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Sinteza izoksazolopirimidinskih agonistov Tollu podobnega receptorja 7 z različnimi substitucijami na izoksazolnem obroču
ID Slokan, Tjaša (Author), ID Sova, Matej (Mentor) More about this mentor... This link opens in a new window, ID Strašek, Nika (Co-mentor)

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Abstract
Tollu podobni receptorji (TLR) so pomembna skupina receptorjev, ki igrajo ključno vlogo v prirojenem in pridobljenem imunskem sistemu. So obetavne tarče za zdravljenje okužb, avtoimunskih bolezni in raka. Pri človeku so do sedaj odkrili 10 različnih tipov TLR. V okviru magistrske naloge smo se osredotočili na TLR7, ki je endosomski receptor in prepoznava enoverižno RNA virusov. S TLR7 povzročena aktivacija imunskega sistema privede do protivnetnega, protivirusnega in protitumornega delovanja, zato TLR7 predstavlja potencialno tarčo za zdravljenje virusnih okužb, alergijske astme in rakavih obolenj. Na podlagi znanega TLR7 agonista 3-(4-fluorofenil)-4-(3-metilpiperidin-1-il)-6- (trifluorometil)izoksazolo[5,4-d]pirimidina smo načrtovali in sintetizirali 11 novih potencialnih agonistov TLR7. Za sintezo analogov 6-(trifluorometil)izoksazolo[5,4-d]pirimidina z različnimi substitucijami na izoksazolnem obroču smo uporabili šeststopenjski sintezni postopek. Končne spojine smo ovrednotili na humani celični liniji HEK293. Določili smo jim topnost v DMSO in celičnem mediju, citotoksičnost ter preverili njihovo agonistično delovanje na TLR7. Ugotovili smo, da so vse sintetizirane spojine zaradi svoje lipofilnosti slabo topne v celičnem mediju. Posledično so bili preliminarni testi agonizma izvedeni pri nizkih koncentracijah, kar je vplivalo na jakost agonističnega delovanja na TLR7. Spojine z izobutilaminskim fragmentom na pirimidinskem obroču (37, 38, 40 in 41), so se izkazale za citotoksične. Izmed vseh sintetiziranih spojin je le 3-(4-klorofenil)-4-(3-metilpiperidin-1-il)-6- (trifluorometil)izoksazolo[5,4-d]pirimidin (35) izkazoval agonistično delovanje na TLR7 z vrednostjo EC50 21,4 μM. Spojina 35 predstavlja dobro izhodišče za nadaljno optimizacijo, predvsem v smislu izboljšanja fizikalno-kemijskih lastnosti.

Language:Slovenian
Keywords:Tollu-podobni receptorji, TLR7, agonist, 6-(trifluorometil)izoksazolo[5, 4- d]pirimidin
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2022
PID:20.500.12556/RUL-141302 This link opens in a new window
Publication date in RUL:28.09.2022
Views:572
Downloads:93
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Secondary language

Language:English
Title:Synthesis of isoxazolopyrimidine Toll-like receptor 7 agonists with different substitutions on the isoxazole ring
Abstract:
Toll-like receptors (TLRs) are an important group of receptors that play a critical role in the innate and adaptive immune system. TLRs are promising targets for the treatment of infections, autoimmune diseases, and cancer. To date, 10 members of TLRs have been identified in humans. In this thesis, we focused on TLR7, an endosomal receptor that recognizes single-stranded RNA. Enhanced activation of the immune system by TLR7 leads to anti-inflammatory, antiviral, and antitumor activity. Therefore, TLR7 is a potential target for the treatment of viral infections, allergic asthma, and cancer. Based on the chemical structure of the known TLR7 agonist 3-(4-fluorophenyl)-4-(3-methyl piperidine-1-il)-6-(trifluoromethyl)isoxazolo[5,4-d]pirimidine, we designed and synthesized 11 new potential TLR7 agonists. A six-step synthetic pathway was used to synthesize the 6- (trifluoromethyl)isoxazolo[5,4-d]pirimidine analogs with different substitutions on the isoxazole ring. The final compounds were tested on the human HEK293 cell line. The solubility of the synthesized compounds in DMSO and cell media, cytotoxicity, and potential TLR7 agonist activity were determined. We found that all synthesized compounds dissolved poorly in cell media due to their high lipophilicity. For this reason, preliminary tests for agonism were performed at low concentrations, which affected the potency of TLR7 agonist activity. Compounds 37, 38, 40, and 41, all with an isobutylamine fragment on the pyrimidine ring, are cytotoxic. Of all the synthesized compounds, only 3-(4-chlorophenyl)-4-(3-methylpiperidine-1-il)-6- (trifluoromethyl)isoxazolo[5,4-d]pyrimidine (35) shows TLR7 agonist activity with an EC50 value of 21,4 μM. Compound 35 represent a good starting point for further optimization, especially in terms of improving physicochemical properties.

Keywords:Toll-like receptors, TLR7, agonist, 6-(trifluoromethyl)isoxazolo[5, 4-d]pirimidine

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