LÆKNABLAÐIÐ 1996; 82 231 al cortisol metabolism at physiological matern- al concentrations and inhibition of 1113- HSD with either the liquorice constituent glycyrr- hetinic acid or its hemi-succinate, carbenoxo- lone, resulted in abolition of the glucocorticoid barrier, allowing maternally administered cortisol to pass unmetabolised through the placenta. In a prospective study, on 16 normal primiparous women whose placentas were stu- died with this technique, a positive and signif- icant correlation was found between the ef- fectiveness of 116-HSD and offspring birth weight (r = 0.67; p < 0.005). The relationship between placental 116- HSD effectiveness in-vivo and term cord blood osteocalcin (a sensitive marker of glucocort- icoid exposure) was prospectively examined in 19 women. Cord blood levels of the bone specific protein osteocalcin were determined with radioimmunoassay. The lowest cord blood osteocalcin levels were found in the foetuses whose placental 116-HSD barrier function was poorest (r = 0.58; p < 0.02), (and had presumably had the greatest glucocort- icoid exposure), suggesting that term cord blood osteocalcin levels might be a useful predictor of hypertension, ischaemic heart dis- ease and possibly metabolic bone disease. The findings presented in this thesis repres- ent direct evidence that 116-HSD is the barrier to maternal glucocorticoids, its effectiveness correlating with foetal growth in rats (in-vitro), in humans (ex-vivo), and in-vivo with human cord blood osteocalcin levels (osteocalcin may be a marker of glucocorticoid exposure). In the light of studies on pregnant rats in which administration of exogenous glucocorticoids or 116-HSD inhibitors reduces birth weight and programmes hypertension in the offspring, it is reasonable to propose that increased foetal glucocorticoid exposure consequent upon att- enuated placental 116-HSD function may play a role in intrauterine programming of later hypertension.

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