A new derivative of acetylsalicylic acid and carnosine: synthesis, physical and chemical properties, biological activity.
Autor: | Kulikova, Olga I., Stvolinsky, Sergey L., Migulin, Vasily A., Andreeva, Ludmila A., Nagaev, Igor Yu., Lopacheva, Olga M., Kulichenkova, Ksenia N., Lopachev, Alexander V., Trubitsina, Irina E., Fedorova, Tatiana N. |
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Předmět: |
ERYTHROCYTES
ANIMAL experimentation ANTIOXIDANTS ASPIRIN BIOCHEMISTRY CHEMILUMINESCENCE assay CHRONIC diseases DOSAGE forms of drugs PHENOMENOLOGY MOLECULAR structure NATURAL immunity NEUROPEPTIDES PEPTIC ulcer RATS SPECTROPHOTOMETRY SYNTHETIC drugs OXIDATIVE stress PLATELET aggregation inhibitors INVESTIGATIONAL drugs PHARMACODYNAMICS |
Zdroj: | DARU: Journal of Pharmaceutical Sciences; 1/4/2020, Vol. 28, p119-130, 12p |
Abstrakt: | Purpose: The aim of this study was to create and assess biological activity of a new compound based on carnosine and acetylsalicylic acid (ASA) that will comprise antioxidant effect with antiplatelet activity, while simultaneously preventing side effects on the gastrointestinal tract. Methods: Salicyl-carnosine (SC) was synthesized by condensation of ASA and carnosine. Antioxidant activity was determined by spectrophotometric and chemiluminescence methods. Antiplatelet activity was carried out by the light transmission-aggregometry method using the inductor ADP. Chronic gastric ulcer in rats was modeled using glacial acetic acid. Results: Using SOD-like activity, iron-induced chemiluminescence, BaSO4-activated respiratory burst, and evaluation of red blood cell structure stabilization during oxidative damage induced by sodium hypochlorite, it was shown that SC possesses antioxidant activity analogous, or better, than that of carnosine. Antiplatelet activity of SC was evaluated in the blood of healthy individuals, and was also shown to be comparable to, or exceeding that of ASA. Also SC demonstrates high resistance to hydrolysis by tissue and serum carnosinases. Most importantly, it was shown that SC has protected the gastric mucosa against the formation of stomach ulcerative lesions and promoted their epithelization, therefore overcoming the undesirable inherent side effects of ASA. Conclusions: SC preserves pharmacologically significant properties of ASA and carnosine while retaining an anti-ulcer activity and resistance to the carnosinase hydrolysis at the same time. These properties are particularly promising for the potential development of new anti-inflammatory and antithrombotic drugs. [ABSTRACT FROM AUTHOR] |
Databáze: | Complementary Index |
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