Articles www.thelancet.com Vol 371 April 19, 2008 1337 Eﬃcacy of ISA247 in plaque psoriasis: a randomised, multicentre, double-blind, placebo-controlled phase III study K Papp, R Bissonnette, L Rosoph, N Wasel, C W Lynde, G Searles, N H Shear, R B Huizinga, W P Maksymowych Summary Background The use of systemic calcineurin inhibitors for the treatment of patients with psoriasis is limited by toxicity, particularly nephrotoxicity. ISA247, a novel inhibitor, was eﬀective and well tolerated in a phase II study of patients with plaque psoriasis. Therefore its eﬃcacy was assessed in this phase III study. Methods 451 patients aged 18–65 years with plaque psoriasis involving at least 10% of the body surface area were randomly assigned in equal proportions to receive placebo or ISA247 at 0·2 mg/kg, 0·3 mg/kg, or 0·4 mg/kg orally twice a day in dermatology clinics. The primary endpoint was a 75% reduction in the psoriasis area and severity index (PASI 75) score at week 12. Treatment allocation was concealed from patient and physicians doing the assessments by use of sealed envelopes. The method of analysis was by modiﬁed intention to treat. The trial is registered at ClinicalTrials.gov, number NCT00244842. Findings 107, 113, and 116 patients were assigned to the ISA247 0·2 mg/kg, 0·3 mg/kg, and 0·4 mg/kg groups, respectively, and 115 to the placebo group. At week 12, PASI 75 scores were achieved in the ISA247 0·2 mg/kg, 0·3 mg/kg, and 0·4 mg/kg groups by 14 (16%; 95% CI 9–24) of 105, 26 (25%; 17–24) of 111, and 44 (47%; 27–57) of 113 patients, respectively, and in the placebo group by 4 (4%; 0–8) of 113 patients. Eﬃcacy was maintained during 24 weeks. Mild to moderate glomerular ﬁltration rate reductions were noted in seven patients in the ISA247 0·4 mg/kg group and in one in the ISA247 0·3 mg/kg group. ISA247 blood concentrations showed a strong correlation with mean percentage reduction in PASI. Interpretation ISA247 was safe and eﬀective in the treatment of patients with moderate to severe psoriasis during 24 weeks, with the highest dose providing the best eﬃcacy. The strong correlation between ISA247 concentrations and eﬃcacy might allow for accurate dosing of patients compared with existing calcineurin inhibitors. Funding Isotechnika. Introduction One of the most eﬀective treatments for psoriasis is the calcineurin inhibitor ciclosporin. 1–3 However, the side- eﬀect proﬁle of ciclosporin, in particular nephrotoxicity, restricts its long-term use. 4–7 Studies have shown that new biological treatments, in particular inﬂiximab, 8,9 are safe and eﬀective for treatment of plaque psoriasis. However, with their high cost, inconvenience of administration, and few data on long-term safety and eﬀectiveness, their widespread use might not be possible. 10 ISA247 (Isotechnika, Edmonton, AB, Canada) is a novel calcineurin inhibitor intended for the treatment of autoimmune diseases, such as psoriasis and uveitis, and prevention of organ transplant rejection. It diﬀers from ciclosporin by a chemical modiﬁcation of the functional group at the aminoacid-1 residue (ﬁgure 1). This modiﬁcation has improved the molecule in two ways. First, ISA247 binds more tightly to calcineurin than does ciclosporin, leading to a more complete inhibition of calcineurin. Second, the metabolism of ISA247 has been shifted away from aminoacid-1, which is the major site of metabolism for ciclosporin. This shift leads to a faster elimination of metabolites and a lower drug and metabolite load after the administration of ISA247 than with ciclosporin. In turn, fewer metabolites lead to improved pharmacokinetic and pharmacodynamic predictability. In animal models, ISA247 was more potent and had a more favourable side-eﬀect proﬁle than ciclosporin, particularly with regards to renal toxicity. 11–13 Consistent with these preclinical data, results of a phase II study of patients with stable plaque psoriasis showed that ISA247 was eﬀective and well tolerated, without much change in blood pressure or concentrations of lipids or triglycerides. 14 Therefore the eﬃcacy of a commercial preparation of ISA247 was assessed in this phase III clinical trial. Methods Patients Male and female patients aged 18–65 years with stable chronic plaque psoriasis involving at least 10% of the body surface area (BSA) for at least 6 months before screening were enrolled. These patients had a psoriasis area and severity index (PASI) score of 10 or more, a glomerular ﬁltration rate (GFR) greater than 60 mL/min, and less than 30% change in the GFR between screening and randomisation. Use of nephrotoxic medications or medications known to interact with ciclosporin or ISA247 was not allowed. Patients with erythrodermic, guttate, or pustular psoriasis, or other dermatoses that would Lancet 2008; 371: 1337–42 See Comment page 1311 Probity Medical Research, Waterloo, ON, Canada (K Papp MD); Innovaderm Research, Montreal, QC, Canada (R Bissonnette MD); North Bay Dermatology Clinic, North Bay, ON, Canada (L Rosoph MD); Stratica Medical, Edmonton, AB, Canada (N Wasel MD); Lynderm Research, Markham, ON, Canada (C W Lynde MD); Western Canada Dermatology Institute, Edmonton, AB, Canada (G Searles MD); Sunnybrook Dermatology, Toronto, ON, Canada (Prof N H Shear MD); Isotechnika, Edmonton, AB, Canada (R B Huizinga MSc); and University of Alberta, Edmonton, AB, Canada (Prof W P Maksymowych MD) Correspondence to: Kim Papp, 135 Union Street East, Waterloo, ON, Canada N2J 1C4 kapapp@probitymedical.com