Bioactive compounds from Matricaria chamomilla: structure identification, in vitro antiproliferative, antimigratory, antiangiogenic, and antiadenoviral activities

Author:

Shaaban Mohamed1ORCID,El-Hagrassi Ali M.2,Osman Abeer F.1,Soltan Maha M.3ORCID

Affiliation:

1. Chemistry of Natural Compounds Department , Division of Pharmaceutical Industries, National Research Centre , El-Behoos St. 33 , Dokki-Cairo 12622 , Egypt

2. Department of Phytochemistry and Plant Systematics , Division of Pharmaceutical Industries, National Research Centre , El-Behoos St. 33 , Dokki-Cairo 12622 , Egypt

3. Biology Unit, Central Laboratory for Pharmaceutical and Drug Industries Research Division , Chemistry of Medicinal Plants Department, National Research Centre , Dokki-Cairo , Egypt

Abstract

Abstract During our exploring the anticancer activity of some medicinal plants and their major metabolites, the aerial parts of the Egyptian Matricaria chamomilla (flowers and stems) were studied. GC–MS analysis of the organic soluble extracts of the flowers and stems fractions revealed the presence of 43 and 45 compounds, respectively. Individual chromatographic purification of the flowers and stems’ extracts afforded three major compounds. Structures of these compounds were identified by 1D- and 2D-NMR and HRESI-MS spectroscopic data as bisabolol oxide A (1) and (E)-tonghaosu (2) (as mixture of ratio 2:1) from the flowers extract, meanwhile apigenin-7-β-d-glucoside (3) from the stems fraction. Biologically, the chamomile extracts announced significant antiproliferative activities exceeded in potency by ∼1.5 fold in case of the stem, recording GI50 13.16 and 17.04 μg/mL against Caco-2 and MCF-7, respectively. Both fractions were approximately equipotent against the migration of the same cell type down to 10 μg/mL together, compounds 1, 2 but not 3, showed considerable growth inhibition of the same cells at GI50 13.36 and 11.83 μg/mL, respectively. Interestingly, they were able to suppress Caco-2 colon cancer cells migration at 5.8 μg/mL and potently inactivate the VEGFR2 angiogenic enzyme (1.5-fold relative to sorafenib. The obtained compounds and corresponding chamomile extracts were evaluated against Adeno-7 virus, revealing that both chamomiles’ extracts (flowers and stems) and their corresponding obtained compounds (1–3) were potent in their depletion to the Adeno 7 infectivity titer, however, the flower extract and compounds 1–2 were more effective than those of the stem extract and its end-product (3).

Publisher

Walter de Gruyter GmbH

Subject

General Biochemistry, Genetics and Molecular Biology

Reference73 articles.

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2. Issac, O. Recent progress in chamomile research – medicines of plant origin in modern therapy, 1st ed. Czecho-Slovakia: Prague Press; 1989.

3. Schilcher, H, Kamille, D. Handbuch furarzte, apotheker und andere naturwissenschaftler, 1st ed. Germany: Wissenschaft Verlagsgesellschaft; 1987.

4. Kotov, AG, Khvorost, PP, Komissarenko, NF. Coumarins of Matricaria recutita. Khim Prirod Sojed 1991;6:853–4.

5. Redaelli, C, Formentini, L, Santaniello, E. HPLC determination of coumarins in Matricaria chamomilla. Planta Med 1981;43:412–3. https://doi.org/10.1055/s-2007-971536.

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