ABSTRACT. The surfactant system and the antioxidant enzyme system of the fetal lung have chronologically similar developmental patterns and both can be accelerated by the administration of exogenous glucocorticoids. To test whether the antioxidant enzyme system, like the surfactant system, is regulated, at least in part, by endogenous glucocorticoids, we injected pregnant rats for 3 days prior to delivery with me&rapone, an adrenal 11-/3 hydroxylase inhibitor which crosses the ~lacenta and blocks endogenous glucocorticoid synthesis, o; saline. Metyrapone ofispring had significantly decreased lung tissue disaturated phosphatidylcholine and disaturatedphosphatidylcholine/total phospholipids ( p < 0.05) compared to controls at days 21 and 22 of gestation. Activities of the antioxidant enzymes superoxide dismutase, catalase, and glutathione peroxidase were similarly significantly reduced ( p < 0.01) in the lungs of metyrapone offspring at both gestational days studied. One day premature metyrapone pups demonstrated poorer survival than control pups from 25 min after delivery (44% survival versus 83%, p < 0.05) to 90 min (6% survival versus 78%, p < 0.01). These findings of delayed maturation of the surfactant and antioxidant enzyme systems following adrenal glucocorticoid blockade suggest that both systems are regulated, at least in part, by an endogenous glucocorticoid mechanism. (Pediatr Res 20: 672-675, 1986) Abbreviations DSPC, disaturated phosphatidylcholine TPL, total phospholipids AOE, antioxidant enzymes SOD, superoxide dismutase CAT, catalase GP, glutathione peroxidaseThe developmental patterns of the surfactant system and the antioxidant enzyme system of the fetal lung are chronologically similar, with both systems demonstrating marked increases during the final 10-15% of gestation in the several species studied (1-3). Both systems are important in the neonatal adaptation to independent respiration in the relatively oxygen-rich ex utero Received December 16, 1985; accepted March 11, 1986. Address all correspondence to Ilene R. environment. While the surfactant system provides reduction in alveolar surface tension and prevents alveolar collapse at end expiration, the antioxidant enzyme system of the lung prevents cell injury from reactive species of oxygen which are produced under normoxic and hyperoxic conditions (4-6). Multiple lines of evidence indicate that surfactant development is regulated, in part, by endogenous glucocorticoids: elevation of plasma glucocorticoid levels prior to the increase in surfactant (7), the presence of and increase in glucocorticoid receptors in fetal lung prior to elevation in surfactant (8-lo), and delays in surfactant maturation following interference with glucocorticoid production either biochemically (i.e. with metyrapone) or surgically (i.e. by fetal decapitation or hypophysectomy) (1 1-15).It has recently been demonstrated that the maturation of the pulmonary AOE, namely superoxide dismutase, catalase, and glutathione peroxidase, as well as surfactant (as measured ...
