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. 2021 Apr 19;2021(4):CD011535. doi: 10.1002/14651858.CD011535.pub4

Heydendael 2003.

Study characteristics
Methods RCT, active‐controlled, open‐label trial
Date of study: October 1998‐June 2000
Location: multicentre (> 1) in Amsterdam/the Netherlands
Participants Randomised: 88 participants, mean age 40 years, 57 male
Inclusion criteria

  • Participants with moderate‐severe psoriasis, PASI>8,

  • Age ≥18

  • Non‐response to topical treatment

  • Non‐response to phototherapy

  • Number of allowed previous treatment line: 2


Exclusion criteria

  • Pregnancy, kidney insufficiency, liver insufficiency, high‐risk liver function abnormalities, hepatitis B

  • Had received methotrexate or ciclosporin

  • Had an active infection

  • Had uncontrolled diabetes (Insulin‐dependent)

  • Had uncontrolled cardiovascular disorder

  • Had uncontrolled hypertension

  • Had past history of malignant tumours


Dropouts and withdrawals

  • 3/88 (3.4%)

  • Methotrexate group (1): withdrew consent (1)

  • Ciclosporin group (2): ineligible (2)
Interventions Intervention
A. Methotrexate (n = 44), orally, 15 mg/week until 4 weeks then increase up to 22.5 mg if reduction from baseline PASI < 25%, 3 divided doses with 12‐h interval, 12 weeks
Control intervention
B. Ciclosporin (n = 44), orally, 3 mg/kg until 4 weeks then increase up to 5 mg/kg if reduction from baseline PASI < 25%, 2 divided doses, 12 weeks
Outcomes Assessments at weeks 16 weeks
Primary outcomes of the trial

  • PASI


Secondary outcomes of the trial

  • Side effects

  • SF36
Notes Funding sources, Quote (p 664): "Supported by a grant (OG 97‐009) from the Dutch Health Authorities"
Declarations of interest: not stated
Risk of bias
Bias Authors' judgement Support for judgement
Random sequence generation (selection bias) Low risk Quote (p 660): "Randomisation was performed centrally with the use of computer‐generated random numbers and block size of eight patients"
Comment: probably done
Allocation concealment (selection bias) Low risk Quote (p 660): "Randomisation was performed centrally with the use of computer‐generated random numbers and block size of eight patients"
Comment: probably done
Blinding of participants and personnel (performance bias)
All outcomes High risk Comment: no blinding
Blinding of outcome assessment (detection bias)
All outcomes Unclear risk Quote (p 660): "The score of the PASI ... was determined... by trained assessors who were unaware of the treatment assignment"
Comment: no description of method used to guarantee no communication between care givers or participants and assessors
Incomplete outcome data (attrition bias)
All outcomes Low risk 88 randomised, 85 analysed
Quote (pp 660‐1): "If a patient missed a visit, we used the score from the previous visit".
Comment: few lost to follow‐up, well‐balanced number and reasons between groups
Selective reporting (reporting bias) Unclear risk Comment: no protocol was available. The prespecified outcomes mentioned in the Methods section appeared to have been reported