Acute AT1-receptor blockade reverses the hemodynamic and baroreflex impairment in adult sheep exposed to antenatal betamethasone.

To accelerate lung development and protect neonates from other early developmental problems, synthetic steroids are administered maternally in the third trimester, exposing fetuses that are candidates for premature delivery to them. However, steroid exposure at this point of gestation may lead to elevated blood pressure [mean arterial pressure (MAP)] during adolescence. We hypothesize that fetal exposure to steroids activates the renin-angiotensin system, inducing an elevation in blood pressure and attenuation of baroreflex sensitivity (BRS) that is angiotensin It dependent in early adulthood. To test this hypothesis, fetal sheep were exposedto betamethasone (Beta) or vehicle (control) administered to ewes at day 80 of gestation and delivered at full term. At 1.8 yr of age, male offspring were instrumented for conscious recording of MAP, heart rate, and measurement of BRS [as lowfrequency-a, high-frequency-a, sequence (seq) UP, seq DOWN, and seq TOTAL]. Beta-exposed sheep (n = 6) had higher MAP than control sheep (n = 5) (93 ± 2 vs. 84 ± 2 mmHg, P < 0.01). Acute blockade of angiotensin type I receptors with candesartan (0.3 mg/kg iv) normalized MAP in Beta-exposed sheep (85 ± 4 mmHg), with no effect in control sheep (82 ± 3 mmHg). Before angiotensin type 1 blockade, BRS maximum gain was significantly lower in Betaexposed vs. control sheep (11 ± 3 vs. 26 ± 3 ms/mmHg, P < 0.0.01). However, 45 mm after candesartan injection, BRS was increased in Beta-exposed (21 ± 5 ms/mmHg) and control (35 ± 4 ms/mmHg) sheep. Heart rate variability (HRV) and blood pressure variability (BPV) revealed lower HRV (SD of beat-to-beat interval and root mean square of successive beat-to-beat differences in R-R interval duration) and higher BPV (SD of MAP, systolic arterial pressure in low-frequency range) in Beta-exposed sheep. Candesartan partially restored HRV in Beta-exposed sheep and fully corrected BPV. Thus, in utero exposure to synthetic glucocorticoids causes long-lasting programming of the cardiovascular system via renin-angiotensin system-dependent mechanisms. [ABSTRACT FROM AUTHOR]