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Načrtovanje in sinteza himernih razgrajevalcev monoamin oksidaze A s piperidinskim in piperazinskim distančnikom
ID Dobnik, Gašper (Author), ID Knez, Damijan (Mentor) More about this mentor... This link opens in a new window

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Abstract
Spremembe v aktivnosti oziroma izražanju proteinov so povezane s patologijo številnih bolezni, kot so nevrodegenerativne bolezni in rakava obolenja (npr. rak prostate in rak dojke). Marsikateri proteini so lahko zahtevna tarča za terapijo s klasičnimi majhnimi molekulami, ki so trenutno na trgu, zato poteka intenziven razvoj novih terapevtskih pristopov, kot so himerni razgrajevalci (angl. proteolysis targeting chimeras, PROTAC). Le-ti katalitsko odstranjujejo tarčne proteine, kar omogoča nižje odmerke in razširi nabor potencialnih tarčnih proteinov. Tekom magistrske naloge smo se osredotočili na encim monoamin oksidazo A (MAO-A), ki je v centralnem živčnem sistemu odgovorna za razgradnjo nevrotransmiterjev, posledično igra pomembno vlogo v nastanku in razvoju mentalnih motenj (depresija) in nevrodegenerativnih bolezni, študije pa so potrdile tudi njeno vlogo pri progresiji raka prostate. Na osnovi strukture harmina, selektivnega zaviralca MAO-A, smo načrtovali himerne razgrajevalce s pomalidomidom, kot distančnik pa smo uvajali različne fleksibilne in rigidne elemente. Sintezo smo pričeli s pripravo distančnika: na eni strani smo amin zaščitili v obliki terc-butiloksikarbonilne zaščitene skupine, na drugi strani pa smo pripravili alkil halid. Tako pripravljen distančnik smo v reakciji O-alkiliranja pripeli na molekulo desmetilharmina, nato smo z acidolizo odstranili zaščitno skupino na aminu, z nukleofilno aromatsko substitucijo pa vpeljali še 4-fluorotalidomid in tako pripravili končni heterobifunkcionalni ligand. Izolacija produktov posameznih reakcij je potekala z normalnofazno in reverznofazno kolonsko kromatografijo. Tekom sinteze smo pomembnim vmesnim in končnim ligandom identiteto potrdili z jedrsko magnetno resonanco in masno spektrometrijo, za končne ligande pa smo dodatno določili še čistost s tekočinsko kromatografijo ultra-visoke ločljivosti. Uspešno smo sintetizirali dve molekuli s fleksibilnima distančnikoma in štiri z rigidnimi, za katere smo z biokemijskim testiranjem potrdili, da zavrejo encimsko aktivnost MAO-A. Najmočnejši zaviralec je bila spojina z n-butilnim distančnikom, katerih aktivnost je bila primerljiva s harminom. Rigidni distančniki so bili šibkejši zaviralci MAO-A, kar nakazuje manj ugodno vezavo v aktivno mesto MAO-A.

Language:Slovenian
Keywords:himerni razgrajevalci, monoamin oksidaza, nevrodegenerativne bolezni, rak prostate, rigidni distančniki
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2024
PID:20.500.12556/RUL-155987 This link opens in a new window
Publication date in RUL:26.04.2024
Views:456
Downloads:94
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Secondary language

Language:English
Title:Design and synthesis of monoamine oxidase A proteolysis targeting chimeras with piperidine and piperazine linker
Abstract:
Alterations in the activity or expression of proteins are associated with the pathology of many diseases, e.g., neurodegenerative diseases, and cancer, such as prostate cancer and breast cancer. Many proteins can be challenging targets for therapy with classical small molecules currently on the market. Therefore, new therapeutic modalities are being intensively developed, one example is the proteolysis targeting chimeras (PROTACs), which catalytically remove target proteins, allowing lower doses and broadening the spectrum of possible target proteins. During the master's thesis, we focused on monoamine oxidase A (MAO-A), which is responsible for the degradation of neurotransmitters in the central nervous system and thus plays a key role in the onset and development of mental disorders (depression) and neurodegenerative diseases. Studies have also confirmed its role in the development of prostate cancer. Based on the structure of harmine, a selective MAO-A inhibitor, we have developed chimeric degraders with pomalidomide, using various flexible and rigid linkers. We began the synthesis with the preparation of linkers: on one side the amine was protected in the form of a tert-butyloxycarbonyl protecting group, and on the other side, an alkyl halide was prepared. The linker prepared was attached to the desmethylharmine in the O-alkylation reaction, followed by deprotection of the amine by acidolysis. Final heterobifunctional ligand was prepared by nucleophilic aromatic substitution with 4-fluorothalidomide. Isolation of the products was done by normal-phase and reverse-phase column chromatography. The identity of the intermediates and final ligands was confirmed by nuclear magnetic resonance and mass spectrometry, and the purity of the heterobifunctional ligands was determined by ultra-high-performance liquid chromatography. Two molecules with flexible spacers and four with rigid spacers were successfully synthesized, which inhibited the enzymatic activity of MAO-A as determined in a biochemical assay. The most potent inhibitor was a compound with an n-butyl linker – the inhibitory potency was comparable to that of harmine. Rigid spacers were weaker inhibitors of MAO-A, suggesting less favorable binding to the active site of MAO-A.

Keywords:heterobifunctional degraders, monoamine oxidase, neurodegenerative diseases, prostate cancer, rigid linkers

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