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Sinteza fragmentov za pripravo [1,2,4]triazolo[4,3-a]piridonskih zaviralcev butirilholin esteraze
ID Bojc, Karin (Author), ID Obreza, Aleš (Mentor) More about this mentor... This link opens in a new window, ID Ferjančič Benetik, Svit (Comentor)

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Abstract
Alzheimerjeva bolezen (AB) je najpogostejša oblika demence in predstavlja velik zdravstveni izziv sodobne družbe. Zanjo so značilni kognitivni, funkcionalni in vedenjski simptomi, katerih pojav je povezan z odlaganjem amiloidnih plakov in tvorbo nevrofibrilarnih pentelj zaradi hiperfosforilacije proteina tau. Ker natančen mehanizem nastanka bolezni še ni pojasnjen, so bile razvite različne hipoteze, kot so amiloidna hipoteza, hipoteza proteina tau, holinergična in nevrovnetna hipoteza ter druge. Trenutna zdravila za AB omogočajo predvsem lajšanje simptomov, ne pa tudi zaustavitve patoloških procesov. Pri sodobnih raziskavah se za zdravljenje AB vedno bolj uveljavlja pristop večtarčnih ligandov, ki omogočajo hkratno delovanje na več ključnih tarč. Namen magistrske naloge je bil sinteza spojin, ki bi sočasno zavirale butirilholin esterazo (BChE) in z mitogenom aktivirano protein kinazo p38α (p38α MAPK). BChE ima namreč pomembno vlogo v pozni fazi AB, saj postane glavni encim za razgradnjo acetilholina, medtem ko p38α MAPK sodeluje pri nevrovnetnih procesih, povezanih s toksičnim učinkom Aβ in hiperfosforilacijo tau proteina. Njuno hkratno zaviranje predstavlja potencialno strategijo za izboljšanje kognitivnih funkcij in vplivanje na patofiziološki potek bolezni. Eksperimentalno delo je temeljilo na razvoju spojin, pri čemer nam je kot izhodiščna molekula služila spojina 41, ki je znan zaviralec p38α MAPK. V sklopu sintez so bile izvedene reakcije ciklizacije, aromatske nukleofilne substitucije, redukcije in diazotiranja. Med postopki so se pokazali številni izzivi, med drugim nestabilnost produktov, težave s selektivnostjo reakcij, stranski produkti in praktične omejitve pri delu z žveplovimi spojinami. Kljub temu je uspela priprava več vmesnih produktov, ki predstavljajo obetavne fragmente za nadaljnji razvoj. Čeprav nam ni uspelo sintetizirati končnih spojin z dvojnim zaviralnim učinkom, rezultati nakazujejo smiselnost nadaljnjega raziskovanja. Pridobljeni fragmenti lahko služijo kot osnova za optimizacijo in pripravo učinkovitih večtarčnih ligandov, ki bi v prihodnje prispevali k celovitejšemu zdravljenju Alzheimerjeve bolezni.

Language:Slovenian
Keywords:Alzheimerjeva bolezne, BChE, p38α MAPK, večtarčni ligandi, zaviralci encimov
Work type:Master's thesis/paper
Typology:2.09 - Master's Thesis
Organization:FFA - Faculty of Pharmacy
Year:2025
PID:20.500.12556/RUL-175483 This link opens in a new window
COBISS.SI-ID:256632579 This link opens in a new window
Publication date in RUL:29.10.2025
Views:125
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Secondary language

Language:English
Title:Synthesis of fragments for preparing [1,2,4]triazolo[4,3-a]pyridinone butyrylcholine esterase inhibitors
Abstract:
Alzheimer's disease is the most common form of dementia and represents a major public health challenge in modern society. It is characterized by cognitive, functional and behavioral symptoms which are associated with the deposition of amyloid plaques and the formation of the neurofibrillary tangles caused by tau protein hyperphosphorylation. Since the exact mechanism underlying the disease remains unclear, several hypotheses have been proposed, including the amyloid hypothesis, hypothesis protein tau, cholinergic hypothesis, neuroinflammatory and others. Current therapies primarily alleviate symptoms but do not halt the pathological processes. In recent research, the concept of multitarget ligands has gained increasing importance, as it allows simultaneous action on multiple key targets. The aim of master’s thesis was the synthesis of compounds capable of simultaneously inhibiting butyrylcholine esterase (BChE) and p38α mitogen-activated protein kinase (p38α MAPK). BChE plays an important role in the later stages of Alzheimer’s disease, as it becomes the main enzyme responsible for acetylcholine degradation, while p38α MAPK is involved in neuroinflammatory processes associated with the toxic effects of Aβ and tau protein hyperphosphorylation. Their concurrent inhibition represents a potential strategy to improve cognitive functions and influence the pathophysiological progression of the disease. The experimental work was based on the development of compounds, using compound 41, a known p38α MAPK inhibitor, as the starting molecule. The synthesis included cyclization, aromatic nucleophilic substitution, reduction and diazotization reactions. Several challenges emerged during these procedures, such as instability of products, limited reaction selectivity, the formation of side products and practical difficulties associated with sulfur-containing compounds. Nevertheless, several intermediates were successfully synthesized, representing promising fragments for further development. Although the final compounds with dual inhibitory activity were not successfully synthesized, the results indicate the relevance of further research. The synthesized fragments can serve as a foundation for optimization and the design of effective multitarget ligands, which may in the future contribute to more comprehensive treatment strategies for Alzheimer’s disease.

Keywords:Alzheimer’s disease, BChE, p38α MAPK, multitarget ligands, enzyme inhibitors

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