Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines
Globally, ovarian cancer is the fifth most common cancer among women that affects approximately 1 in 75 women in the developed countries. Over 75% of cases were presented at an advanced stage, with disease spread beyond the ovaries. To date, cervical cancer in women remains a major problem with a...
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my-upm-ir.63182023-10-23T04:25:04Z Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines 2005-04 Mohd Zain, Zetty Nadia Globally, ovarian cancer is the fifth most common cancer among women that affects approximately 1 in 75 women in the developed countries. Over 75% of cases were presented at an advanced stage, with disease spread beyond the ovaries. To date, cervical cancer in women remains a major problem with about 400,000 new cases per year and almost 250, 000 reported deaths. However, this disease affects predominantly poor women in underdeveloped countries. It is estimated that 60% of the glcbal market for anticancer and anti-infectious drugs or those under clinical trial are of natural origin. Zerumbone, a sesquiterpene compound isolated from the rhizomes Zingiber zerumbet was shown to suppress TNF-a release and also induces apoptosis in a variety of human colonic adenocarcinoma cell lines. In this current study, the chemotherapeutic potential of zerumbone in cervical cancer (HeLa) and ovarian cancer (Caov-3) cell lines of human origin was evaluated together with cisplatin, a commercially used drug currently used for treating ovarian and cervical cancers. Exposure of both cancer cells to a range of zerumbone concentrations demonstrated growth inhibition in both cancer cells at a dose-dependent manner. The ICso values, determined by the MTT (3-[4,5-dimethylthiazol-2-yl]-2,Sdiphenyltetrazolium bromide) reduction assay were as follows: zerumbone; Caov-3, 24.0 pM (5.2 pg/ml), HeLa, 20.7 pM (4.5 pg/ml) and cisplatin; Caov-3, 3.7 pM (1.1 pglml), HeLa, 5.3 pM (1.6 pg/ml). Laser scanning confocal microscopy following AOIPI staining were used to examine morphological changes of both cancer cells after zerumbone and cisplatin treatment. Apoptotic features that included membrane blebbing and nucleus condensation were evident in both treated cancer cells. Following this, TUNEL (TdT-mediated dUTP Nick-End Labeling) assay was conducted to confirm apoptosis. The studies conducted seems to suggest that zerumbone induce cell death by stimulating apoptosis better than cisplatin, based on significantly higher percentage of apoptotic cells in zerumbone treated cancer cells as compared to cisplatin. In addition, zerumbone and cisplatin arrests cancer cells at G2/M phase as analyzed by flow cytometry. Abnormal synthesis of 1L-6 appears to contribute to the pathogenesis of several kinds of diseases and the constitutive production of IL-6 has been implicated in malignant diseases. Increased levels of IL-6 indicated the aggressiveness of a disease. IL-6 is suggested to provide prognostic value based on its role as a cancer cell growth factor. The effects of zerumbone on IL- 6 levels were studied using a human base ELISA. The results indicated that zerumbone significantly decreased the levels of IL-6 secreted by both cancer cells. However, membrane-bound IL-6 receptor is still intact after zerumbone treatment as demonstrated using immunology fluorescence technique. This study concludes that the compound, zerumbone inhibits both cancer cells growth through the induction of apoptosis, arrests cell cycle at G2/M phase and inhibits the secretion levels of IL-6 in both cancer cells. Therefore, zerumbone is a potential candidate as a useful chemotherapeutic agent in treating both cervical and ovarian cancers in future. 2005-04 Thesis http://psasir.upm.edu.my/id/eprint/6318/ http://psasir.upm.edu.my/id/eprint/6318/1/FPSK%28M%29_2005_3.pdf text en public masters Universiti Putra Malaysia Faculty Medicine and Health Sciences Abdul, Ahmad Bustamam English |
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English English |
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Abdul, Ahmad Bustamam |
| topic |
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Mohd Zain, Zetty Nadia Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines |
| description |
Globally, ovarian cancer is the fifth most common cancer among women that affects
approximately 1 in 75 women in the developed countries. Over 75% of cases were
presented at an advanced stage, with disease spread beyond the ovaries. To date,
cervical cancer in women remains a major problem with about 400,000 new cases per
year and almost 250, 000 reported deaths. However, this disease affects
predominantly poor women in underdeveloped countries. It is estimated that 60% of
the glcbal market for anticancer and anti-infectious drugs or those under clinical trial
are of natural origin. Zerumbone, a sesquiterpene compound isolated from the
rhizomes Zingiber zerumbet was shown to suppress TNF-a release and also induces
apoptosis in a variety of human colonic adenocarcinoma cell lines. In this current
study, the chemotherapeutic potential of zerumbone in cervical cancer (HeLa) and
ovarian cancer (Caov-3) cell lines of human origin was evaluated together with
cisplatin, a commercially used drug currently used for treating ovarian and cervical
cancers. Exposure of both cancer cells to a range of zerumbone concentrations
demonstrated growth inhibition in both cancer cells at a dose-dependent manner. The
ICso values, determined by the MTT (3-[4,5-dimethylthiazol-2-yl]-2,Sdiphenyltetrazolium
bromide) reduction assay were as follows: zerumbone; Caov-3, 24.0 pM
(5.2 pg/ml), HeLa, 20.7 pM (4.5 pg/ml) and cisplatin; Caov-3, 3.7 pM (1.1 pglml),
HeLa, 5.3 pM (1.6 pg/ml). Laser scanning confocal microscopy following AOIPI
staining were used to examine morphological changes of both cancer cells after
zerumbone and cisplatin treatment. Apoptotic features that included membrane
blebbing and nucleus condensation were evident in both treated cancer cells.
Following this, TUNEL (TdT-mediated dUTP Nick-End Labeling) assay was
conducted to confirm apoptosis. The studies conducted seems to suggest that
zerumbone induce cell death by stimulating apoptosis better than cisplatin, based on
significantly higher percentage of apoptotic cells in zerumbone treated cancer cells as
compared to cisplatin. In addition, zerumbone and cisplatin arrests cancer cells at
G2/M phase as analyzed by flow cytometry. Abnormal synthesis of 1L-6 appears to
contribute to the pathogenesis of several kinds of diseases and the constitutive
production of IL-6 has been implicated in malignant diseases. Increased levels of IL-6
indicated the aggressiveness of a disease. IL-6 is suggested to provide prognostic
value based on its role as a cancer cell growth factor. The effects of zerumbone on IL-
6 levels were studied using a human base ELISA. The results indicated that
zerumbone significantly decreased the levels of IL-6 secreted by both cancer cells.
However, membrane-bound IL-6 receptor is still intact after zerumbone treatment as
demonstrated using immunology fluorescence technique. This study concludes that the
compound, zerumbone inhibits both cancer cells growth through the induction of
apoptosis, arrests cell cycle at G2/M phase and inhibits the secretion levels of IL-6 in
both cancer cells. Therefore, zerumbone is a potential candidate as a useful
chemotherapeutic agent in treating both cervical and ovarian cancers in future. |
| format |
Thesis |
| qualification_level |
Master's degree |
| author |
Mohd Zain, Zetty Nadia |
| author_facet |
Mohd Zain, Zetty Nadia |
| author_sort |
Mohd Zain, Zetty Nadia |
| title |
Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines |
| title_short |
Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines |
| title_full |
Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines |
| title_fullStr |
Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines |
| title_full_unstemmed |
Cytotoxic Effects of Zerumbone on Ovarian and Cervical Cancer Cell Lines |
| title_sort |
cytotoxic effects of zerumbone on ovarian and cervical cancer cell lines |
| granting_institution |
Universiti Putra Malaysia |
| granting_department |
Faculty Medicine and Health Sciences |
| publishDate |
2005 |
| url |
http://psasir.upm.edu.my/id/eprint/6318/1/FPSK%28M%29_2005_3.pdf |
| _version_ |
1783725727565217792 |