J
Clin Invest 1998 May 15;101(10):2174-8
Glucocorticoid exposure in late gestation permanently programs rat hepatic
phosphoenolpyruvate carboxykinase and glucocorticoid receptor expression and
causes glucose intolerance in adult offspring.
Nyirenda MJ, Lindsay RS, Kenyon CJ, Burchell A, Seckl JR
Molecular Endocrinology Laboratory, Molecular Medicine Centre, University of
Edinburgh, Western General Hospital, Edinburgh EH4 2XU, United Kingdom. mn@srv0.med.ed.ac.uk
Low birth weight in humans is predictive of insulin resistance and diabetes in
adult life. The molecular mechanisms underlying this link are unknown but fetal
exposure to excess glucocorticoids has been implicated. The fetus is normally
protected from the higher maternal levels of glucocorticoids by feto-placental
11beta hydroxysteroid dehydrogenase type-2 (11beta-HSD2) which inactivates
glucocorticoids. We have shown previously that inhibiting 11beta-HSD2
throughout pregnancy in rats reduces birth weight and causes hyperglycemia in
the adult offspring. We now show that dexamethasone (a poor substrate for
11beta-HSD2) administered to pregnant rats selectively in the last week of
pregnancy reduces birth weight by 10% (P < 0.05), and produces adult fasting
hyperglycemia (treated 5.3+/-0.3; control 4.3+/-0.2mmol/ liter, P = 0.04),
reactive hyperglycemia (treated 8.7+/-0.4; control 7.5+/-0.2 mmol/liter, P =
0.03), and hyperinsulinemia (treated 6.1+/-0.4; control 3.8+/-0.5 ng/ml, P =
0.01) on oral glucose loading. In the adult offspring of rats exposed to dexamethasone
in late pregnancy, hepatic expression of glucocorticoid receptor (GR) mRNA and
phosphoenolpyruvate carboxykinase (PEPCK) mRNA (and activity) are increased by
25% (P = 0.01) and 60% (P < 0.01), respectively, while other liver enzymes
(glucose-6-phosphatase, glucokinase, and 11beta-hydroxysteroid dehydrogenase
type-1) are unaltered. In contrast dexamethasone, when given in the first or
second week of gestation, has no effect on offspring insulin/glucose responses
or hepatic PEPCK and GR expression. The increased hepatic GR expression may be crucial,
since rats exposed to dexamethasone in utero showed potentiated glucose
responses to exogenous corticosterone. These observations suggest that excessive
glucocorticoid exposure late in pregnancy predisposes the offspring to glucose
intolerance in adulthood. Programmed hepatic PEPCK overexpression, perhaps
mediated by increased GR, may promote this process by increasing
gluconeogenesis.
PMID: 9593773, UI: 98256357