Abstract—We determined whether genetic deficiency of angiotensin II Type 1A (AT_1A) receptors in mice results in altered neuronal responsiveness and reduced cardiovascular reactivity to stress. Telemetry devices were used to measure mean arterial pressure, heart rate, and activity. Before stress, lower resting mean arterial pressure was recorded in AT_1A^-/- (85±2 mm Hg) than in AT_1A^+/+ (112±2 mm Hg) mice; heart rate was not different between groups. Cage-switch stress for 90 minutes elevated blood pressure by +24±2 mm Hg in AT_1A^+/+ and +17±2 mm Hg in AT_1A^-/- mice (P<0.01), and heart rate increased by +203±9 bpm in AT_1A^+/+ and +121±9 bpm in AT_1A^-/- mice (P<0.001). Locomotor activation was less in AT_1A^-/- (3.0±0.4 U) than in AT_1A^+/+ animals (6.0±0.4 U), but differences in blood pressure and heart rate persisted during nonactive periods. In contrast to wild-type mice, spontaneous baroreflex sensitivity was not inhibited by stress in AT_1A^-/- mice. After cage-switch stress, c-Fos immunoreactivity was less in the paraventricular (P<0.001) and dorsomedial (P=0.001) nuclei of the hypothalamus and rostral ventrolateral medulla (P<0.001) in AT_1A^-/- compared with AT_1A^+/+ mice. Conversely, greater c-Fos immunoreactivity was observed in the medial nucleus of the amygdala, caudal ventrolateral medulla, and nucleus of the solitary tract (P<0.001) of AT_1A^-/- compared with AT_1A^+/+ mice. Greater activation of the amygdala suggests that AT_1A receptors normally inhibit the degree of stress-induced anxiety, whereas the lesser activation of the hypothalamus and rostral ventrolateral medulla suggests that AT_1A receptors play a key role in autonomic cardiovascular reactions to acute aversive stress, as well as for stress-induced inhibition of the baroreflex.