Systemic Sclerosis Clinical Trial
Official title:
A Double-Blind Placebo-Controlled Pilot Study of Safety and Tolerability of AIMSPRO in Established Diffuse Cutaneous Systemic Sclerosis
To study the safety and tolerability of a hyperimmune goat serum product (AIMSPRO) in the treatment of systemic sclerosis (SSc) through a period of 26 weeks of study participation. The secondary objective of the study is to assess the efficacy of AIMSPRO as a therapeutic agent for SSc using inter alia the SSc-HAQ questionnaire and the modified Rodnan skin score.
Systemic sclerosis (scleroderma, SSc) is a multisystemic disease clinically characterized by
fibrosis of the skin, joints, muscles and internal organs. Systemic sclerosis is a rare
disease, with an estimated incidence of 19 individuals per million population per year.
The pathogenesis of SSc remains incompletely understood although it seems likely that there
is an interplay between inflammatory, vascular and fibroblast dysfunction, leading
ultimately to the sustained activation of a population of fibroblasts that deposit increased
amounts of extracellular matrix in lesional tissues, including the skin and internal organs.
Impairment of the immune system is currently thought to play an important role. This is
based on the observation that in the early phases of SSc, mononuclear cells migrate to the
dermis and accumulate around small blood vessels, nerves and skin appendages. Furthermore,
there is a direct relation between the extent of cutaneous inflammation and the extent and
progression of fibrosis of the skin. Stimulated T-lymphocytes of patients with SSc produce
more tumor necrosis factor-α, interleukin-1 and -2 compared with healthy controls and the
serum concentrations of IL-2, IL-4, IL-6 and IL-8 and soluble IL-2 receptors are elevated.
The occurrence of autoantibodies, predominantly antitopoisomerase-1 (ATA) and anticentromere
antibodies (ACA), in approximately 90% of the patients, points to an alteration of the
humoral immune system.
Systemic sclerosis can be subdivided into diffuse and limited forms. Diffuse cutaneous SSc
(dcSSc) is characterised by skin involvement proximal to the elbows and knees, limited
cutaneous SSc (lcSSc) by skin involvement distal to these joints. In approximately 50% of
patients with dcSSc, ATA can be detected, and in approximately 50% of patients with lcSSc
ACAs are present. Other hallmark autoantibodies have also been identified in smaller
proportions of SSc patients including anti-RNA polymerase I/III and anti-fibrillarin
antibodies (5).
The course of SSc is variable. In some patients the disease remains confined to
sclerodactyly and Raynaud's phenomenon. In other patients there is a relentless progression
of internal organ fibrosis, ultimately leading to death. A recent study showed a cumulative
5-year survival rate of 63%. There are efforts to try to identify clinical and
investigational predictors of outcome in SSc. One study has identified three clinical
variables: raised ESR, proteinuria and impaired lung function indices which are associated
with poor outcome. In addition, the various hallmark autoantibodies occurring in SSc are
mutually exclusive and several studies in Europe and North America have demonstrated that
individuals carrying each of these autoantibodies are associated with different frequencies
of internal organ complications. This also allows patients who are at increased risk of
pulmonary, cardiac or renal complications to be identified.
At present, no treatment has been definitely shown to be effective in SSc. Because of its
presumed immunologic pathogenesis, modulation of the immune system has been the major goal
in therapeutic interventions in SSc. Several studies have reported effectiveness of immune
modulating drugs in the treatment of this disease, although these have mostly been in open,
uncontrolled trials. These drugs include azathioprine, cyclosporin, methotrexate and
cyclophosphamide. Amongst these, methotrexate and cyclophosphamide are currently the most
widely used. New, more specific immunological treatment modalities have been harnessed in
order to improve the treatment and prognosis of scleroderma patients.
In 2005, a patient with systemic sclerosis was treated with AIMSPRO on a compassionate basis
with a sustained improvement in mobility and, in particular, there was an improvement in
proximal muscle power and skin characteristics.
In this study, twenty patients will receive either AIMSPRO or placebo, 1.0ml subcutaneously,
twice weekly for 26 weeks. Standard outcome measures and novel biomarkers will be used to
investigate safety, efficacy and response to treatment.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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