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Unravelling the anticancer efficacy of 10-oxo-7-epidocetaxel: in vitro and in vivo results
Authors:Arehalli S Manjappa  Rayasa S Ramachandra Murthy
Affiliation:1. Department of Pharmaceutcs, Tatyasaheb Kore College of Pharmacy, Kolhapur, India;2. TIFAC Centre of Relevance and Excellence in New Drug Delivery Systems, G.H. Patel Pharmacy Building, Pharmacy Department, The Maharaja Sayajirao University of Baroda, Vadodara, India;3. Advanced Centre for Treatment Research and Education in Cancer, Tata Memorial Centre, Kharghar, India;4. TIFAC Centre of Relevance and Excellence in New Drug Delivery Systems, G.H. Patel Pharmacy Building, Pharmacy Department, The Maharaja Sayajirao University of Baroda, Vadodara, India
Abstract:Purpose: To prepare 7-epidocetaxel (7ED) and 10-oxo-7-epidocetaxel (10-O-7ED) formulations as like marketed Taxotere® (TXT) injection and to screen them for in vitro and in vivo anticancer efficacy including their in vivo toxicity behavior.

Methods: The 7ED and 10-O-7ED formulations were screened for in vitro anti-proliferative, anti-metastatic and cell cycle arresting behaviors. Further, in vivo acute toxicity of TXT injection containing 10% of 7ED and 10-O-7ED separately and the therapeutic study of 10-O-7ED alone were studied in B16F10 experimental metastasis mouse model.

Results: 10-O-7ED caused significantly higher cytotoxicity after 48 and 72?h than 22?h study. 10-O-7ED showed significantly increased in vitro anti-metastatic activity than TXT. The TXT caused more arrest of cells at S phase, whereas 10-O-7ED arrested more at G2-M phase and vice versa at higher concentration. In vivo acute toxicity study revealed better therapeutic effect with reduced toxicity of TXT containing 10% 10-O-7ED than TXT alone. Similarly, the therapeutic study revealed significantly less number of surface metastatic nodules formation with 10-O-7ED treated group (107?±?49) (***p?<?.0001) than control group (348?±?56). Also, the control group showed significant weight loss at the end (20th day) of the experiment (*p?<?.05, p?=?.041) than 10-O-7ED treated group which showed about 4% increased mean group weight.

Conclusion: Our study revealed the significantly higher in vivo anti-metastatic behavior, with no toxicity, of 10-O-7ED. However, it is a preliminary observation being noticed but further investigations are needed to address the potential of 10-O-7ED in cancer treatment with mechanisms behind the improved therapeutic efficacy with no toxicity.

Keywords:10-oxo-7-epidocetaxel  7-epidocetaxel  B16F10 lung melanoma model  acute toxicity  therapeutic study
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