Sinteza N-acil-N-(piperidin-4-ilmetil)aminskih zaviralcev imunoproteasoma

Turšič, Živa

Sinteza N-acil-N-(piperidin-4-ilmetil)aminskih zaviralcev imunoproteasoma
ID Turšič, Živa (Avtor), ID Obreza, Aleš (Mentor) Več o mentorju... Povezava se odpre v novem oknu

, ID Sosič, Izidor (Komentor)

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Izvleček

Ubikvitin-proteasomski sistem je v evkariontskih celicah odgovoren za razgradnjo znotrajceličnih proteinov in vzdrževanje njihove homeostaze. Poleg konstitutivnega proteasoma, ki je odgovoren za regulacijo celičnih procesov s selektivno razgradnjo proteinov, poznamo tudi imunoproteasom, ki se nahaja v celicah imunskega izvora in nastane pri vnetju, stresnih in imunskih odzivih. Imunoproteasom ima pomembno vlogo pri razgradnji proteinov, ki so nastali zaradi oksidativnega stresa in vnetnega odziva, ter tako predstavlja pomembno terapevtsko tarčo za zdravljenje vnetnih, rakavih, avtoimunih in nevrodegenerativnih bolezni. Na trgu je že nekaj zaviralcev proteasoma, ki se uporabljajo za zdravljenje, nekateri pa so v postopku kliničnega preizkušanja. Večina izmed njih je neselektivnih in zavirajo več katalitičnih podenot obeh proteasomov, kar je vzrok za številne neželene učinke. Razvoj zaviralcev imunoproteasoma gre v smer sinteze selektivnih nepeptidnih zaviralcev β5i katalitične podenote imunoproteasoma, saj bi se s tem zmanjšala pojavnost neželenih učinkov, povečala metabolna stabilnost zaviralcev, povečala njihova biološko uporabnost in izboljšale fizikalno-kemijske lastnosti. V magistrski nalogi smo načrtovali in sintetizirali N-(4-morfolinobenzil)-1-(piperidin-4-il)metanaminske zaviralce, ki so imeli v strukturi elektrofilno »bojno glavo«, namenjeno zaviranju imunoproteasoma preko tvorbe kovalentne vezi s katalitičnim treoninom v β5i podenoti imunoproteasoma. Po reduktivnem aminiranju ustrezno izbranega amina in aldehida smo dobili vmesni produkt, na katerega smo s postopkom N-aciliranja na nastalo sekundarno aminsko skupino pripenjali različne fragmente, ki so se razlikovali po velikosti in terminalni funkcionalni skupini. Na koncu smo spojinam pod kislimi pogoji odstranili še terc-butilkarbamatno zaščitno skupino. Istovetnost končnih spojin smo potrdili z metodami 1H NMR, HRMS, IR in z 13C NMR. Tako smo uspešno sintetizirali šest končnih spojin, ki smo jih na koncu biokemijsko ovrednotili z merjenjem rezidualne aktivnosti β5i aktivnosti imunoproteasoma v prisotnosti zaviralcev. Nobena od sintetiziranih spojin ni zavirala imunoproteasoma, vendar rezultati pomembno prispevajo k boljšemu razumevanju strukturnih lastnosti zaviralcev tega kemijskega razreda in vplivu strukture na njihovo zaviranje katalitične podenote β5i imunoproteasoma.

Jezik:	Slovenski jezik
Ključne besede:	imunoproteasom, elektrofilna »bojna glava«, UPS, zaviralci, podenota β5i
Vrsta gradiva:	Magistrsko delo/naloga
Organizacija:	FFA - Fakulteta za farmacijo
Leto izida:	2022
PID:	20.500.12556/RUL-134841
Datum objave v RUL:	04.02.2022
Število ogledov:	889
Število prenosov:	171
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Izvleček:
Jezik:	Angleški jezik
Naslov:	Synthesis of N-acyl-N-(piperidin-4-ylmethyl)amine immunoproteasome inhibitors
Ubiquitin-proteasome system in eukaryotic cells is the main system responsible for the degradation of intracellular proteins and maintaining their homeostasis. In addition to the constitutive proteasome, which is responsible for regulation of cell processes with selective degradation of proteins, immunoproteasome has also been characterized. It is mainly located in cells of immune origin however, its expression can be induced when inflammation, stressful or autoimmune situations occur. Immunoproteasome has important role in degradation of proteins, which have been modified because of oxidative stress and inflammatory responses, and therefore represents an important therapeutic target for the treatment of inflammatory, cancerous, autoimmune, and neurodegenerative diseases. There are three proteasome inhibitors present on the market and few additional inhibitors are undergoing clinical trial procedures. Most of them do not distinguish between catalytically active subunits of both proteasomes and this lack of selectivity is the main reason for many side effects of currently available proteasome targeting drugs. Development of immunoproteasome-selective inhibitors is oriented to preparation of non-peptide inhibitors of β5i subunit of immunoproteasome, as this would reduce the incidence of side effects, increase metabolic stability of compounds, increase their bioavailability and improve physicochemical properties. In the master´s thesis, we designed and synthesized N-(4-morpholinobenzyl)-1-(piperidin-4-yl)methanamine-based inhibitors, which possessed an electrophilic »warhead« in their structure, aimed to form a covalent bond with the catalytic threonine β5i subunit and thus to contribute to inhibition of immunoproteasome significantly. After reductive amination of the appropriately-substituted amine and aldehyde we obtained the main secondary amine intermediate, which was further N-acylated by attaching various fragments that differed in size and terminal functional group. Finally, tert-butylcarbamate protecting group was removed under acidic conditions. The final compounds were characterized by means of 1H NMR, HRMS, IR and 13C NMR methods. To assess inhibitory activities, we biochemically evaluated six successfully synthesized compounds by measuring the residual β5i activity of the enzyme in the presence of inhibitors. None of the synthesized compound inhibited the immunoproteasome however, the results will contribute to the understanding of structure-activity relationship of this compound class immunoproteasome inhibitors.
Ključne besede:	immunoproteasom, electrophilic “warhead”, UPS, inhibitors, β5i subunit

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