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Item #15
Oral
Insulin Controls Postprandial Plasma Glucose
Oral
insulin was more effective than subcutaneous regular
insulin controlling postprandial glycemia.
The
objectives of this exploratory study were to assess the
postprandial glucose-lowering effects and evaluate the
safety and tolerability of single, escalating doses of an oral
insulin product, hexyl-insulin monoconjugate 2 (HIM2), in
patients with type 2 diabetes. Subcutaneous insulin and oral placebo
were also administered for comparison.
Eighteen
patients with type 2 diabetes were enrolled in this
randomized, single-blind, placebo-controlled, three-way
crossover, dose-escalation study. A single dose of each of
the following study drugs was administered to each patient on
3 separate days: oral HIM2 (at one of three dose levels: 0.375,
0.5, or 1.0 mg/kg), subcutaneous regular insulin (8 units Humulin
R), and oral placebo. At 30 min after dosing, patients ingested
a standardized test meal (16 oz/720 calories of Boost Plus).
Serial blood samples were collected for determination of
plasma glucose and insulin concentrations during the 4-h postdose
period.
The
mean glucose area under the curve for 0 to 240 min (AUC0–240)
values were lower following administration of 0.5 and 1.0
mg/kg HIM2 vs. placebo (1,097.1 vs. 1,196.9 and 801.1 vs.
992.1 mg · h-1 · dl-1, respectively). This
difference was statistically significant at the 1.0-mg/kg HIM2
dose level. Insulin exposure, as measured by insulin AUC0–240
values, for the 0.375-, 0.5-, and 1.0-mg/kg dose levels of HIM2
were 169.9, 193.1, and 230.8 µU · h-1 · ml-1,
respectively; insulin AUC0–240 values for placebo were
165.8, 196.1, and 169.2 µU · h-1 · ml-1,
respectively. The mean glucose AUC0–240 values were similar
following administration of 0.5 and 1.0 mg/kg HIM2 vs. subcutaneous
insulin (1,097.1 vs. 1,048.0 and 801.1 vs. 875.2 mg · h-1
· dl-1, respectively). For pooled data from the
0.5- and 1.0-mg/kg dose groups, the HIM2/subcutaneous insulin
ratios for the 2-h postprandial glucose concentration (0.97,
95% CI 0.90–1.06), maximum postprandial glucose concentration
(0.99, 95% CI 0.93–1.06), and glucose AUC0–240 (0.98,
95% CI 0.9–1.06) were within 10% of unity, implying glucodynamic
equivalence. Although HIM2 (0.5 and 1.0 mg/kg) and
subcutaneous insulin (8 units) provided comparable control of
postprandial plasma glucose concentrations, HIM2 resulted in
peripheral insulin concentrations that were lower than subcutaneous
insulin (mean insulin AUC0–240 of 193.1 vs. 233.6
and 230.8 vs. 270.3 µU · h-1 · ml-1,
respectively).
From
the results it was concluded that single, oral doses of HIM2 were safe
and well tolerated. HIM2 (0.5 and 1.0 mg/kg) was more
effective than placebo and as effective as subcutaneous
regular insulin (8 units) at controlling postprandial
glycemia with respect to the following parameters: 2-h
postprandial glucose concentration, maximum glucose
concentration, and glucose AUC0–240. This occurred
even though peripheral insulin concentrations were lower
following the administration of HIM2 (0.5 and 1.0 mg/kg) than
subcutaneous insulin. Thus, HIM2 therapy may control postprandial
glycemia without causing peripheral hyperinsulinemia in patients
with type 2 diabetes. Diabetes
Care; Feb 03
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