| dc.contributor.advisor | Pour, Milan | |
| dc.creator | Šnajdr, Ivan | |
| dc.date.accessioned | 2018-10-19T09:27:57Z | |
| dc.date.available | 2018-10-19T09:27:57Z | |
| dc.date.issued | 2009 | |
| dc.identifier.uri | http://hdl.handle.net/20.500.11956/23674 | |
| dc.description.abstract | V ramci teto disertačni prace byla vyvinuta metodika připravy 3,6- disubstituovanych pyranonů a bylo připraveno 15 finalnich laktonů, u kterych byla pote zkoumana jejich cytostaticka a antifungalni aktivita. Kličovymi kroky připravy latek byla Yamaguchi-Hiraova alkylace, hydroaluminace nasledovana jodaci a Pd-katalyzovana karbonylativni laktonizace. Žadna z cilovych latek nevykazovala cytostatickou ani antifungalni aktivitu, což je vzhledem k vyznamne antifugalni aktivitě butenolidovych analogů překvapive. V dalši časti je popsan vyvoj syntezy 3-monosubstituovanych pyranonů. Vyvinuty postup využiva jako vychozi latky 5,6-dihydro-2H-pyran-2-onu, ktery je v dalšim kroku převeden na 3-jod-5,6- dihydro-2Hpyran- 2-on. Kličovym krokem je pak nasledny Pd-katalyzovany Suzukiho coupling. V posledni časti je popsana připrava několika derivatů α- a β-substituovanych-γ- alkylidenpentenolidů. Cilove latky se vyznačovaly vyznamnou cytostatickou aktivitou (IC50 < 5 μmol/L) vůči všem testovanym nadorovym liniim (CCRF-CEM, HeLa S3, HT 29, HL 60, L 1210). | cs_CZ |
| dc.description.abstract | Within the framework of this Thesis, a method fot the preparation of 3,6- disubstituted pyranones was developed and 15 final lactones were synthesized, and their cytostatic and antifungal activity was investigated. Principal steps in the preparation of the compounds were Yamaguchi-Hirao alkylation, hydroalumination followed by iodation and Pd- catalyzed carbonylative lactonization. None of the target compounds displayed interesting cytostatic or antifungal activity (IC50 < 10 μmol/L), which was suprising given the significant antifungal activity of analogous butenolides. The development of the synthesis of 3- monosubstituted pyranones is described next. Our strategy is based on the use of 5,6-dihydro-2H- pyran-2-one as the starting material, which was converted into the 3-iodo-5,6-dihydro-2H- pyran-2-one in one step. The key step of the synthesis was Pd-catalyzed Suzuki coupling. Finally, the preparation of α- and β-substituted-γ-alkylidenepentenolides is described. The target compounds exhibited significant cytostatic activity (IC50 < 5 μmol/L) against all tested tumor cells (CCRF-CEM, HeLa S3, HT 29, HL 60, L 1210). | en_US |
| dc.language | Čeština | cs_CZ |
| dc.language.iso | cs_CZ | |
| dc.publisher | Univerzita Karlova, Farmaceutická fakulta v Hradci Králové | cs_CZ |
| dc.title | Využití Pd-katalyzovaných reakcí v syntéze laktonů | cs_CZ |
| dc.type | dizertační práce | cs_CZ |
| dcterms.created | 2009 | |
| dcterms.dateAccepted | 2009-12-11 | |
| dc.description.department | Katedra organické a bioorganické chemie | cs_CZ |
| dc.description.department | Department of Organic And Bioorganic Chemistry | en_US |
| dc.description.faculty | Faculty of Pharmacy in Hradec Králové | en_US |
| dc.description.faculty | Farmaceutická fakulta v Hradci Králové | cs_CZ |
| dc.identifier.repId | 85680 | |
| dc.title.translated | Application of Pd-Catalyzed Reactions to the Synthesis of Lactones | en_US |
| dc.contributor.referee | Kotora, Martin | |
| dc.contributor.referee | Opletalová, Veronika | |
| dc.identifier.aleph | 001406834 | |
| thesis.degree.name | Ph.D. | |
| thesis.degree.level | doktorské | cs_CZ |
| thesis.degree.discipline | Bioorganic Chemistry | en_US |
| thesis.degree.discipline | Bioorganická chemie | cs_CZ |
| thesis.degree.program | Organic Chemistry | en_US |
| thesis.degree.program | Organická chemie | cs_CZ |
| uk.thesis.type | dizertační práce | cs_CZ |
| uk.taxonomy.organization-cs | Farmaceutická fakulta v Hradci Králové::Katedra organické a bioorganické chemie | cs_CZ |
| uk.taxonomy.organization-en | Faculty of Pharmacy in Hradec Králové::Department of Organic And Bioorganic Chemistry | en_US |
| uk.faculty-name.cs | Farmaceutická fakulta v Hradci Králové | cs_CZ |
| uk.faculty-name.en | Faculty of Pharmacy in Hradec Králové | en_US |
| uk.faculty-abbr.cs | FaF | cs_CZ |
| uk.degree-discipline.cs | Bioorganická chemie | cs_CZ |
| uk.degree-discipline.en | Bioorganic Chemistry | en_US |
| uk.degree-program.cs | Organická chemie | cs_CZ |
| uk.degree-program.en | Organic Chemistry | en_US |
| thesis.grade.cs | Prospěl/a | cs_CZ |
| thesis.grade.en | Pass | en_US |
| uk.abstract.cs | V ramci teto disertačni prace byla vyvinuta metodika připravy 3,6- disubstituovanych pyranonů a bylo připraveno 15 finalnich laktonů, u kterych byla pote zkoumana jejich cytostaticka a antifungalni aktivita. Kličovymi kroky připravy latek byla Yamaguchi-Hiraova alkylace, hydroaluminace nasledovana jodaci a Pd-katalyzovana karbonylativni laktonizace. Žadna z cilovych latek nevykazovala cytostatickou ani antifungalni aktivitu, což je vzhledem k vyznamne antifugalni aktivitě butenolidovych analogů překvapive. V dalši časti je popsan vyvoj syntezy 3-monosubstituovanych pyranonů. Vyvinuty postup využiva jako vychozi latky 5,6-dihydro-2H-pyran-2-onu, ktery je v dalšim kroku převeden na 3-jod-5,6- dihydro-2Hpyran- 2-on. Kličovym krokem je pak nasledny Pd-katalyzovany Suzukiho coupling. V posledni časti je popsana připrava několika derivatů α- a β-substituovanych-γ- alkylidenpentenolidů. Cilove latky se vyznačovaly vyznamnou cytostatickou aktivitou (IC50 < 5 μmol/L) vůči všem testovanym nadorovym liniim (CCRF-CEM, HeLa S3, HT 29, HL 60, L 1210). | cs_CZ |
| uk.abstract.en | Within the framework of this Thesis, a method fot the preparation of 3,6- disubstituted pyranones was developed and 15 final lactones were synthesized, and their cytostatic and antifungal activity was investigated. Principal steps in the preparation of the compounds were Yamaguchi-Hirao alkylation, hydroalumination followed by iodation and Pd- catalyzed carbonylative lactonization. None of the target compounds displayed interesting cytostatic or antifungal activity (IC50 < 10 μmol/L), which was suprising given the significant antifungal activity of analogous butenolides. The development of the synthesis of 3- monosubstituted pyranones is described next. Our strategy is based on the use of 5,6-dihydro-2H- pyran-2-one as the starting material, which was converted into the 3-iodo-5,6-dihydro-2H- pyran-2-one in one step. The key step of the synthesis was Pd-catalyzed Suzuki coupling. Finally, the preparation of α- and β-substituted-γ-alkylidenepentenolides is described. The target compounds exhibited significant cytostatic activity (IC50 < 5 μmol/L) against all tested tumor cells (CCRF-CEM, HeLa S3, HT 29, HL 60, L 1210). | en_US |
| uk.file-availability | V | |
| uk.publication.place | Hradec Králové | cs_CZ |
| uk.grantor | Univerzita Karlova, Farmaceutická fakulta v Hradci Králové, Katedra organické a bioorganické chemie | cs_CZ |
| thesis.grade.code | P | |
| dc.identifier.lisID | 990014068340106986 | |
