Nitric oxide releasing aspirin protects the gastric mucosa against stress and promotes healing of stress-induced gastric mucosal damage: role of heat shock protein 70

Peter C Konturek; Thomas Brzozowski; Agata Ptak; Joanna Kania; Sławomir Kwiecień; Eckhart G Hahn; Stanisław J Konturek

doi:10.1159/000066762

Nitric oxide releasing aspirin protects the gastric mucosa against stress and promotes healing of stress-induced gastric mucosal damage: role of heat shock protein 70

Digestion. 2002;66(3):160-72. doi: 10.1159/000066762.

Authors

Peter C Konturek¹, Thomas Brzozowski, Agata Ptak, Joanna Kania, Sławomir Kwiecień, Eckhart G Hahn, Stanisław J Konturek

Affiliation

¹ First Department of Medicine I, University Erlangen-Nürnberg, Erlangen, Germany. pkonturek@aol.com

PMID: 12481162
DOI: 10.1159/000066762

Abstract

Background/aim: Nitric oxide (NO) releasing nonsteroidal anti-inflammatory drugs do not cause gastric mucosal damage, despite inhibition of the cyclooxygenase activity to a similar extent as conventional nonsteroidal anti-inflammatory drugs that induce such damage. We compared the effects of native aspirin (ASA) with those of NO-releasing ASA (NO-ASA) on the development and healing of acute gastric lesions induced by water immersion and restraint stress (WRS) and the mucosal expression of heat shock protein 70 (HSP70).

Methods: Wistar rats received: (1). vehicle; (2). ASA (40 mg/kg i.g), and (3). NO-ASA (2.5-40 mg/kg i.g.), followed 0.5 h later by 3.5 h of WRS with or without glyceryl trinitrate, the donor of NO, and carboxy-PTIO, a NO scavenger. Healing of WRS lesions was assessed 0-24 h after termination of WRS. Number of gastric lesions, gastric mucosal blood flow (GBF), malondialdehyde (MDA) content, and RT-PCR expression of HSP70 mRNA were determined.

Results: WRS caused typical bleeding erosions that were aggravated by aspirin and this was accompanied by a fall in the GBF and a significant rise in the mucosal MDA concentrations. In contrast, NO-ASA, which raised significantly the luminal content of NO(x), reduced number of WRS lesions and mucosal MDA levels while increasing significantly the GBF. These protective and hyperemic effects of NO-ASA against WRS lesions were mimicked by addition of glyceryl trinitrate to native ASA and significantly attenuated by carboxy-PTIO added to NO-ASA. HSP70 mRNA was significantly upregulated by WRS, and this was significantly attenuated by ASA, but not by NO-ASA. NO-ASA decreased significantly the MDA content and induced overexpression of HSP70 mRNA during healing of WRS lesions.

Conclusion: NO-ASA exhibits mucosal protective and healing effects against WRS-induced gastric lesions due to the release of NO, which induces gastric hyperemia, and the attenuation of lipid peroxidation and counteracts the inhibition of HSP70 expression induced by native ASA.

Publication types

Comparative Study

MeSH terms

Animals
Aspirin / analogs & derivatives*
Aspirin / pharmacology*
Gastric Mucosa / drug effects*
HSP70 Heat-Shock Proteins / biosynthesis
HSP70 Heat-Shock Proteins / physiology*
Lipid Peroxidation
RNA, Messenger / genetics
Rats
Rats, Wistar
Reverse Transcriptase Polymerase Chain Reaction
Stress, Physiological / physiopathology*

Substances

HSP70 Heat-Shock Proteins
RNA, Messenger
nitroxy-butyl-acetylsalicylic acid
Aspirin