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Diabetes Care, Vol 21, Issue 5 701-705, Copyright © 1998 by American Diabetes Association
The effects of metformin on glycemic control and serum lipids in insulin-treated NIDDM patients with suboptimal metabolic control
AC Robinson, J Burke, S Robinson, DG Johnston and RS Elkeles
Unit of Metabolic Medicine, Imperial College of Medicine at St. Mary's, London, U.K. a.c.robinson@sm.ic.ac.uk
OBJECTIVE: To test the hypothesis that metformin therapy, given as an
adjunct to insulin therapy, improves metabolic control in insulin-treated
NIDDM patients with suboptimal glycemic control. RESEARCH DESIGN AND
METHODS: A total of 33 subjects with insulin-treated NIDDM were
investigated; all had commenced insulin after secondary failure of
antihyperglycemic agents. Two randomized double-blind placebo-controlled
crossover studies were run. In study 1 (n = 19), insulin-treated subjects
with suboptimal glycemic control received 12 weeks of metformin 1 g b.i.d.
and 12 weeks of placebo. In study 2 (n = 14), subjects already established
on adjunctive metformin/insulin therapy stopped the metformin component and
received 12 weeks of metformin at their baseline dosage (range 1-2.5 g) and
12 weeks of equivalent placebo. Fasting plasma glucose, HbA1c, and serum
lipids were measured at baseline and midway through and at the end of each
treatment phase. The effect of 12 weeks of metformin treatment was compared
with the effect of 12 weeks of placebo in each study and in both studies
combined. RESULTS: In study 1, metformin treatment was associated with
significant improvements in fasting plasma glucose (mean 12-week difference
from placebo [95% CI]: 5.8 mmol/l [3.5-8.1], P < 0.001) and HbA1c (1.6%
[0.9-2.4], P < 0.001). In study 2, metformin treatment was associated
with significantly lower fasting plasma glucose (5.3 mmol/l [0.6-9.9], P =
0.029) and lower HbA1c (2.4% [1.0-3.8], P = 0.003) compared with those for
placebo. Study 2 also showed metformin treatment to be associated with
significantly lower total cholesterol than that for placebo (1.0 mmol/l
[0.1-1.9], P = 0.032) and lower LDL cholesterol (1.0 mmol/l [0.1-1.9], P =
0.028). This significant difference in serum lipids seen in study 2 was not
seen in study 1, but was present when both sets of data were combined (n =
33, mean total cholesterol difference at 12 weeks [95% CI]: 0.6 mmol/l
[0.1-1.1], P = 0.015). Metformin had no significant effect on triglyceride,
HDL cholesterol, weight, or blood pressure. Two subjects on metformin
withdrew because of side effects. CONCLUSIONS: Metformin, when given as
adjunctive therapy, was well tolerated and improved glycemic control and
lipid concentrations in patients with insulin-treated NIDDM whose diabetes
was poorly controlled. These improvements could be maintained over the long
term.

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Copyright © 1998 by the American Diabetes Association.
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