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Biokonjugacija in poskus inducirane (homo)dimerizacije proteinov z azid-alkin cikloadicijo
ID Suhorepec, Nadja (Author), ID Svete, Jurij (Mentor) More about this mentor... This link opens in a new window

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Abstract
Reakcije biokonjugacije so primeri bioortogonalnih reakcij, pri katerih se tvori kovalentna vez med dvema molekulama, pri čemer je ena izmed njih biološka molekula ali njen fragment. Tovrstne reakcije med drugim predstavljajo tudi način kemijskega navzkrižnega povezovanja ali zamreženja (angl. cross-linking) proteinov brez uporabe genetskega inženirstva. Za kovalentno označevanje proteinov se uporabljajo različni reagenti, med najpogostejšimi so N-hidroksisukcinimidni estri (NHS estri), ki reagirajo s prostimi aminskimi skupinami lizinskih ostankov ali tiolnimi skupinami cisteinskih ostankov. Na ta način lahko proteine kovalentno označimo z želeno funkcionalno skupino z vezavo (konjugacijo) s primerno funkcionaliziranim reagentom. V sklopu magistrskega dela, usmerjenega k inducirani dimerizaciji nativnih proteinov, smo pripravili različne NHS estre in benzotriazolide, funkcionalizirane bodisi z azidno bodisi s ciklooktinsko skupino. Razvili smo protokol za vezavo teh molekul na proteine ter analitsko metodo za kvantifikacijo vezave na proteine. Kvantifikacija je bila sestavljena iz ''klik'' reakcije med azido-funkcionaliziranim fluoresceinom in z alkinom označenim proteinom (in obratno), ki ji je sledilo merjenje fluorescence iz gela, dobljenega z SDS-PAGE. S pomočjo dobljenih informacij o količini vezanih označevalcev na protein, smo izvedli poskuse inducirane dimerizacije proteinov preko azid-ciklooktin [3+2] cikloadicije, kar je privedlo do tvorbe kovalentnega 1,2,3-triazolnega povezovalca. Z namenom podaljšanja povezovalne verige med proteinoma smo pripravili tudi bifunkcionalne reagente.

Language:Slovenian
Keywords:biokonjugacija, fluorescein, inducirana dimerizacija, cikloadicija
Work type:Master's thesis/paper
Typology:2.09 - Master's Thesis
Organization:FKKT - Faculty of Chemistry and Chemical Technology
Year:2024
PID:20.500.12556/RUL-165364 This link opens in a new window
COBISS.SI-ID:220256771 This link opens in a new window
Publication date in RUL:04.12.2024
Views:892
Downloads:360
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Secondary language

Language:English
Title:Bioconjugation and attempted induced (homo)dimerization of proteins utilizing azide-alkyne cycloaddition
Abstract:
Bioconjugation reactions are examples of bioorthogonal reactions in which a covalent bond is formed between two molecules, one of which is a biological molecule or its fragment. Such bioorthogonal reactions are also suitable for chemical cross-linking of proteins without the use of genetic engineering. Various reagents are used for covalent binding to proteins, with N-hydroxysuccinimidyl esters (NHS esters) being among the most common. These molecules preferentially react with free amine groups of lysine residues or thiol groups of cysteine residues. In this way, proteins can be covalently labelled with a desired functional group by conjugation (binding) with a suitably functionalized reagent. As part of this thesis, we prepared various NHS esters and benzotriazolides that were functionalized with either an azide group or a cyclooctyne group. We developed a protocol for binding these molecules to proteins and an analytical method for quantifying the binding (loading) to proteins. Quantification consisted of a ‘click’ reaction between the azide-labelled fluorescein and the alkyne-labelled protein (and vice versa), followed by measuring the fluorescence intensity from the gel obtained by SDS-PAGE. With known loading of labels on the protein in hand, we were able to perform experiments on induced protein dimerization via azide–cyclooctyne [3+2] cycloaddition reaction, resulting in formation of a covalent 1,2,3-triazole linker. To extend the linker, we also prepared bifunctional reagents that could act as intermediate connectors of the two protein molecules.

Keywords:bioconjugation, fluorescein, induced dimerization, cycloaddition

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