Interactions between angiotensin II, aortic and sympathetic nerve during development of coarctation hypertension.

In the chronic phase of coarctation hypertension (CH) we have shown both marked depression of baroreceptor reflex control of heart rate (Michelini et al, Hypertension, 1992, 19: II159-II163) and normalization of the depressed reflex control even with the persistence of hypertension in losartan-treated animals (Santos et al, Am. J. Physiol, 1995, 269: H812-H818). In the present study we analyzed the effects of chronic AT1tors blockade on the both the afferent aortic nerve activity (AON, protocol I) and splanchnic sympathetic nerve activity (SSNA, protocol II) of CH and sham operated controls in two conditions: spontaneous activity (basal condition) and stimulated discharge during transient increases/decreases in arterial pressure. Male Wistar rats (180-300g aged 2-3 months) were chronically treated with vehicle (VEH=distilled water, 1ml/kg/day, po.) or losartan (LOS=10mg/kg/day, po.) during 8 days. Tail pressure was measured at the beginning and on the 4th day, before subdiaphragmatic aortic coarctation (CH) or sham surgery (SHAM). On day 7 the rats were instrumented with a catheter to record arterial pressure in conscious freely moving rats on day 8. Rats were then anesthetized to record AON or SSNA simultaneously with pressure during 10-15 min (basal or spontaneous activity) and during baroreceptor loading/unloading (infusion/withdrawal of blood or injections/infusions of phenylephrine and sodium nitroprusside iv.). Nerve activity was rectified and integrated and acquired simultaneously with pressure in a computer (Windaq DI-200, Ohio, USA). Losartan-treatment caused a significant decrease in tail pressure (104+-3 vs. 117+-3 mmHg in VEH groups). In both LOS- and VEH-treated groups, CH caused significant and similar increases in arterial pressure (mean of 29%) that was accompanied in the VEH groups by both significant increase in variability and depression of the AON/activity/pressure relationship (CHVEH=1,04+-0,11 vs. SHAMVEH=1,63+-0,14 %/cycle/mmHg, p<0,05, protocol I) and by potentiation of SSNA responses (CHVEH=-10,36+-1,05 vs. SHAMVEH=-5,81+-0,60 %/cycle/mmHg, p<0,05, protocol II). In the LOS-treated groups, establishment of CH was accompanied by smaller variability and marked improvement in AON gain: in the physiological range of pressure changes, depression of AON activity was significantly smaller (CHLOS=3,30+-0,33 vs. CHVEH=2,18+-0,37 %/cycle/mmHg, p<0,05, a recovery of 40% when compared to respective controls of ~5,01+-0,33 %/cycle/mmHg). CHLOS showed also normalization of SSNA responses: gain in the CHLOS=-6,58+-0,62 %/cycle/mmHg, that was not different from SHAMLOS and SHAMVEH groups. In addition chronic treatment with LOS caused partial correction of spontaneous AON activity but did not change spontaneous SSNA discharge. Both AON and SSNA responses observed in CHLOS occurred simultaneously but were independent from pressure reductions observed in these groups. The date suggested that Ang II, activated during development of hypertension, depresses the afferent signaling by aortic receptors and is factor responsible for the facilitation of SSNA during pressure changes. The date permits to discriminate between pressor and a modulatory effects of Ang II and indicates that after chronic AT1 receptors blockade hypertension persists, but there is a partial restoration of AON gain accompanied by normalization of the sympathetic response. (AU)