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dc.contributor.author Zsákai, Lilian
dc.contributor.author Nemeth G,
dc.contributor.author Szantai-Kis C,
dc.contributor.author Greff Z,
dc.contributor.author Horvath Z,
dc.contributor.author Szokol, Bálint
dc.contributor.author Baska, Ferenc
dc.contributor.author Őrfi, László
dc.contributor.author Kéri, György
dc.date.accessioned 2015-11-23T21:40:10Z
dc.date.available 2015-11-23T21:40:10Z
dc.date.issued 2013
dc.identifier 84886237797
dc.identifier.citation pagination=47-56; journalVolume=83; journalIssueNumber=2; journalTitle=ACTA PHARMACEUTICA HUNGARICA;
dc.identifier.uri http://repo.lib.semmelweis.hu//handle/123456789/2487
dc.description.abstract Fibroblast Growth Factor Receptor (FGFR) family is a sequentially highly related subgroup of membrane proteins consisting of four tyrosine kinase type enzyme: FGFR1, FGFR2, FGFR3 and FGFR4. These are kinases of great interest in a wide spectrum of physiological processes such as tissue repair via controlling cell proliferation. As initiatiors of cell proliferation, in some cases they have leading roles in several types of cancer, eg. breast cancer, pancreas cancer, gastric tumors and multiple myeloma via overexpression and/or mutation. This phenomenon makes them promising targets for drug development in order to develop signal transduction therapies based on small molecule FGFR inhibitors. We have developed two main groups of lead molecules: compounds with benzotiophene and oxindole cores utilizing numerous methods from in silico modelling via in vitro biochemichal assays and testing on relevant cell lines to citotoxicity assays.
dc.relation.ispartof urn:issn:0001-6659
dc.title Potencialis antitumor hatasu FGFR inhibitorok fejlesztese.
dc.type Journal Article
dc.date.updated 2015-11-20T13:58:39Z
dc.language.rfc3066 hu
dc.identifier.mtmt 2379928
dc.identifier.pubmed 23926649
dc.contributor.department SE/GYTK/Gyógyszerészi Kémiai Intézet
dc.contributor.department SE/AOK/I/OVMBPI/MTA-SE Pathobiokémiai Kutatócsoport
dc.contributor.institution Semmelweis Egyetem


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