Please use this identifier to cite or link to this item: http://hdl.handle.net/10603/254874
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dc.date.accessioned2019-08-26T06:16:53Z-
dc.date.available2019-08-26T06:16:53Z-
dc.identifier.urihttp://hdl.handle.net/10603/254874-
dc.description.abstractiv newlineABSTRACT newline Synthesis and Biological Evaluation of Inhibitors of Topoisomerases and newlineHistone Deacetylase for In Vitro Anticancer Activity newlineName of student : Gaurav Joshi newlineRegistration Number : 15phdphm01 newlineDegree for which submitted: Ph. D. (Pharmaceutical Sciences) newlineSupervisor : Dr. Raj Kumar newlineCo-Supervisor : Dr. Sandeep Singh newlineDepartment : Pharmaceutical Sciences and Natural Products newlineSchool of Studies : Basic and Applied Sciences newlineKeywords : Cancer, Topoisomerases, Histone deacetylase, newlineTopoisomerases (Topos) and histone deacetylases (HDACs) are validated newlineoncotherapeutic targets due to their involvement in most of the cellular events such as newlineinitiation, proliferation, and survival of cancer cells. Widespread research has newlineundergone to design and discover small molecule inhibitors of each protein which has newlineled to the development of several drugs that are making their presence felt in clinic. newlineConsidering the issues of stability, toxicity, reported crosstalk(s) and resitance of newlineexisting pharmacophores, we herein report the discovery of target-based molecules newlinepertaining to pyrazolo[1,5-c]quinazolines, 2-aryl quinolines and imidazo[1,2- newlinea]quinoxaline scaffolds as inhibitors of TopoI or dual TopoI and II designed rationally newlinevia in silico tools. The chemical space of scaffolds was further exploited to design and newlinesynthesise dual/multi inhibitors of Topo-HDAC by connecting pharmacophoric features newlineof HDAC inhibitors via a linker. newlineDetailed biological evaluation of synthetics was performed using multiple cancer cell newlinelines as well as normal cells/cell lines. Utilizing MTT, dye exclusion, redox potential, cell newlinecycle and annexin V vs PI assays in 2D as well as 3D cultures, we established their newlinepreferential cytotoxic potential. Signaling responsible for anticancer mechanism was newlinedelineated using western immunoblotting and qPCR assays. Further, in vitro assays newlinev newlinefor topoisomerases (DNA relaxation and catenation), and/or HDAC1 revealed target newlinespecificity of synthetics. newlineIn addition, we also demonstrated a novel bioreductive methodology, sp
dc.format.extent
dc.languageEnglish
dc.relation
dc.rightsuniversity
dc.titleSynthesis And Biological Evaluation Of Inhibitors Of Topoisomerases And Histone Deacetylase For In Vitro Anticancer Activity
dc.title.alternative
dc.creator.researcherJoshi, Gaurav
dc.subject.keywordCancer, Topoisomerases, Histone deacetylase
dc.subject.keywordClinical Pre Clinical and Health,Pharmacology and Toxicology,Pharmacology and Pharmacy
dc.description.note
dc.contributor.guideKumar, Raj
dc.publisher.placeBathinda
dc.publisher.universityCentral University of Punjab
dc.publisher.institutionDepartment of Pharmaceutical Sciences and Natural Products
dc.date.registered10/08/2015
dc.date.completed19/08/2019
dc.date.awarded
dc.format.dimensions
dc.format.accompanyingmaterialCD
dc.source.universityUniversity
dc.type.degreePh.D.
Appears in Departments:Department of Pharmaceutical Sciences and Natural Products

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01_title page.pdfAttached File20.48 kBAdobe PDFView/Open
02_declaration.pdf101.21 kBAdobe PDFView/Open
03_certificate.pdf63.29 kBAdobe PDFView/Open
04_abstract.pdf52.86 kBAdobe PDFView/Open
05_acknowledgements.pdf117.6 kBAdobe PDFView/Open
06_table of contents.pdf195.83 kBAdobe PDFView/Open
07_chapter 1.pdf151.1 kBAdobe PDFView/Open
08_chapter 2.pdf1.23 MBAdobe PDFView/Open
09_chapter 3.pdf721.83 kBAdobe PDFView/Open
10_chapter 4.pdf732.76 kBAdobe PDFView/Open
11_chapter 5.pdf3.06 MBAdobe PDFView/Open
12_chapter 6.pdf192.48 kBAdobe PDFView/Open
13_references.pdf238.98 kBAdobe PDFView/Open
14_appendecs.pdf1.59 MBAdobe PDFView/Open
15_publication and awards.pdf18.71 MBAdobe PDFView/Open


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