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Cardiovascular effects of Matricaria chamomilla extract: calcium channel modulation and vasorelaxant activity

Omonturdiev SirojiddinInstitute of Bioorganic Chemistry named after A.Sadykov, Laboratory of Plant Cytoprotectors, Mirzo Ulugbek, 83, Tashkent, UzbekistanAbdullaev IzzatulloInstitute of Bioorganic Chemistry named after A.Sadykov, Laboratory of Plant Cytoprotectors, Mirzo Ulugbek, 83, Tashkent, UzbekistanGayibov UlugbekInstitute of Bioorganic Chemistry named after A.Sadykov, Laboratory of Plant Cytoprotectors, Mirzo Ulugbek, 83, Tashkent, UzbekistanInomjonov DolimjonNamangan State University, Namangan, UzbekistanGayibova SabinaInstitute of Bioorganic Chemistry named after A.Sadykov, Laboratory of Plant Cytoprotectors, Mirzo Ulugbek, 83, Tashkent, UzbekistanMakhmudov RustamjonInstitute of Bioorganic Chemistry named after A.Sadykov, Laboratory of Plant Cytoprotectors, Mirzo Ulugbek, 83, Tashkent, UzbekistanAripov TakhirInstitute of Bioorganic Chemistry named after A.Sadykov, Laboratory of Plant Cytoprotectors, Mirzo Ulugbek, 83, Tashkent, UzbekistanEMİNE İNCİLAY TORUNOĞLUFaculty of Medicine, Department of Medical Biochemistry, Necmettin Erbakan University, Konya, Türkiye, 42090, TurkeyErdi Can AytarFaculty of Agriculture Department of Horticulture, Usak University, Uşak, Türkiye, 64200, Turkey. [email protected]
Die Naturwissenschaftenjournal2026en
ABI

Аннотация

This study aimed to investigate the vasorelaxant potential of M. chamomilla extract and its modulatory effects on calcium ion channels.In vitro experiments assessed the extract’s impact on voltage-gated and GPCR-mediated calcium channels in aortic preparations. In vivo, the Tail Cuff method evaluated blood pressure-lowering effects in adrenaline-induced hypertensive rats. Phytochemical profiling was performed via GC-MS, and molecular docking assessed interactions of key compounds with vascular regulation targets (7VFS, 8THK, 3NOS). In vitro, 5 µg/ mL of the extract slightly increased aortic contractility (3.9 ± 3.4%), whereas 60 µg/ mL markedly reduced it (89.5 ± 3.1%). At 50 µg/ mL, it inhibited phenylephrine-induced GPCR-mediated contractions by 84.9 ± 3.8%. In vivo, 40 mg/kg of the extract lowered systolic and diastolic pressures to 150 mmHg and 110 mmHg, respectively. GC-MS identified pinocarveol, coumarin, apigenin derivatives, and dicaffeoylquinic acids. Molecular docking revealed strong affinities of apigenin-7-O-neohesperidoside and other compounds to key vascular targets. Both experimental approaches consistently demonstrated vasorelaxant activity, likely linked to polyphenol and flavonoid content. M. chamomilla extract exhibits significant vasorelaxant and antihypertensive effects, mediated through modulation of calcium channels and bioactive polyphenols. These findings support its potential as a therapeutic agent for hypertension and hypoxia-related cardiovascular disorders, warranting further clinical investigation.

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