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The chemotherapeutic effect of β-2-himachalen-6-ol in chemically induced skin tumorigenesis

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dc.contributor.author Daaboul, Hamid E.
dc.contributor.author Dagher, Carole
dc.contributor.author Taleb, Robin I.
dc.contributor.author Bodman-Smith, Kikki
dc.contributor.author Shebaby, Wassim N.
dc.contributor.author El-Sibai, Mirvat
dc.contributor.author Mroueh, Mohamad A.
dc.contributor.author Daher, Costantine F.
dc.date.accessioned 2019-10-08T13:29:29Z
dc.date.available 2019-10-08T13:29:29Z
dc.date.copyright 2018 en_US
dc.date.issued 2019-10-08
dc.identifier.issn 1950-6007 en_US
dc.identifier.uri http://hdl.handle.net/10725/11398
dc.description.abstract β-2-himachalen-6-ol (HC), a novel sesquiterpene derived from Lebanese wild carrot, was shown to possess a remarkable anticancer activity. The present study investigates the in vitro anticancer activity of HC and its effect on papillomas induced using a DMBA/TPA skin carcinogenesis mouse model. HaCaT-ras II-4 epidermal squamous cell viability was assessed using WST-1 kit. Cell cycle was analyzed by flow cytometry, and pro/anti-apoptotic proteins were measured using western blot. Mice papillomas were induced by DMBA and promoted with TPA for 18 weeks. At week 12, animals were divided into four groups: HC topically treated (5%Top), HC intraperitoneally treated (25 mg/kg; HC25), Cisplatin treated (2.5 mg/kg), and control (DMSO treated). Papilloma yield, volume, histology, and mice weight and liver function were assessed. HC treatment decreased significantly cell survival (IC50 = 7 and IC90 = 40 μg/ml) and increased significantly cells undergoing late apoptosis and necrosis. It also significantly decreased the levels of pro-caspase-3, p53, Bcl-2, p-Erk/Erk and p-Akt/Akt and increased p21 and Bax proteins. Treatment with HC25, HC5%Top or Cisplatin showed a significant decrease in papilloma yield and volume. Only Cisplatin treatment caused a significant decrease in body weight and increase in serum ALT. In conclusion, β-2-himachalen-6-ol induced significant tumor shrinkage, an effect partly mediated via promoting apoptosis through inhibition of the MAPK/ERK and PI3K/AKT pathways, with no significant toxicity to laboratory mice. en_US
dc.language.iso en en_US
dc.title The chemotherapeutic effect of β-2-himachalen-6-ol in chemically induced skin tumorigenesis en_US
dc.type Article en_US
dc.description.version Published en_US
dc.author.school SAS en_US
dc.author.school SOP en_US
dc.author.idnumber 200902770 en_US
dc.author.idnumber 201205733 en_US
dc.author.idnumber 200703859 en_US
dc.author.idnumber 199190130 en_US
dc.author.idnumber 199190130
dc.author.department Natural Sciences en_US
dc.description.embargo N/A en_US
dc.relation.journal Biomedicine & Pharmacotherapy en_US
dc.journal.volume 103 en_US
dc.journal.issue 2018 en_US
dc.article.pages 443-452 en_US
dc.keywords Daucus carota en_US
dc.keywords Skin cancer en_US
dc.keywords β-2-himachalen-6-ol en_US
dc.keywords Wild carrot en_US
dc.keywords DMBA/TPA carcinogenesis en_US
dc.identifier.doi https://doi.org/10.1016/j.biopha.2018.04.027 en_US
dc.identifier.ctation Daaboul, H. E., Dagher, C., Taleb, R. I., Bodman-Smith, K., Shebaby, W. N., El-Sibai, M., ... & Daher, C. F. (2018). The chemotherapeutic effect of β-2-himachalen-6-ol in chemically induced skin tumorigenesis. Biomedicine & Pharmacotherapy, 103, 443-452. en_US
dc.author.email robin.taleb@lau.edu.lb en_US
dc.author.email wassim.shebaby@lau.edu.lb en_US
dc.author.email mirvat.elsibai@lau.edu.lb en_US
dc.author.email mmroueh@lau.edu.lb en_US
dc.author.email cdaher@lau.edu.lb
dc.identifier.tou http://libraries.lau.edu.lb/research/laur/terms-of-use/articles.php en_US
dc.identifier.url https://www.sciencedirect.com/science/article/pii/S0753332217350837 en_US
dc.orcid.id https://orcid.org/0000-0001-8033-6951 en_US
dc.orcid.id https://orcid.org/0000-0002-9782-1870 en_US
dc.orcid.id https://orcid.org/0000-0003-4084-6759 en_US
dc.orcid.id https://orcid.org/0000-0003-1572-7133 en_US
dc.orcid.id https://orcid.org/0000-0002-8275-7263 en_US
dc.author.affiliation Lebanese American University en_US


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