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Antiausterity agents from Uvaria dac and their preferential cytotoxic activity against human pancreatic cancer cell lines in a nutrient-deprived condition

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dc.contributor.author Awale S.
dc.contributor.author Ueda J.-Y.
dc.contributor.author Athikomkulchai S.
dc.contributor.author Abdelhamed S.
dc.contributor.author Yokoyama S.
dc.contributor.author Saiki I.
dc.contributor.author Miyatake R.
dc.date.accessioned 2021-04-05T03:34:08Z
dc.date.available 2021-04-05T03:34:08Z
dc.date.issued 2012
dc.identifier.issn 1633864
dc.identifier.other 2-s2.0-84866465067
dc.identifier.uri https://ir.swu.ac.th/jspui/handle/123456789/14320
dc.identifier.uri https://www.scopus.com/inward/record.uri?eid=2-s2.0-84866465067&doi=10.1021%2fnp300295h&partnerID=40&md5=4effeb550f4d7fc8bb4bcbf645de20bb
dc.description.abstract Human pancreatic cancer cell lines are known for their inherent tolerance to nutrition starvation, which enables them to survive under a hypovascular (austerity) tumor microenvironment. The search for agents that preferentially retard the survival of cancer cells under low nutrition conditions (antiausterity agent) is a novel approach to anticancer drug discovery. In this study, it was found that a dichloromethane extract of the stem of Uvaria dac preferentially inhibited PANC-1 human pancreatic cancer cells survival under nutrition-deprived conditions at a concentration of 10 μg/mL. Workup of this bioactive extract led to the discovery of (+)-grandifloracin (8) as a potent antiausterity agent as evaluated in a panel of four human pancreatic cancer cell lines, PANC-1 (PC50, 14.5 μM), PSN-1 (PC50, 32.6 μM), MIA PaCa-2 (PC50, 17.5 μM), and KLM-1 (32.7 μM). (+)-Grandifloracin (8) has been isolated from a natural source for the first time. Its absolute stereochemistry was established by single-crystal X-ray crystallography and circular dichroism spectroscopic analysis. In addition to this, seven other new highly oxygenated cyclohexene derivatives, named uvaridacanes A (1) and B (2), uvaridacols A-D (3, 4, 6, 7), and uvaridapoxide A (5), were also isolated and structurally characterized. © 2012 American Chemical Society and American Society of Pharmacognosy.
dc.subject cyclohexene derivative
dc.subject dichloromethane
dc.subject grandifloracin
dc.subject unclassified drug
dc.subject uvaridacane A
dc.subject uvaridacane B
dc.subject uvaridacol A
dc.subject uvaridacol B
dc.subject uvaridacol C
dc.subject uvaridacol D
dc.subject uvaridapoxide A
dc.subject antineoplastic agent
dc.subject bridged compound
dc.subject cyclohexene derivative
dc.subject grandifloracin
dc.subject uvaridacane A
dc.subject uvaridacane B
dc.subject Annonaceae
dc.subject article
dc.subject cancer cell culture
dc.subject cell strain KLM 1
dc.subject cell strain MIA PaCa 2
dc.subject cell strain PANC 1
dc.subject cell strain PSN 1
dc.subject circular dichroism
dc.subject cytotoxicity
dc.subject drug isolation
dc.subject drug structure
dc.subject human
dc.subject human cell
dc.subject nutritional deficiency
dc.subject pancreas cancer
dc.subject stereochemistry
dc.subject tumor microenvironment
dc.subject Uvaria dac
dc.subject X ray crystallography
dc.subject chemistry
dc.subject drug screening
dc.subject isolation and purification
dc.subject nuclear magnetic resonance
dc.subject pancreas tumor
dc.subject Thailand
dc.subject Uvaria
dc.subject Agouti paca
dc.subject Uvaria
dc.subject Antineoplastic Agents, Phytogenic
dc.subject Bridged Compounds
dc.subject Crystallography, X-Ray
dc.subject Cyclohexenes
dc.subject Drug Screening Assays, Antitumor
dc.subject Humans
dc.subject Nuclear Magnetic Resonance, Biomolecular
dc.subject Pancreatic Neoplasms
dc.subject Thailand
dc.subject Uvaria
dc.title Antiausterity agents from Uvaria dac and their preferential cytotoxic activity against human pancreatic cancer cell lines in a nutrient-deprived condition
dc.type Article
dc.rights.holder Scopus
dc.identifier.bibliograpycitation Journal of Natural Products. Vol 75, No.6 (2012), p.1177-1183
dc.identifier.doi 10.1021/np300295h


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