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Sinteza 1H-pirazol-5-il karbamatnih zaviralcev butirilholin esteraze in z mitogenom aktivirane protein kinaze p38α
ID Knapić, Maja (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 kronična, progresivna in ireverzibilna nevrodegenerativna bolezen, ki predstavlja veliko socialno in ekonomsko breme, predvsem pa velik izziv za bolnika in njegove bližnje. Je najpogostejši vzrok za demenco, kaže pa se z upadom kognitivnih sposobnosti (zlasti spomina), ki ga lahko spremljajo tudi nevropsihiatrični simptomi. Patofiziologija bolezni še ni povsem pojasnjena, obstajajo pa različne hipoteze, ki pojav in napredovanje bolezni pripisujejo različnim spremembam v možganih, kot so odmiranje holinergičnih nevronov v delih možganov, pomembnih za oblikovanje spomina, in sprememba v presnovi amiloidnega prekurzorskega proteina, ki vodi v odlaganje amiloida β, ta pa dodatno pripomore k ob bolezni že prisotnemu nevrovnetju in oksidativnemu stresu ter povečanemu nastajanju hiperfosforiliranega proteina tau. Trenutno še nimamo zdravila, ki bi bolezen povsem ozdravilo, pač pa z obstoječimi zaviralci holin esteraz in antagonistom receptorjev N-metil-D-aspartata (NMDA) lajšamo simptome bolezni, z monoklonskimi protitelesi pa upočasnjujemo kognitivni upad. V sklopu magistrske naloge smo se lotili načrtovanja in sinteze 1H-pirazol-5-il karbamatnih dvojnih zaviralcev encimov butirilholin esteraze (BChE) in z mitogenom aktivirane protein kinaze 38α (p38α MAPK). Pri zasnovi spojin smo izhajali iz spojine DP-802, ki je znan nekompetitivni zaviralec p38α MAPK, da pa bi omogočili hkratno delovanje tudi na encim BChE, smo sečninski fragment nadomestili s karbamatom. Nato smo naše spojine zasnovali kot disubstituirane karbamate, in sicer kot alkil aril karbamate, pri čemer je alkilni del pri vseh naših končnih spojinah (11A-C) metilna skupina, arilni del pa predstavlja fenilni obroč, ki je pri spojini 11A substituiran s klorom na orto mestu, pri spojini 11B s klorom na meta mestu in pri spojini 11C disubstituiran z metilno skupino na orto in meta mestu. Sintetiziranim končnim spojinam smo zaviralno aktivnost na BChE določili z Ellmanovo metodo, zaviralno aktivnost na p38α MAPK pa z ADP-Glo testom. Nobena spojina ni izkazovala aktivnosti na acetilholin esterazo, kar je zaželeno, saj so bile vse selektivne na BChE, vendar pa je samo spojina 11B nanomolarni psevdo-ireverzibilni zaviralec BChE. Spojini 11A in 11C sta mikromolarna kompetitivna zaviralca BChE. Nobena od spojin, žal, ni zavirala encima p38α MAPK, kar je verjetno posledica izgube vodikovih vezi, ki smo jih izgubili z zamenjavo sečnine s karbamatom, delno pa tudi z metiliranjem karbamatnega dušika.

Language:Slovenian
Keywords:Alzheimerjeva bolezen, BChE, p38α MAPK, dvojni zaviralci, večtarčno zdravljenje.
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2025
PID:20.500.12556/RUL-170126 This link opens in a new window
Publication date in RUL:02.07.2025
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Downloads:54
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Secondary language

Language:English
Title:Synthesis of 1H-pyrazole-5-yl carbamate inhibitors of butyrylcholinesterase and p38α mitogen-activated protein kinase
Abstract:
Alzheimer's disease (AD) is a chronic, progressive and irreversible neurodegenerative disease that imposes a heavy social and economic burden and is especially challenging for the patient and his family. It is the most common cause of dementia and is characterised by cognitive decline (especially in memory), which may be accompanied by neuropsychiatric symptoms. The pathophysiology of the disease is not yet fully understood, but there are various hypotheses that attribute the onset and progression of the disease to different changes in the brain, such as the atrophy of cholinergic neurons in parts of the brain important for memory formation and a change in the metabolism of amyloid precursor protein leading to the deposition of amyloid β, which contributes to the neuroinflammation and oxidative stress already present in the disease, and to the increased production of the hyperphosphorylated protein tau. We still do not have a cure, but we are using existing choline esterase inhibitors and N-methyl-D-aspartate (NMDA) receptor antagonist to alleviate the symptoms of the disease and monoclonal antibodies to slow cognitive decline. In the context of this thesis, we set out to design and synthesise 1H-pyrazol-5-yl carbamate dual inhibitors of butyrylcholine esterase (BChE) and p38α mitogen-actived protein kinase (p38α MAPK). The design of the compounds was based on DP-802, a known non-competitive inhibitor of p38α MAPK, but to allow simultaneous action on the BChE enzyme, the urea fragment of this compound was replaced by carbamate. We then designed our compounds as disubstituted carbamates, namely as alkyl aryl carbamates, where the alkyl moiety in all our final compounds (11A-C) is the methyl group and the aryl moiety is the phenyl ring, which is substituted with a chlorine at the ortho site in compound 11A, with a chlorine at the meta site in compound 11B and with a methyl group at the ortho and meta sites in compound 11C. The inhibitory activity on BChE was determined by the Ellman method and the inhibitory activity on p38α MAPK by the ADP-Glo test. None of the compounds showed activity on acetylcholinesterase, which is desirable as all were selective on BChE, but only compound 11B is a nanomolar pseudo-irreversible inhibitor of BChE. Compounds 11A and 11C are micromolar competitive inhibitors of BChE. However, none of the compounds showed inhibitory activity on the p38α MAPK enzyme, which is probably due to the loss of the hydrogen bonds lost by the replacement of urea by carbamate and by methylation of carbamate nitrogen.

Keywords:Alzheimer's disease, BChE, p38α MAPK, dual inhibitors, multi-target therapy.

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