Mechanisms Underlying Capsaicin-Stimulated  Secretion in the Stomach: Comparison with Mucosal Acidification

Aihara, Eitaro; Hayashi, Masamune; Sasaki, Yoko; Kobata, Atsushi; Takeuchi, Koji

doi:10.1124/jpet.105.087619

Cited by 27 publications

(36 citation statements)

References 41 publications

(62 reference statements)

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“…Indeed, we observed that the isolated stomach generated NO under basal conditions without any treatment and that the production was significantly reduced by the serosal addition of L-NAME. Consistent with our previous findings (Aihara et al, 2005a), we further observed in this study that NOR-3 stimulated HCO 3 Ϫ secretion in the stomach, partly mediated by endogenous PGs and through the activation of EP1 receptors. Thus, it is assumed that the inhibition of PDE1 and PDE5 first increases intracellular levels of cGMP and then stimulates gastric HCO 3 Ϫ secretion in two ways, directly via cGMP and indirectly mediated by PGE 2 /EP1 receptors.…”

Section: Discussionsupporting

confidence: 81%

“…Furukawa et al (1999Furukawa et al ( , 2000 showed that the secretion of HCO 3 Ϫ in isolated duodenum in vitro was stimulated by NOR-3, at least partly, via production of PGE 2 through activation of COX-1. We also showed that NOR-3 also increased PGE 2 production in the rat stomach, resulting in stimulation of HCO 3 Ϫ secretion (Aihara et al, 2005a). The levels of cGMP in the isolated mouse stomach were also significantly increased by NOR-3.…”

Section: Discussionmentioning

confidence: 53%

“…We previously reported that the acid-induced secretion of HCO 3 Ϫ in the stomach was inhibited by the prior administration of L-NAME, an inhibitor of NO production as well as indomethacin (Aihara et al, 2005a, suggesting the involvement of endogenous NO in the response, in addition to PGs. Indeed, HCO 3 Ϫ secretion was stimulated by the NO donor NOR-3 in the rat stomach and duodenum, and these actions were significantly attenuated by indomethacin (Sugamoto et al, 2001;Aihara et al, 2005bAihara et al, , 2006.…”

Section: Discussionmentioning

confidence: 99%

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Phosphodiesterase Isozymes Involved in Regulation of Secretion in Isolated Mouse Stomach in Vitro

Kita

Takahashi²,

Ohashi³

et al. 2008

J Pharmacol Exp Ther

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(Ϯ)-(E)-4-Ethyl-2-[(E)-hydroxyimino]-5-nitro-3-hexenamide](NOR-3), a nitric-oxide (NO) donor, is known to increase HCO 3 Ϫ secretion in rat stomachs, intracellularly mediated by cGMP; yet, there is no information about the phosphodiesterase (PDE) isozyme involved in this process. We examined the effects of various isozyme-selective PDE inhibitors on the secretion of HCO 3 Ϫ in the mouse stomach in vitro and the type(s) of PDE isozymes involved in the response to NO. The gastric mucosa of DDY mice was stripped of the muscle layer and mounted on an Ussing chamber. HCO 3 Ϫ secretion was measured at pH 7.0 using a pH-stat method and by adding 2 mM HCl. NOR-3, 8-bromoguanosine 3Ј,5Ј-cyclic monophosphate (8-Br-cGMP), and various PDE inhibitors were added to the serosal side. Vinpocetine (PDE1 inhibitor) or zaprinast (PDE5 inhibitor) was also added serosally 30 min before NOR-3 or 8-Br-cGMP. Both NOR-3 and 8-Br-cGMP stimulated HCO 3 Ϫ secretion in a dosedependent manner, and the response to NOR-3 was significantly inhibited by methylene blue. Likewise, the secretion induced by NOR-3 or 8-Br-cGMP was significantly attenuated by 6-((2S,3S)-3-(4-chloro-2-methylphenylsulfonylaminomethyl)-bicyclo(2.2.2)octan-2-yl)-5Z-hexenoic acid (ONO-8711), the PGE receptor (EP)1 antagonist, as well as indomethacin and potentiated by both vinpocetine and zaprinast at doses that had no effect by themselves on the basal secretion, whereas other subtype-selective PDE inhibitors had no effect. NOR-3 increased the mucosal PGE 2 content in a methylene blueinhibitable manner. These results suggest that NO stimulates gastric HCO 3 Ϫ secretion mediated intracellularly by cGMP and modified by both PDE1 and PDE5, and this response is finally mediated by endogenous PGE 2 via the activation of EP1 receptors.

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Section: Discussionsupporting

confidence: 81%

Section: Discussionmentioning

confidence: 53%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Phosphodiesterase Isozymes Involved in Regulation of Secretion in Isolated Mouse Stomach in Vitro

Kita

Takahashi²,

Ohashi³

et al. 2008

J Pharmacol Exp Ther

Self Cite

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“…O 2 − , superoxide; H 2 O 2 , hydrogen peroxide; ONOO, peroxynitrite; N2O 3 B2 receptor antagonists also exert a protective effect in the postischemic intestine (465). Bradykinin, PAF and LTB4 are involved in the early immediate recruitment of neutrophils and appear to mediate this effect largely through transcription-independent mechanisms (160,467).…”

Section: Consequences and Mechanisms Of Ischemic Injurymentioning

confidence: 97%

“…The submucosal arterioles branch into capillaries at the base of the glands and postcapillary vessels pass to the luminal surface of the mucosa where they form another capillary network surrounding the gastric pits (147). This seriescoupled arrangement allows for the HCO 3 − released from the parietal cell during H + secretion to be delivered to the basal side of the mucosal surface cells (Fig. 1).…”

Section: Salient Features Of the Mucosal Microcirculationmentioning

confidence: 98%

The Gastrointestinal Circulation: Physiology and Pathophysiology

Granger

Holm

Kvietys

2015

Comprehensive Physiology

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The gastrointestinal (GI) circulation receives a large fraction of cardiac output and this increases following ingestion of a meal. While blood flow regulation is not the intense phenomenon noted in other vascular beds, the combined responses of blood flow, and capillary oxygen exchange help ensure a level of tissue oxygenation that is commensurate with organ metabolism and function. This is evidenced in the vascular responses of the stomach to increased acid production and in intestine during periods of enhanced nutrient absorption. Complimenting the metabolic vasoregulation is a strong myogenic response that contributes to basal vascular tone and to the responses elicited by changes in intravascular pressure. The GI circulation also contributes to a mucosal defense mechanism that protects against excessive damage to the epithelial lining following ingestion of toxins and/or noxious agents. Profound reductions in GI blood flow are evidenced in certain physiological (strenuous exercise) and pathological (hemorrhage) conditions, while some disease states (e.g., chronic portal hypertension) are associated with a hyperdynamic circulation. The sacrificial nature of GI blood flow is essential for ensuring adequate perfusion of vital organs during periods of whole body stress. The restoration of blood flow (reperfusion) to GI organs following ischemia elicits an exaggerated tissue injury response that reflects the potential of this organ system to generate reactive oxygen species and to mount an inflammatory response. Human and animal studies of inflammatory bowel disease have also revealed a contribution of the vasculature to the initiation and perpetuation of the tissue inflammation and associated injury response.

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Mechanisms of gastroprotective effect of eugenol in indomethacin‐induced ulcer in rats

Morsy

Fouad

2008

Phytotherapy Research

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Possible mechanisms underlying the gastroprotective effect of eugenol against indomethacin-induced ulcer in rats were investigated. Pyloric ligation was performed for collection of gastric juice, and gastric ulceration was induced by a single intraperitoneal (i.p.) injection of indomethacin (30 mg/kg). Pretreatment with a single dose of eugenol (100 mg/kg, orally), 1 h before indomethacin administration caused significant reductions in gastric mucosal lesions, gastric acid outputs and pepsin activity associated with a significant increase in mucin concentration. Additionally, eugenol significantly attenuated the elevations in gastric mucosal malondialdehyde and total nitrite, and the decrease in reduced glutathione observed with indomethacin. The protective effect afforded by eugenol was significantly inhibited by prior administration of glibenclamide, the ATP-sensitive potassium (K(ATP)) channel blocker, but not by prior use of ruthenium red, the transient receptor potential vanilloid 1 (TRPV1) antagonist. The results indicate that the anti-ulcer effect of eugenol is mediated by opening of K(ATP) channels, scavenging free radicals, decreasing acid-pepsin secretion, increasing mucin production, and preventing the deleterious rise in nitric oxide level.

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Mechanisms Underlying Capsaicin-Stimulated Secretion in the Stomach: Comparison with Mucosal Acidification

Cited by 27 publications

References 41 publications

Phosphodiesterase Isozymes Involved in Regulation of Secretion in Isolated Mouse Stomach in Vitro

Phosphodiesterase Isozymes Involved in Regulation of Secretion in Isolated Mouse Stomach in Vitro

The Gastrointestinal Circulation: Physiology and Pathophysiology

Mechanisms of gastroprotective effect of eugenol in indomethacin‐induced ulcer in rats

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