, and 2 were added according to participants’ comments. Nineteen out of 43 items (44%) from the translational research component of the first questionnaire were selected for the second round; of these, 10 remained unchanged and 9 were modified according to participants’ comments; no new item was proposed.
Delphi exercise: second round
From the clinical practice component of the second round, 20/23 (87%) and 18/19 items (95%) from the clinical practice and translational research components, respectively, were selected for the third round.
Face-to-face meeting
Results of the second round were disseminated through participating members and orally presented to the task force at the EULAR Synovitis Study Group meeting in June 2017. All task force members agreed on the final set of items. Items with a median score > 3.5 and percentage of agreement > 70% were selected for further rounds. Statistics were performed using GraphPad Prism 6.0.
Results of synovial biopsy study
The planned multicenter (n = 5 per center) study will analyze STB histological markers for macrophages, T cells, B cells, lymphoid aggregates, and blood vessels to determine likelihood of response to treatment with bDMARD (tocilizumab, abatacept, TNF inhibitor, or rituximab). These results will be presented once the planned study has been completed.
Results from discussion at OMERACT 2018
At the OMERACT STB SIG, results of the Delphi survey and methodological details of the next component (analysis of histological markers on retrospectively collected STB) were presented and discussed.
A consensus was reached regarding quality control for histology and SQA and IHC markers to be used in STB analyses. It was decided that the next steps would be the finalization of participating centers and a uniformly agreed-upon protocol, to establish an atlas of SQA to ensure uniformity across centers and provide a reference standard for future studies. A qualitative study on participant experiences with arthroscopy and US-guided STB was also proposed.
DISCUSSION
Standardization of synovial tissue analysis as a predictor to guide therapy and response to treatment
Although there is considerable literature on responsiveness to changes in RA disease activity following treatment with c/bDMARD16, there are limited data, despite a strong pathobiologic rationale that demonstrates the usefulness of STB guiding treatment choices13. This is particularly relevant in the current context of availability of bDMARD with diverse mechanisms of action, but relatively similar responses across treatments13 and may likely reflect synovial pathotype heterogeneity as shown in a recent prospective study that reported higher levels of B cell infiltrates and lymphoid aggregates in anticitrullinated protein antibody-positive patients20. Another notable study by Dennis, et al9 revealed better responses to TNF inhibitors with an underlying “myeloid” as opposed to “lymphoid” or other synovial phenotypes.
Another important factor contributing to the heterogeneity of results is the varying methodology assessing STB across centers. Although analysis of IHC by SQA has been used as one of the fastest quantification techniques, it is subject to observer error. Despite attempts to reduce this error by observer training and standardization and using 2 observers and a consensus score, none of these methods have been thoroughly validated16.
Data and insights following discussion at OMERACT 2018
Following the OMERACT STB SIG, further steps are to finalize a staining protocol, and formally invite STB centers of excellence to participate in the study, which will be undertaken through the EULAR/ACR STB SIG. A quality-control exercise will follow, which will result in an atlas of SQA as the reference standard for this and future studies. Following patient selection across centers and appropriate IHC staining, slides will be uploaded onto a central server for blinded analyses, followed by formal statistical analyses, including histopathological correlations with clinical and imaging outcomes.
Following this exercise, it is expected that the OMERACT STB working group will be able to create and validate an acceptable uniform quality score, gain insights into histological markers that will help identify relationships between synovial immunopathology and treatment responses (or lack thereof), and facilitate identification of novel STB biomarkers of disease phenotype and outcomes and match these with circulating biomarkers and imaging techniques.
ONLINE SUPPLEMENT
Supplementary material accompanies the online version of this article.
- Accepted for publication November 20, 2018.