Diabetes Mellitus, Type 1 Clinical Trial
Official title:
Pilot Study Using Oral Insulin at Early Age for Immune Efficacy in Primary Prevention of Type 1 Diabetes
Type 1 diabetes (T1D) results from an autoimmune destruction of the insulin-producing beta cells within the pancreatic islets of Langerhans. This process is identified by circulating islet autoantibodies to beta cell antigens, and is mediated by a lack of immunological self-tolerance. Self-tolerance is achieved by T cell exposure to antigen in the thymus or periphery in a manner that deletes autoreactive effector T cells or induces regulatory T cells. Immunological tolerance can be achieved by administration of antigen under appropriate conditions. Administration of oral insulin in islet autoantibody-negative children who are genetically predisposed for T1D offers the potential for inducing immunological tolerance to beta cells and thereby protect against the development of islet autoimmunity and T1D.
The purpose of the Pre-POINT-Early Study is to investigate and consolidate the finding from
the preceding Pre-POINT Study, namely safety and immune efficacy at a daily dose of 67.5 mg
oral insulin. Since younger children will be tested in Pre-POINT-Early, the 67.5 mg dose will
be reached by dose escalation starting at 7.5 mg for 3 months followed by exposure to 22.5 mg
for 3 months, and reaching the desired 67.5 mg dose, which is administered for 6 months in 22
children.
The active substance for oral application is human insulin, synthesized in a special
non-disease-producing laboratory strain of Escherichia coli bacteria that has been
genetically altered by the addition of the gene for human insulin production (Lilly
Pharmaceuticals, Indianapolis, Indiana, USA). The physical, chemical and pharmaceutical
properties of the human insulin have been well documented by the manufacturer. Oral Insulin
will be applied as a capsule containing 7.5; 22.5 and 67.5 mg of the active substance
together with filling substance cellulose. After oral administration insulin will be rapidly
degraded by gastric acids. Enteric delivery and systemic availability is therefore unlikely
and efficacy of active insulin is likely to be restricted to the oral mucosa.
In human studies oral insulin administration was safe and without adverse side effects at
doses between 2.5 and 7.5 mg per day. Additionally Bonifacio et al. have conducted and
completed the Pre-POINT study, the first primary autoantigen vaccination dose-finding study
in which children with high genetic risk for type 1 diabetes were administered insulin orally
daily. Oral insulin at all tested doses (2.5 mg; 7.5 mg; 22.5 mg and 67.5 mg) in Pre-POINT
was considered safe: None of the children who received study drug or placebo experienced
hypoglycaemic episodes after administration of medication, and no allergic reactions were
observed.
The Pre-POINT-Early intended doses for oral application are 7.5, 22.5 and 67.5 mg per day.
The aim of the study is to determine whether daily administration of oral insulin starting
with dose 7.5 mg (3 months), moving to dose 22.5 mg (3 months) and to the highest dose of
67.5 mg (6 months) insulin to young children aged 6 months to 2 years with high genetic risk
for T1DM induces immune responses to insulin and/or proinsulin with features of immune
regulation.
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