Graft vs Host Disease Clinical Trial
Official title:
Prospective, Phase II/III, Randomized Clinical Study to Compare BEGEDINA® Versus "Conventional Treatment" for Treating Steroid Resistant Acute Graft-versus Host Disease
The objectives of this study are to determine the efficacy and safety of BEGEDINA® in subjects with steroid resistant acute graft versus host disease (GvHD). GvHD is a rare and complex immunological disease occurring in some recipients of allogeneic hematopoietic stem cell transplants (HSCTs) and affecting principally the skin, liver and gastrointestinal (GI) tissues. The disease is life threatening and may be acute or chronic and the first choice treatment for patients with acute GvHD (Grade II or higher) is the immunosuppressive corticosteroid hormone methylprednisolone. However, some GvHD patients may be resistant to this treatment leading to disease progression and a high rate of morbidity and mortality, primarily from infections and/or multi-organ failure. There are currently no other satisfactory therapies. BEGEDINA® is a therapeutic monoclonal antibody that recognises and binds to CD26 on CD4+ T lymphocytes. BEGEDINA® reduces the activity of CD26 in these cells and inhibits the immune response leading to improvement in patients that have shown steroid resistance. This study is therefore aimed at demonstrating that BEGEDINA® is a safe and effective treatment for steroid-resistant GvHD patients where no other such treatments are currently available.
This is a prospective, phase II/III, randomized clinical study to compare the efficacy and
safety of BEGEDINA® (Begelomab) versus "conventional treatment" for treating
steroid-resistant acute graft versus host disease (GvHD). Despite prophylactic treatment,
GvHD still develops in up to 30% of allogeneic hemopoietic stem cell transplant (HSCT)
recipients. GvHD is a life-threatening and complex immunological disease that may be acute or
chronic. Acute GvHD affects mainly the skin, liver and gastrointestinal (GI) tissues with
long-term survival directly related to the severity of skin, liver and gut involvement. First
line treatment for patients with acute GvHD (Grade II or higher) is the immunosuppressive
corticosteroid methylprednisolone. Although effective in over 50% of patients, durable
responses are observed in only a third of patients and it also confers a risk of severe
infection. Steroid-resistant acute GvHD is associated with a high rate of morbidity and
mortality, primarily from infections and/or multi-organ failure. Despite this, there are no
authorized treatments for non-responders and GvHD remains largely an untreatable disease with
limited survival and thus a great unmet therapeutic need. BEGEDINA® (Begelomab) is a murine
immunoglobulin G (IgG) 2b monoclonal antibody against CD26 (dipeptidyl peptidase-4; DPP4) and
is produced by biotechnological means and is a new potential therapeutic approach. BEGEDINA®
has been shown to bind to CD26 which is present on a subset of CD4+ T helper lymphocytes
leading to down-regulation of CD26 signaling and inhibition of immune response and thus
therapeutic improvements. BEGEDINA has been investigated in two completed clinical studies: a
pilot study and a dose-finding study and so far showing promising efficacy, safety and
tolerability.
The primary objective for this study is therefore to determine the efficacy of BEGEDINA®
versus conventional therapy in steroid-resistant acute GvHD. To satisfy this objective, two
co primary hypothesis will be tested. The first is that the overall response rate consisting
of the Complete Responders and the Partial Responders (CR+PR) at Study Day 28 will be higher
in the BEGEDINA® treated subjects. The second is that the incidence of transplant-related
mortality (TRM) at 6 months will be reduced in those subjects treated with BEGEDINA® versus
those treated with conventional therapy. Additional secondary efficacy endpoints will also be
assessed as a measure of effectiveness. In addition, some pharmacokinetics assessments will
be performed. Adverse events (AEs) will be coded using MedDRA and the frequency, causality
and intensity of AEs will be compared to conventional therapies. Further safety analysis will
also include laboratory findings, vital signs, immunogenicity and other assessments. Finally,
some exploratory analysis will also be performed.
This will be a prospective, multicenter, randomized, open-label, phase II/III clinical study
in which subjects will be randomly assigned in a 1:1 ratio to receive BEGEDINA® treatment or
the best conventional treatment available in their territory as no second line therapy is
currently approved. It is planned to enroll 184 male or female adult subjects with an upper
age limit of 65 years with steroid-resistant acute GvHD. BEGEDINA® will be administered at a
dose of 2.7 mg/m2/day for 5 consecutive days from Study Day 1 through to Study Day 5, and on
Study Days 10, 14, 17, 21, 24, and 28. Thus, the expected duration for each subject will be
approximately 12 months. The final statistical analysis plan (SAP) will be finalized prior to
database lock. Baseline characteristics of the subject sample will be described using summary
statistics. All statistical tests will be conducted at a 2-sided significance level of 5%
unless specifically specified. Multiple Imputation methods will be used as the primary method
for accounting for missing data.
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