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Sinteza in vrednotenje C-1 substituiranih derivatov glukozamina kot zaviralcev encima MurA
ID Kambič, Ana (Avtor), ID Frlan, Rok (Mentor) Več o mentorju... Povezava se odpre v novem oknu

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Izvleček
Bakterijske okužbe so v porastu zaradi vse bolj pogoste pojavnosti rezistence na antibiotike, kar predstavlja resno grožnjo sodobni medicini. Uspešno obvladovanje tega problema zahteva mednarodno sodelovanje, celovit pristop in prilagajanje strategij glede na nove ugotovitve in trende, predvsem pa spremljanje pojavnosti odpornih bakterij in izvajanje ukrepov za preprečevanje njihovega širjenja. Ker se smrtnost povečuje, je nujno raziskovati nove možnosti v razvoju učinkovitih protibakterijskih učinkovin. V postopku sinteze pomembnega gradnika bakterijske celične stene peptidoglikana ima osrednjo vlogo encim MurA. MurA katalizira prenos enolpiruvata iz fosfoenolpiruvata (PEP) na UDP-N-acetilglukozamin (UDP-GlcNAc), kar je ključni korak v sintezi predhodnice peptidoglikana, UDP-N-acetilmuraminske kisline. Omenjeni encim je pomembna tarča za razvoj novih protibakterijskih učinkovin. V magistrski nalogi je opisana sinteza analogov glukozamina z modifikacijami na mestu C1. Začetni korak je bila sinteza spojine, na katero bomo v nadaljevanju pripenjali kisle fragmente. Iz acetiliranega glukozamin klorida smo z nukleofilno substitucijo in katalitskim hidrogeniranjem sintetizirali spojino, s katero smo v nadaljevanju na mestu C-1 tvorili amidne vezi z različnimi reagenti (kislinami) s pomočjo sklopitvenih reagentov. Med reakcijo se tvori amidna vez med primarno amino skupino izhodne spojine in karbonilno skupino različnih dikislin, ki imajo eno od karboksilnih skupin zaščitenih, da reakcija poteče selektivno. V nadaljevanju sledi hidroliza zaščitnih skupin. Tako smo sintetizirali analoge glukozamina, ki z aktivnim mestom encima MurA tvorijo ustrezne interakcije. Končne spojine smo analizirali s spektroskopskimi, kromatografskimi in spektrometričnimi metodami.

Jezik:Slovenski jezik
Ključne besede:rezistenca, peptidoglikan, encim MurA, analog glukozamina, antibiotik
Vrsta gradiva:Magistrsko delo/naloga
Organizacija:FFA - Fakulteta za farmacijo
Leto izida:2024
PID:20.500.12556/RUL-163024 Povezava se odpre v novem oknu
Datum objave v RUL:01.10.2024
Število ogledov:101
Število prenosov:16
Metapodatki:XML DC-XML DC-RDF
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Sekundarni jezik

Jezik:Angleški jezik
Naslov:Synthesis and evaluation of C-1 substituted glucosamine derivatives as MurA inhibitors
Izvleček:
Bacterial infections are on the rise due to the increasing incidence of antibiotic resistance, which poses a serious threat to modern medicine. Successful management of this problem requires international cooperation, a comprehensive approach and the adaptation of strategies in the light of new findings and trends, and above all the monitoring of the occurrence of resistant bacteria and the implementation of measures to prevent their spread. As mortality increases, it is imperative to explore new options in the development of effective antibacterial agents. In the process of synthesis of an important part of the bacterial cell wall peptidoglycan, the enzyme MurA plays a central role. MurA catalyzes the transfer of enolpyruvate from phosphonolpyruvate (PEP) to UDP-N-acetylglucosamine (UDP-GlcNAc), a key step in the synthesis of the peptidoglycan precursor, UDP-N-acetylmuramic acid. This enzyme is an important target for the development of new antibacterial agents. The thesis describes the synthesis of glucosamine analogues with modifications at the C1 site. The initial step was the synthesis of the compound, to which the acidic fragments will be attached. A compound was synthesized from acetylated glucosamine chloride by nucleophilic substitution and catalytic hydrogenation, with which I subsequently formed amide bonds with various reagents (acids) by means of coupling reagents at the C-1 site. During the reaction, an amide bond is formed between the primary amino group of the parent compound and the carbonyl group of various diacids, of which one of the carboxylic groups is protected to ensure the reaction proceeds selectively. This is followed by hydrolysis of the acetyl groups and the protective groups. Thus, we synthesized analogues of glucosamine, which form corresponding interactions with the active site of the enzyme MurA. Finally, glucosamine analogues were analysed by spectroscopic, chromatographic and spectrometric methods.

Ključne besede:resistance, peptidoglycan, MurA enzyme, glucosamine analogues, antibiotik

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