RAS plays an important role in the mechanism of gastric integrity and gastroprotection and the pathogenesis of stress, indomethacin and ischemia-reperfusion induced gastric damage [12–15]. It is well known that stress induces acute gastric mucosal lesions by complex psychological factors influencing individual vulnerability, stimulation of specific brain pathways regulating autonomic function, decreased blood flow to the mucosa, hypermotility, mast cell degranulation, leukocyte activation, and increased free radical generation resulting in increased lipid peroxidation [16, 17] (fig. 1). Cold-restraint stress is commonly used and a clinically relevant experimental model for acute gastric damage [18]. The cessation of gastric microcirculation within gastric mucosa and increased free radical formation could be the major explanation for hemorrhagic gastric lesions and erosions predisposing to ulcer formation [17]. The maintenance of gastric blood flow is important to protect the mucosa from endogenous and exogenous damage factors. This gastric blood flow is impaired due to Ang II and catecholamines that are activated during stress in both plasma and peripheral tissues including the stomach [11]. Ang II contributes to the pathogenesis of inflammation induced by various stressors such as cold stress and ischemia-reperfusion (I/R) resulting in acute lesions in the gastric mucosa of rodents [17, 19] (fig. 1). Ang II elicits a cellular response through several molecular signaling pathways, such as calcium mobilization, reactive oxygen metabolite generation, and activation of protein kinase and nuclear transcription factors including nuclear factor-κB (NFκB) [20]. On the other hand, this peptide might contribute to the mucosal defense mechanism via activation of the vascular tone in the arteries of resistance. However, Ang II was shown to not only regulate vascular tone in the arteries of resistance and in the brain tissue but also constricts the gastric vasculature through AT1 receptor stimulation [21]. In addition, Ang II was shown to generate an excessive amount of reactive oxygen species followed by cellular damage and inflammation and to cross-talk with other inflammatory second messengers such as nitric oxide (NO), and PGs through NFκB-dependent mechanism [22, 23].

The inhibition of Ang II AT1 receptors with peripheral and central receptor antagonists prevents the sympathoadrenal and hypothalamic-pituitary-adrenal response to isolation stress and protects the brain from injury by reducing the cerebral blood flow during a stroke [19, 24]. The question remains whether antagonism of the AT1 receptors could attenuate the incidence of cold stress-induced gastric lesions and whether AT1 receptor blockade could be of therapeutic usefulness in this stress-related disorder. To address this question, a widely used strain of spontaneously hypertensive rats (SHR) characterized by increased sympathoadrenal reactivity to stress was employed because of the well-known association between stress and cardiovascular disease [11]. In this study, the AT 1 antagonists exhibited the protection against stress-induced gastric lesions due to the suppression of the stress-induced hormonal axis and sympathoadrenal response, the attenuation of the vasoconstrictor effects of Ang II in the gastric microcirculation, thereby causing an inhibition of mucosal inflammation [11, 12].

During intense acute stress, such as immobilization, there is an initial m...