Triple Therapy Better Than Insulin Alone
for Type 2 Diabetics
Combining rosiglitazone, metformin, and
insulin aspart improved glucose metabolism in
obese type 2 diabetic patients compared with
mixed insulin alone.
That, according to the results of a
open-label, randomized trial published in the
December issue of Diabetes Care.
"Type 2 diabetes is caused by reduced
insulin secretion and insulin resistance in
skeletal muscle and liver," write Mikael
Kjær Poulsen, MD, from Odense University
Hospital in Denmark, and colleagues.
"There has been a tradition for many
years to use only one antidiabetic drug at a
time, and most patients are still treated with
either insulin secretagogues or insulin alone.
However, these drugs have only a minor effect
on cardiovascular events and mortality,
whereas metformin, which improves insulin
sensitivity, is able to reduce the risk of
myocardial infarction and reduce the mortality
rate."
For six months, 16 obese type 2 diabetic
outpatients receiving human NPH or MIX
(regular + NPH) insulin twice daily either
received triple therapy or continued their NPH
or MIX insulin twice daily. Triple therapy
consisted of insulin aspart, a rapid-acting
insulin analog, at meals; metformin, which
improves hepatic insulin sensitivity; and
rosiglitazone, which improves peripheral
insulin sensitivity. Algorithms directed
adjustment of insulin doses in both groups.
In the triple therapy group, mean HbA1c
decreased from 8.8% to 6.8% (P <
.01) without occurrence of severe hypoglycemic
events, and insulin sensitivity improved in
both skeletal muscle and liver. Postprandial
hyperglycemia was infrequent. The diurnal
profile of serum insulin was characterized by
fast and high peaks without the need to
increase insulin dose. Triple therapy was not
associated with significant weight gain or
impairment in plasma lipids, blood pressure,
or safety parameters other than hemoglobin.
Although the insulin dose was increased by
50% in the control group, there was no change
in HbA1c levels, 24-hour blood
glucose levels, or insulin sensitivity.
"These results strongly indicate that
normalization of the three major
pathophysiological defects of type 2 diabetic
subjects, namely peripheral insulin
resistance, hepatic insulin resistance, and
reduced insulin response following meals, can
significantly improve glucose
metabolism," the authors write.
"Triple therapy seems a promising
treatment for hyperglycemia in type 2 diabetic
subjects, but long-term studies are necessary.
However, if these results are confirmed,
diabetes complications may be dramatically
reduced."
Novo Nordisk provided insulin aspart,
GlaxoSmithKline provided rosiglitazone, and
Merck provided metformin. Novo Nordisk and
GlaxoSmithKline provided honoraria for
speaking engagements to three of the study
authors. The Clinical Institute, University of
Southern Denmark; Bernard Rasmussen and wife
Meta Rasmussen's foundation, Overlægerodets
Legatudvalg; Den Almindelige Danske
Lægeforening's science foundation; Novo
Nordisk, Denmark; and GlaxoSmithKline,
Denmark, supported this study. Diabetes
Care. 2003;26:3273-3279
Did
you know: Avandia
is Good for the Skin.
The onset
of foot ulcers in people with diabetes is
often attributed to diminished blood flow and
insufficient nitric oxide in the skin. In a
recent study, they followed 10 individuals
with type 2 diabetes who took 8mg of Avandia
per day. The researchers conclude that the
drug increased nitric oxide production by
about 33 percent, essentially improving blood
flow and the ability of skin to withstand
injury. Jour. Diabetes Complications Sept-Oct
2003
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