Biological Evaluation of Noscapine analogues as Potent and Microtubule-Targeted Anticancer Agents

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作者
Vartika Tomar
Neeraj Kumar
Ravi Tomar
Damini Sood
Neerupma Dhiman
Sujata K. Dass
Satya Prakash
Jitender Madan
Ramesh Chandra
机构
[1] University of Delhi,Department of Chemistry
[2] McGill University,BioMedical Engineering Department, Faculty of Medicine
[3] Amity Institute of Pharmacy,Dr. B. R. Ambedkar Center for Biomedical Research
[4] BL Kapur Hospital,undefined
[5] Chandigarh College of Pharmacy,undefined
[6] University of Delhi,undefined
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In present investigation, an attempt was undertaken to modify the C-9 position of noscapine (Nos), an opium alkaloid to yield 9 -hydroxy methyl and 9 -carbaldehyde oxime analogues for augmenting anticancer potential. The synthesis of 9-hydroxy methyl analogue of Nos was carried out by Blanc reaction and 9-carbaldehyde oxime was engineered by oxime formation method and characterized using FT-IR, 1H NMR, 13C NMR, mass spectroscopy, and so on techniques. In silico docking techniques informed that 9-hydroxy methyl and 9-carbaldehyde oxime analogues of Nos had higher binding energy score as compared to Nos. The IC50 of Nos was estimated to be 46.8 µM signficantly (P < 0.05) higher than 8.2 µM of 9-carbaldehyde oxime and 4.6 µM of 9-hydroxy methyl analogue of Nos in U87, human glioblastoma cells. Moreover, there was significant (P < 0.05) difference between the IC50 of 9-carbaldehyde oxime and 9-hydroxy methyl analogue of Nos. Consistent to in vitro cytotoxicity data, 9-hydroxy methyl analogue of Nos induced significantly (P < 0.05) higher degree of apoptosis of 84.6% in U87 cells as compared to 78.5% and 64.3% demonstrated by 9-carbaldehyde oxime and Nos, respectively. Thus the higher therapeutic efficacy of 9-hydroxy methyl analogue of Nos may be credited to higher solubility and inhibitory constant (K).
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