Inflammatory Bowel Diseases Clinical Trial
Official title:
Relevance of Valganciclovir in Recurrent Bouts of Cryptogenic Inflammatory Bowel Diseases With an Infection by Cytomegalovirus
The main objective of this study is to demonstrate the relevance of Valganciclovir on recurrent bouts of cryptogenic inflammatory bowel diseases with infection by cytomegalovirus (CMV). The goal is to obtain 90% (for Valganciclovir treated patients) versus 50% (for placebo treated patients) remission at 3 months (including the discontinuation of corticoids or reducing their dose to under 20 mg of prednisone equivalence), without any relapse over the 6 following months.
The cytomegalovirus (CMV) is a DNA virus from the herpes virus family. It is passed on
between humans and even if infection is widespread (50 to 80% of people older than 35 are
CMV immunoglobulin G positive) it is often asymptomatic for immunocompetent people. However,
for immunocompromised people, such an infection takes on particular frequency, expression
and seriousness, with a high frequency of attack to the digestive track (CMV colitis).
For immunocompetent people, colitis causes feverish bloody diarrhea associated with
abdominal pain. Colitis diagnosis is often late and cases with complications have been
reported (digestive bleeding, toxic giant colon and perforation). The endoscopic aspect of
colitis is not specific and diagnosis is based on serology, anatomopathology or
immunochemistry. Recently, PCR approaches have allowed more sensitive diagnosis.
CMV INVOLVEMENT IN CIBD PHYSIOPATHOLOGY:
Even though CMV involvement in colitis is rare but sure for immunocompetent people, its
involvement in CIBD triggering and morbidity has not been solved yet.
Some authors think infection by CMV may act on CIBD as a trigger factor; since 2 cases of
CMV colitis coinciding with the onset of a CIBD have been reported. For other authors,
infection by CMV acts by direct pathogenicity causing ulcerative lesions of colonic mucosa
and just imitates a CIBD without triggering it.
A third hypothesis is that infection by CMV aggravates inflammatory bowel diseases acting as
an exacerbating factor.
In all cases, people suffering from CIBD are highly-exposed to infection by CMV due to
immunosuppressive treatment (corticoids, cyclosporine, azathioprin, and methotrexate) and
the inflammation itself (which is supposed to be a proning factor).
CMV AND POUCHITIS:
Pouchitis is the most common long-term complication after total proctocolectomy. Usually, it
can be cured by antibiotic therapy, but in 15% of cases it becomes chronic and turns onto
refractory pouchitis which is difficult to cure.
Infection by CMV can imitate a chronic pouchitis from a clinical and endoscopic view. In
such cases, it had been shown that Valganciclovir treatment (10mg/kg/day) led to significant
improvement over a 21 day treatment period.
CONCLUSION:
Infection by CMV seems to play an important role and has to be taken into account in CIBD
physiopathogeny. Probably underestimated since it is not necessarily searched, it could be a
triggering factor or a treatment resistance factor. Immunosuppressive drugs used towards
recurrent bouts, in particularly cyclosporine, favors viral reactivation. Then, recurrent
bouts of CIBD may be complicated by CMV infection. That is why it could be interesting to
establish relevance of antiviral treatment on recurrent bouts of CIBD with infection by CMV.
The main objective of this study is to demonstrate relevance of Valganciclovir on recurrent
bouts of Cryptogenic Inflammatory Bowel Diseases with infection by Cytomegalovirus. The goal
is to obtain 90% (for Valganciclovir treated patients) versus 50% (for placebo treated
patients) of remission at 3 months (including the discontinuation of corticoids or reducing
their dose to under 20 mg of prednisone equivalence), without any relapse over the 6
following months.
Secondary objectives are:
- Reversal of CMV immunoglobulin G serology and PCR results on colonic biopsies.
- Improvement in appearance of histological lesions
- Reduction in the number of colectomies
- Evaluation of Valganciclovir tolerance and its side effects
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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