Type 1 Diabetes Mellitus Clinical Trial
Official title:
Effect of Linagliptin on Incretin Axis in Type 1 Diabetes
Type 1 diabetes is an autoimmune disorder characterized by beta cell destruction resulting in insulinopenia. Currently it is being treated with insulin. Dipeptidylpeptidase inhibitors (DPP4 inhibitors e.g. linagliptin & sitagliptin) has been used for type 2 diabetes mellitus (T2DM) traditionally. Previous studies has shown that it is also effective in type 1 diabetes mellitus (T1DM), but the mechanism of action not well understood. This study will evaluate possible mechanism of action of linagliptin in T1DM patients.
Glucose is the most important physiologic substance involved in the regulation of insulin
release. The effect of glucose on the beta cell is dose related. Dose-dependent increases in
concentrations of insulin and C-peptide and in rates of insulin secretion have been observed
after oral and intravenous glucose loads with 1.4 units of insulin, on average, being
secreted in response to an oral glucose load as small as 12 g. The insulin secretory
response is greater with oral compared to intravenous glucose administration. This
difference in insulin secretion is known as the incretin effect. This enhanced response to
oral glucose has been interpreted as an indication that absorption of glucose by way of the
gastrointestinal tract stimulates the release of hormones and other mechanisms that
ultimately enhance the sensitivity of the beta cell to glucose. The release of insulin from
the beta cell after a meal is facilitated by a number of gastrointestinal peptide hormones,
including GIP (Glucose dependent insulinotropic peptide), cholecystokinin, and GLP1
(Glucagon like peptide 1). These hormones are released from small-intestinal endocrine cells
postprandialy and travel in the bloodstream to reach the beta cells, where they act through
second messengers to increase the sensitivity of these islet cells to glucose. In general,
these hormones are not themselves secretagogues, and their effects are evident only in the
presence of hyperglycemia. This incretin effect could account for the greater beta-cell
response observed after oral as opposed to intravenous glucose administration.
GLP1, the most potent of the incretin peptides, lowers glucose in patients with T2DM by
stimulating endogenous insulin secretion and perhaps by inhibiting glucagon secretion and
gastric emptying. Treatment with supra physiologic doses of GIP during hyperglycemia has
been shown to augment insulin secretion in normal humans but not in individual with diabetes
mellitus. Although cholecystokinin has the ability to augment insulin secretion in humans,
it is not firmly established whether it is an incretin at physiologic levels. Its effects
are also seen largely at pharmacological doses.
Type 1 diabetes (T1DM) is characterized by autoimmune pancreatic β cell destruction and
insulin deficiency resulting in hyperglycemia. Insulin is the mainstay of treatment in T1DM.
There are few study which showed effectiveness of OHA (oral hypoglycemic agents) in T1DM.
Linagliptin is a dipeptidyl peptidase 4 (DPP4) inhibitor. It increases endogenous glucagon
like peptide 1 levels by inhibiting its rapid metabolism through the dipeptidyl peptidase 4
enzyme. It is currently Food and Drug Administration (FDA) approved for the treatment of
Type 2 diabetes (T2DM ) as mono therapy or in combination with insulin or other oral
hypoglycemic agents. Increasing endogenous glucagon like peptide 1 levels in patients with
T2DM has been shown to significantly improve postprandial glucose levels by both increasing
glucose-dependent insulin release and reducing glucagon levels.
Studies had shown that sitagliptin, a DPP4 inhibitor is effective in T1DM. But the mechanism
of action is unknown. In this study the investigators want to investigate the effect of
linagliptin, another DPP4 inhibitor on the glycaemic profile, HbA1C and glycaemic
variability in patients with T1DM. The investigators also will assess the GLP1 and glucagon
response during mixed meal test to identify the potential mechanism of this novel form of
therapy. These out come parameters will be compared with placebo treated T1DM patients.
During this study patients will be monitored for any adverse effect like nausea, vomiting,
pancreatitis. Serum urea, creatinin, amylase and lipase will be monitored monthly.
;
Allocation: Randomized, Endpoint Classification: Pharmacodynamics Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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