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Background: Patients (pts) with gout refractory to oral urate-lowering therapy (ULT) have few treatment options. Pegloticase (pegylated uricase) lowers serum uric acid (sUA) in these pts, 1 but response rates are limited by anti-drug antibodies (ADAs), which decrease urate-lowering efficacy and increase infusion reaction (IR) risk. 2 Because methotrexate (MTX) is commonly used in RA and prevents ADA development against biologics, co-administering MTX with pegloticase in uncontrolled gout pts is of interest. A small open-label study of pegloticase+oral MTX suggested an increased efficacy rate, 3 so a randomized controlled trial (RCT) was conducted to compare pegloticase with/without MTX immunomodulation.
Objectives: To determine safety/efficacy of oral MTX as co-therapy with pegloticase for sustained urate-lowering response in a randomized placebo (PBO) controlled trial.
Methods: Pegloticase+MTX and pegloticase+PBO co-therapy were compared in uncontrolled gout pts (sUA≥7 mg/dL, ULT failure/intolerance, and ≥1 of the following: ≥1 tophus, ≥2 flares in past yr, chronic gouty arthritis). Primary endpoint was the proportion of Month 6 treatment responders (sUA<6 mg/dL for ≥80% of the time during Wks 20-24). Key exclusion criteria included MTX contraindication, immunosuppressant use, G6PD deficiency, and renal impairment (eGFR<40 ml/min/1.73 m 2 ). Pts were randomized 2:1 to oral MTX (15 mg/wk) or PBO. Following a 4 wk MTX/PBO run-in, pegloticase was initiated (Day 1). Both pegloticase (biweekly 8 mg infusions) and MTX/PBO were administered over 52-wks (treatment period). Efficacy was examined in the intent-to-treat population (ITT, all randomized pts); safety (AEs, laboratory values) in the safety population (all pts receiving ≥1 dose blinded MTX/PBO). Treatment was discontinued if pre-infusion sUA >6 mg/dL for 2 consecutive visits Wk 2 or later.
Results: 152 pts (88.8% male) were randomized at 42 sites; 100 to pegloticase+MTX, 52 to pegloticase+PBO. 4 MTX, 3 PBO pts discontinued before first pegloticase dose; 26 MTX, 30 PBO pts who received pegloticase discontinued treatment at or before Wk 24. The primary endpoint was met with a 6-month response rate of 71.0% (71/100) vs 38.5% (20/52) in the MTX vs PBO co-therapy groups (p<0.0001; modified ITT [all pts receiving ≥1 pegloticase dose]: 74.0% [71/96] vs 40.8% [20/49], p<0.0001). In the first 24 wks of therapy, 81.3% vs 95.9% experienced ≥1 AE (
Key efficacy and safety findings through Month 6 of treatment.
| Pegloticase+MTX | Pegloticase+PBO | |
|---|---|---|
| ITT population | N=100 | N=52 |
| Age, yrs, mean±SD | 55.6±12.7 | 53.0±12.1 |
| Tophi at baseline, % | 74.0% | 78.8% |
| sUA at baseline, mg/dL, mean±SD | 8.7±1.6 | 9.1±1.7 |
| 6-mo treatment responders (primary endpoint), % | 71.0% | 38.5% |
| Safety population | N=96 | N=49 |
| ≥1 Serious AE, % | 8.3% | 10.2% |
| ≥1 treatment-emergent AE, % | 81.3% | 95.9% |
| Gout flare* | 66.7% | 69.4% |
| IR*, anaphylaxis* | 3.1%, 1.0% | 30.6%, 0% |
| Cardiac event* | 1.0% | 0% |
| Infection/infestation † | 10.4% | 16.3% |
| Gastrointestinal † | 9.4% | 16.3% |
| Skin † | 7.3% | 12.2% |
| Respiratory/thoracic † | 5.2% | 4.1% |
| Blood/lymphatic † | 2.1% | 2.0% |
| Renal/urinary † , hepatobiliary † | 2.1%, 0% | 2.0%, 2.0% |
*AE of special interest, † known MTX AE
Conclusion: This RCT demonstrated significantly higher rate of sustained urate-lowering response over 6 months in pts co-treated with pegloticase+MTX vs pegloticase+PBO. No new safety concerns were seen through Month 6 and IR incidence was markedly lower in patients co-administered MTX vs PBO.
REFERENCES:
[1]Sundy JS, et al. JAMA 2011;306:711-20
[2]Lipsky PE, et al. Arthritis Res Ther 2014;16:R60
[3]Botson JK, et al. J Rheumatol 2021;48:767-74
[4]MTX package insert
Disclosure of Interests: John Botson Speakers bureau: Horizon Therapeutics, Consultant of: Horizon Therapeutics, Grant/research support from: Horizon Therapeutics, Kenneth Saag Grant/research support from: Horizon Therapeutics, Alinea, Lg, Sobi., Jeff Peterson Grant/research support from: Horizon Therapeutics, Naval Parikh Grant/research support from: Horizon Therapeutics, Stephen Ong Grant/research support from: Horizon, Novo Nordisk, Sanofi, Lilly, NIH/Mount Sinai, Dan La Speakers bureau: Abbvie, Grant/research support from: Horizon Therapeutics, Katie Obermeyer Shareholder of: Horizon Therapeutics, Employee of: Horizon Therapeutics, Brian LaMoreaux Shareholder of: Horizon Therapeutics, Employee of: Horizon Therapeutics, Stephen Sainati Shareholder of: Horizon Therapeutics, Employee of: Horizon Therapeutics, Suneet Grewal Speakers bureau: Horizon Therapeutics, UCB, Glaxo Smith Kline, Grant/research support from: Horizon Therapeutics, Amar Majjhoo Speakers bureau: Abbvie, Amgen, BMS, Horizon Therapeutics, Jansen, Glaxo Smith Kline, Astra Zeneca, Grant/research support from: Horizon Therapeutics, John Tesser Grant/research support from: Horizon Therapeutics, Michael E. Weinblatt Consultant of: Horizon Therapeutics