Clinical Trial: Direct Antiviral Agents for Hepatitis C Virus-associated Cryoglobulinaemia Vasculitis

Study Status: Recruiting
Recruit Status: Recruiting
Study Type: Observational

Official Title: Direct Antiviral Agents for Hepatitis C Virus-associated Cryoglobulinaemia Vasculitis

Brief Summary: Cryoglobulinemia are responsible for systemic vasculitis, and the most frequently targeted organs are the skin, joints, kidney and peripheral nervous system. Cryoglobulinemia vasculitides are associated with significant morbidity and mortality, and require therapeutic intervention. With the discovery of hepatitis C virus (HCV) as the etiologic agent for most cases of mixed cryoglobulinemia new opportunities and problems for crafting therapy of HCV mixed cryoglobulinemia (MC) have emerged. A new and major concern was the potential adverse effects that immunosuppressive therapy with glucocorticoids and cytotoxic drugs could have on an underlying chronic viral infection. Alternatively the discovery of HCV provided the opportunity to control HCV-MC with antiviral therapy based on the belief that the underlying infection was driving immune complex formation and resultant vasculitis. Inducing a sustained virologic and clinical response and minimizing the use of immunosuppressive drugs are the main goals in the treatment of patients with HCV-MC vasculitis. Aggressive antiviral therapy has been shown to induce a complete remission of HCV-MC in up to 70% of patients. New antiviral combination, Interferon (IFN)-free regimens have recently proved very high virological response rate and with a very good safety profile and now need to be evaluated in severe and/or refractory HCV-MC patient's population.

Detailed Summary:
Sponsor: Assistance Publique - Hôpitaux de Paris

Current Primary Outcome: Number of participants with complete clinical response of cryoglobulinaemia vasculitis [ Time Frame: At week 24 ]

The complete clinical response is defined by improvement of all the affected organs involved at baseline and the absence of clinical relapse. The skin and articular improvement will be evaluated clinically (i.e. disappearance of purpura and/or ulcers and/or skin necrosis, disappearance of arthralgia and/or arthritis). Renal improvement will be evaluated biologically (i.e. proteinuria <0.3g/24h, disappearance of hematuria and improvement of Glomerular filtration rate (GFR) > 20% at week 24 if GFR < 60 ml/min/1.73 m² at diagnosis). Peripheral neurological improvement will be evaluated clinically (i.e. improvement of pains and paraesthesia by visual analogue scales, improvement of muscular testing in case of motor impairment at baseline) and/or electrophysiologically (i.e. improvement of electromyogram abnormalities at week 24 compared to baseline). The neuropathy total symptom score-6 (NTSS-6) will be applied to evaluate individual neuropathy sensory symptoms.


Original Primary Outcome: Same as current

Current Secondary Outcome:

  • Number of participants with sustained virological response [ Time Frame: At week 36 ]
    A sustained virological response is defined by the absence of detectable serum HCV RNA twelve weeks after the end of antiviral therapy
  • Number of participants with Immunological complete response [ Time Frame: At week 36 ]
    Immunological complete response is defined by negativation of cryoglobulin at week 36.
  • rate of side effects [ Time Frame: up to week 24 ]


Original Secondary Outcome: Same as current

Information By: Assistance Publique - Hôpitaux de Paris

Dates:
Date Received: July 19, 2016
Date Started: November 2013
Date Completion:
Last Updated: September 28, 2016
Last Verified: July 2016