# An international, multicentre, interventional, randomised, assessor-blinded trial to MAXimise the METHotrexate therapy potential in patients with active rheumatoid arthritis (MethMax trial): study protocol for a randomised controlled trial

**Authors:** Karolina Anderle, Daniela Sieghart, Martina Durechova, François Bonnay, Andreas Kerschbaumer, Katerina Chatzidionysiou, Rachel Knevel, Costantino Pitzalis, Siri Lillegraven, Espen A. Haavardsholm, Eirik Klami Kristianslund, Catalin Codreanu, Claudiu Popescu, Elisa Gremese, Sabina de Geest, Agnes Kocher, Souzi Makri, Daniel Aletaha, Helga Lechner-Radner

PMC · DOI: 10.1186/s13063-026-09519-4 · 2026-03-23

## TL;DR

This trial tests if changing methotrexate delivery method and dose helps more rheumatoid arthritis patients reach remission.

## Contribution

A novel trial design to optimize methotrexate therapy through dose and route adjustment in rheumatoid arthritis.

## Key findings

- Testing if subcutaneous methotrexate improves remission rates compared to oral delivery.
- Exploring biomarkers to understand individual methotrexate metabolism and adherence.
- Providing evidence for optimized methotrexate management in rheumatoid arthritis.

## Abstract

Methotrexate (MTX) is recommended as first-line therapy in patients with rheumatoid arthritis (RA), proven to be effective, safe and inexpensive. However, a significant proportion of patients does not achieve disease remission with MTX monotherapy. Main reasons include insufficient dose up-titration to the maximal recommended oral dose or the delayed switch to a subcutaneous administration route. We hypothesise, that by dose and route optimisation, a higher proportion of patients can achieve remission. Further, exploratory biomarkers will give new insights on individual MTX metabolism and drug adherence.

The MethMax trial is a prospective, randomised, assessor-blinded, parallel-group, superiority, low-intervention trial, including 182 patients across 7 European countries. Patients with active RA, naïve to biologic (except tumour necrosis factor alpha inhibitors; TNFi) or targeted synthetic antirheumatic drugs, who have been on a stable oral MTX therapy for the past 3 months are randomised in a 1:1 ratio to 25 mg MTX weekly, either administered orally or subcutaneously. Additionally, both arms receive a short-term glucocorticoid regimen with a four-week tapering and withdrawal protocol. The primary endpoint is the difference in proportion of patients achieving remission defined as the Clinical Disease Activity Index (CDAI) ≤ 2.8 at week 24, comparing the dose/route optimisation and oral dose optimisation. The active study duration for each patient is 24 weeks. Study visits take place at baseline, weeks 4, 12, 16 and 24. Clinical efficacy and safety parameters are obtained at each visit. Patient-reported outcomes, exploratory biomarkers as well as medication adherence are assessed. Written consent is obtained for all participants. The study has received regulatory approval via the Clinical Trials Information System and Medicines and Healthcare products Regulatory Agency and has included the first patient in August 2024.

The anticipated results will provide insights whether the subcutaneous administration of 25 mg MTX is advantageous in achieving CDAI remission when compared to the oral intake after 24 weeks and inform the community regarding the utility of established and newly developed biomarkers, as well as the potential impact of inadequate drug adherence.

The MethMax study is aimed to optimise individual therapy in RA and provide more precise pharmacological MTX management recommendations.

## Linked entities

- **Chemicals:** Methotrexate (PubChem CID 4112)
- **Diseases:** rheumatoid arthritis (MONDO:0008383)

## Full-text entities

- **Genes:** GPT (glutamic--pyruvic transaminase) [NCBI Gene 2875] {aka AAT1, ALT, ALT1, GPT1, SGPT}, ATIC (5-aminoimidazole-4-carboxamide ribonucleotide formyltransferase/IMP cyclohydrolase) [NCBI Gene 471] {aka AICAR, AICARFT, HEL-S-70p, IMPCHASE, PURH}, TSC1 (TSC complex subunit 1) [NCBI Gene 7248] {aka LAM, TSC}, TNF (tumor necrosis factor) [NCBI Gene 7124] {aka DIF, IMD127, TNF-alpha, TNFA, TNFSF2, TNLG1F}, GGTLC5P (gamma-glutamyltransferase light chain 5 pseudogene) [NCBI Gene 653590] {aka GGT}, ALB (albumin) [NCBI Gene 213] {aka FDAHT, HSA, PRO0883, PRO0903, PRO1341}, CMPK1 (cytidine/uridine monophosphate kinase 1) [NCBI Gene 51727] {aka CK, CMK, CMPK, UMK, UMP-CMPK, UMPK}, CRP (C-reactive protein) [NCBI Gene 1401] {aka PTX1}, SLC17A5 (solute carrier family 17 member 5) [NCBI Gene 26503] {aka AST, ISSD, NSD, SD, SIALIN, SIASD}, MUC1 (mucin 1, cell surface associated) [NCBI Gene 4582] {aka ADMCKD, ADMCKD1, ADTKD2, CA 15-3, CD227, Ca15-3}, DHFR (dihydrofolate reductase) [NCBI Gene 1719] {aka DHFR1, DYR}, GGT1 (gamma-glutamyltransferase 1) [NCBI Gene 2678] {aka CD224, D22S672, D22S732, GGT, GGT 1, GGTD}, CDAN1 (codanin 1) [NCBI Gene 146059] {aka CDA1, CDAI, CDAN1A, DLT, PRO1295}
- **Diseases:** Inflammatory rheumatic diseases (MESH:D012213), pulmonary or infectious complications (MESH:D003141), Fatigue (MESH:D005221), pyelonephritis (MESH:D011704), thrombocytopenia (MESH:D013921), vomiting (MESH:D014839), inflammatory (MESH:D007249), painful joints (MESH:D018771), opportunistic infections (MESH:D009894), gastrointestinal symptoms (MESH:D012817), hepatitis (MESH:D056486), rheumatic diseases (MESH:D012216), Chronic Illness (MESH:D002908), tender joints, swollen joints (MESH:D007592), histoplasmosis (MESH:D006660), FACIT-F (OMIM:102510), pain (MESH:D010146), gastrointestinal adverse events (MESH:D002318), leukopenia (MESH:D007970), toxicity (MESH:D064420), pneumocystis (MESH:D011020), stiffness (MESH:C566112), TDM (MESH:D000081015), Reduced kidney function (MESH:D007680), abdominal discomfort (MESH:D000007), aspergillosis (MESH:D001228), alcohol or substance abuse (MESH:D019966), headache (MESH:D006261), Stomatitis (MESH:D013280), cytomegalovirus (MESH:D003586), RA (MESH:D001172), Haematologic abnormalities (MESH:D006402), EOS (MESH:C538157), inflammatory bowel disease (MESH:D015212), nausea (MESH:D009325), anaemia (MESH:D000743), infection (MESH:D007239), hepatitis B and C (MESH:D006509), ICH (MESH:D002543), CTIS (MESH:D000075902), pneumonia (MESH:D011014), herpes zoster (MESH:D006562)
- **Chemicals:** prednisone (MESH:D011241), adalimumab (MESH:D000068879), Folate (MESH:D005492), MTX polyglutamates (MESH:C014085), 5-Aminoimidazole-4-carboxamide ribonucleotide (MESH:C031143), Crea (MESH:D003404), METHotrexate (MESH:D008727), glutamate (MESH:D018698), PGA (MESH:D011454), bilirubin (MESH:D001663), 7-OH-MTX (MESH:C011864), adenosine (MESH:D000241), EDTA (MESH:D004492), infliximab (MESH:D000069285), PGs (MESH:D010715), HBs antigen (-)
- **Species:** hepatitis C virus [taxon 11103], Homo sapiens (human, species) [taxon 9606], Torque teno virus (species) [taxon 68887]
- **Cell lines:** SF-36v1 — Mus musculus (Mouse), Embryonic stem cell (CVCL_6D22)

## Figures

1 figure with captions in the complete paper: https://tomesphere.com/paper/PMC13036923/full.md

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Source: https://tomesphere.com/paper/PMC13036923