WGET 2005.
Study characteristics | ||
Methods |
Study design: double‐blinded parallel RCT Location: USA: Michigan, San Francisco, Rochester, Maltimore, Durham, Cleveland, Boston, New York Setting: clinical centres Number of centres: 8 Time frame of the study: June 2000 through September 2003 Duration of follow‐up mean: 27 months |
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Participants |
Inclusion criteria:
Exclusion criteria:
Total number of participants: 181 participants randomised. Etanercept group: 89 Placebo group: 91 Characteristics:
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Interventions | All participants were followed for 12 months after randomization of the last participant. Etanercept group: 25 mg twice a week, subcutaneous; for 25 months (median value) Placebo group: lyophilised powder containing 40 mg of mannitol, 10 mg of sucrose, and 1,2 mg of tris(hydroxymethyl)methylamine twice a week, subcutaneous; for 19 months (median value) Concominant treatment for both groups: ‐ Patients with severe GPA received cyclophosphamide + glucocorticoids at the time of enrolment. Those with limited GPA receive methotrexate and glucocorticoids. After control of the patients’ disease, the standard medications are tapered according to regimens consistent with patient safety to reduce the risk of medication‐associated morbidity and to test the benefit of etanercept in sustaining disease remissions. ‐ All patients received prophylaxis against pneumocystis infection and osteoporosis. |
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Outcomes |
Major outcome:
Minor outcomes:
Other outcomes:
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Notes |
Discontinuation: 69 (38.12%) participants (34 participants from placebo group and 35 participant from etanercept group): 12 (6.63%) due to AEs, 4 (2.21%) died, 20 (11.94%) had treatment failure, 9 (4.97%) physician decision, 18 (9.94%) participant decision, 6 (3.31%) other reasons. Funded by:
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Risk of bias | ||
Bias | Authors' judgement | Support for judgement |
Random sequence generation (selection bias) | Low risk | "Treatment assignments are generated in permuted blocks of varying lengths." |
Allocation concealment (selection bias) | Low risk | Central allocation. "Patients are assigned to one of six experimental medication “bins”: A1, B2, C3, D4, E5, or F6" (information obtained from the author of the study) |
Blinding of participants and personnel (performance bias) All outcomes | Low risk | Participants receive medicinal dosage from the same bin. "The packaging of etanercept and placebo into identical vials". Blinding of study personnel ensured. "One potential source of unmasking among clinical personnel is the occurrence of injection site reactions. Injection site reactions have been reported in both the placebo‐ and etanercept‐assigned groups in other trials, albeit more commonly among etanercept‐assigned patients." |
Blinding of outcome assessment (detection bias) All outcomes | Low risk | "The board is masked to the specific treatment assignment of each group. In the evaluation of all data regarding the harm and benefit, the board receives data relating to treatment group (i.e., either etanercept or placebo) labelled as either treatment “A” or “B.” |
Incomplete outcome data (attrition bias) All outcomes | Low risk | ITT analysis, however 7% of patients in control group were excluded from primary analysis because lost to follow‐up and 0% were excluded in etanercept group. Including those patients would not have clinically relevant impact on the intervention effect estimate for major outcome |
Selective reporting (reporting bias) | High risk | One or more outcomes of interest in the review are reported incompletely so that they cannot be entered in a meta‐analysis. |
Other bias | Low risk | No other biases were identified. |
AE – adverse event
ANCA – antineutrophil cytoplasmic antibody
anti‐MPO – anti‐myeloperoxidase
anti‐PR3 – Anti‐proteinase 3 ‐
BMI – body mass index
BREVAS‐ Belimumab in Remission of VASculitis
BVAS – Birmingham Vasculitis Activity Score
BVAS/WG – Birmingham Vasculitis Activity Score for granulomatosis with polyangiitis
CrCl – creatinine clearance
EGPA – eosinophilic granulomatosis with polyangiitis
EudraCT ‐ European Union Drug Regulating Authorities Clinical Trials Database
EULAR – European League against Rheumatism
GPA – granulomatosis with polyangiitis
HBcAb – hepatitis B core antibody
HBsAg – hepatitis B Surface antigen
HIV ‐ human immunodeficiency virus
ITT – intention to treat
IV – intravenous
MPA – microscopic polyangiitis
NR – not reported
QTc(F) – QT interval corrected using Fridericia formula
RCT – randomized controlled trial
SC – subcutaneous
SD – standard deviation
VDI – Vasculitis Damage Index
WGET ‐ Wegener's Granulomatosis Etanercept Trial