Alcohol Exposure During Prenatal Or Early Postnatal Period May Result In
Insulin Resistance, Glucose Intolerance Later In Life
DECEMBER 3, 2003
(Bethesda, MD) – Perinatal factors (those occurring about five months before
birth and one month after) have been implicated in the development of Type 2
diabetes and other disorders. Although the association of adverse events
during pregnancy and glucose intolerance has been well documented, little is
known about the effects of certain events that occur only during the
postnatal period.
It is important to
understand such effects involving lactation because alcohol consumption
among nursing women is common and there is a popular belief that alcohol
(i.e., maternal ethanol (EtOH)) promotes lactation. Ingested EtOH is
secreted in the milk and therefore has the potential for exposing the
developing offspring to toxic effects of EtOH. A new study finds that
alcohol exposure during early development -- though not necessarily during
pregnancy -- may program the offspring for insulin resistance and glucose
intolerance later in life.
A New Study
The authors of the study, “Whole Body Insulin
Resistance in Rat Offspring of Mothers Consuming Alcohol During Pregnancy or
Lactation: Comparing Prenatal and Postnatal Exposure,” are Li Chen and B. L.
Grégoire Nyomba of the Department of Internal Medicine, University of
Manitoba, Winnipeg, Manitoba, CN. Their findings appear in the Journal of
Applied Physiology, “Articles in Press” section. The Journal is
one of 14 scientific journals published each month by the American
Physiological Society (APS).
Methodology
The research team followed the protocol outlined below:
Animals:
Timed-pregnant Sprague-Dawley rats were used (n=3-4/group) and randomly
divided into three weight-matched groups. Throughout pregnancy, one group
was given 2g/kg EtOH (36%) twice daily and the other groups were given the
same volume of water. Body weight and food intake were recorded daily. From
day 1 postpartum until weaning, one of the two groups that were not given
EtOH during gestation was given EtOH, while the other groups were given
water. Average litter size was 14 for each of the three groups. Male
offspring were culled to 4-5 per lactating dam and kept with their mothers
until weaning on day 21. Weaned offspring were housed and fed, and body
weight and food measurements were tracked.
Intravenous Glucose
Tolerance Test: At 16 weeks of age, offspring from each group underwent
a frequently sampled intravenous glucose tolerance test (IVGTT). The rats
were later killed and incremental areas under the glucose (AUG) and insulin
(AUI) curves were calculated. Acute insulin response to glucose (AIR) was
calculated as the area under the AUI for the first 8 min after the glucose
challenge. A glucose tolerance index (KG), representing the net glucose
elimination rate in response to both endogenous and exogenous insulin, was
calculated. Insulin sensitivity index (SI) was determined by modeling. The
products of SI with AIR were used as the disposition index (DI) to
represent insulin effect.
Tissue Triglycerides:
Tissue triglycerides were extracted and, later, triglycerides were
determined spectrophotometrically.
Other Assays: Plasma
glucose was measured. Plasma insulin was measured with a sensitive rat
radioimmunoassay kit. Plasma free fatty acids (FFA) were determined.
Statistics:
Differences between groups were evaluated by ANOVA with Dunnett’s multiple
comparison test. Insulin values were log-transformed before analysis and
values expressed as the mean ± SEM. P<0.05 were considered significant.
Results
The researchers noted the following:
·
Animal weight and food intake: All male offspring in
the control group and in the group exposed to EtOH during lactation had a
birth weight greater than 6.0 g. Among male offspring exposed to EtOH during
pregnancy, 12 had a birth weight smaller than 6.0g, whereas 9 were within
the control range.
The offspring exposed to EtOH during pregnancy
were further separated into two subgroups: small and normal weight at birth.
In the prenatal EtOH group, offspring that were small at birth had a catch
up growth after 4 weeks of age, at which time their growth rate became
indistinguishable from controls. This was also the time their food intake,
which was slightly reduced during the first 2 weeks post-weaning, increased
to controls levels. Surprisingly, however, offspring in the prenatal EtOH
group that had a normal birth weight had a slower growth rate by 11 weeks of
age, despite normal food intake. Offspring exposed to EtOH during lactation
had a growth curve that was comparable to controls.
·
Glucose Tolerance and Insulin Sensitivity: The glucose
curves were similar among the three EtOH groups, but showed higher glycemiae
compared with control rats, especially during the last 70 min. The AUG
curves were also similar among the EtOH groups and were significantly
greater in all three groups compared with controls.
Both groups of offspring that were exposed to
EtOH before birth had elevated AIR, with the greater value in the lighter
group compared with controls. AIR in offspring exposed to EtOH during
lactation was similar to controls. KG, SI, and DI were significantly
decreased in the three EtOH groups compared with controls. SG was not
different between groups. Pooled data showed a hyperbolic relationship
between AIR and SI.
·
FFA and Triglycerides: Because hypertriglyceridemia and
accumulation of triglycerides in nonadipose tissues have been associated
with insulin resistance, the researchers measured plasma FFA and
triglyceride as well as muscle and liver triglycerides. Plasma FFA levels
were similar between EtOH groups and controls. However, plasma, muscle, and
liver triglyceride levels were about twofold higher in EtOH rats that were
born small compared with controls. Surprisingly, plasma and tissue
triglyceride levels in the other two EtOH groups were comparable to
controls.
Conclusions
This study demonstrates that exposure to EtOH during
early development, albeit not necessarily during pregnancy, may program the
offspring to abnormal glucose homeostasis later in life. Further, EtOH
exposure during the prenatal or early postnatal period resulted in insulin
resistance and glucose intolerance later in life. The underlying mechanisms
are still unknown, however, and require further investigation.
-end-
Source: Journal of Applied Physiology,
“Articles in Press” section. The Journal is one of 14 scientific
journals published each month by the American Physiological Society (APS).
***
The American Physiological
Society (APS) was founded in 1887 to foster basic and applied science, much
of it relating to human health. The Bethesda, MD-based Society has more than
10,000 members and publishes 3,800 articles in its 14 peer-reviewed journals
every year.
Editor’s Note: A copy of the research article is
available in pdf format to the press. Members of the press are invited to
obtain a pdf copy of the study and to interview members of the research
team. To do so, please contact Donna Krupa at 703.527.7357 (direct dial),
703.967.2751 (cell) or djkrupa1@aol.com.
