Title of article :
Evaluation of safety and clinical activity of multiple doses of the anti-CD80 monoclonal antibody, galiximab, in patients with moderate to severe plaque psoriasis
Author/Authors :
Gottlieb، نويسنده , , Alice B and Kang، نويسنده , , Sewon and Linden، نويسنده , , Kenneth G and Lebwohl، نويسنده , , Mark and Menter، نويسنده , , Alan and Abdulghani، نويسنده , , Ahsan A and Goldfarb، نويسنده , , Michael and Chieffo، نويسنده , , Nicole and Totoritis، نويسنده , , Mark C، نويسنده ,
Issue Information :
روزنامه با شماره پیاپی سال 2004
Pages :
10
From page :
28
To page :
37
Abstract :
Background: Reduction in lesional, activated T cells induces improvement in psoriatic plaques. Galiximab (IDEC-114), an IgG1 anti-CD80 antibody, binds to CD80, a costimulatory molecule involved in T-cell activation. Objective: A Phase I/II, multidose, multischedule, dose-finding study of galiximab to evaluate safety, pharmacokinetics, and clinical activity was conducted in 35 patients with moderate to severe plaque psoriasis. Methods: Seven cohorts of five patients received galiximab intravenously on three different schedules at different dose levels. Results: Adverse events (AEs) commonly occurred as mild and self-limiting. Improvements were observed in most cohorts without evidence of a dose response in Psoriasis Area and Severity Index (50% or greater reduction in PASI score in 40% of patients), Physicianʹs Global Psoriasis Assessment (PGA rating of Good or above in 57% of patients), and Psoriasis Severity Scale (PSS, baseline mean of 7.6 decreased by Study Day 127 to 5.0). An association was observed between reduction in CD3+ cell count in histologic studies and reduction in PASI score. No antibodies to galiximab were detected. Conclusion: Galiximab appears to be safe and well tolerated with preliminary evidence of clinical and histologic response.
Keywords :
psoriasis , PASI , Galiximab
Journal title :
Clinical Immunology
Serial Year :
2004
Journal title :
Clinical Immunology
Record number :
1850528
Link To Document :
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