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Sinteza diastereomerno čistih trifluorometiliranih ftalimidopiperidonov kot mimetikov glutarimidnih učinkovin
ID Hribar, Manca (Author), ID Cotman, Andrej Emanuel (Mentor) More about this mentor... This link opens in a new window, ID Adamlje, Boštjan (Comentor)

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Abstract
Imunomodulatorna zdravila, ki vsebujejo učinkovine kot so talidomid, lenalidomid in pomalidomid, se uporabljajo pri terapiji multiplega mieloma. Prav tako pa se jih zaradi njihove afinitete do ligaze E3 cereblon uporablja pri tehnologiji himernih razgrajevalev proteinov (PROTAC). To so hetero-bifunkcionalne molekule, sestavljene iz treh delov: liganda, ki se veže na E3 ubikvitin ligazo, ustreznega distančnika in liganda, ki se veže na tarčni protein. Tvorba trikomponentnega kompleksa vodi do ubikvitinacije tarčnega proteina, ki ji sledi razgradnja s proteasomom. S tarčno razgradnjo lahko delujemo že na več kot 30 različnih proteinov, zato se molekule PROTAC uporablja za zdravljenje različnih rakavih obolenj, imunskih obolenj in nevrodegenerativnih bolezni. V sklopu magistrske naloge smo pripravili analoge talidomida in pomalidomida, ki imajo po eno od karbonilnih skupin glutarimidnega fragmenta zamenjano z bioizosterno trifluoroetilno skupino. Načrtovane molekule imajo dva kiralna centra, zato smo razvili sintezne poti za pripravo posameznih diastereomerov. Strukturo spojin smo potrdili z eno- in dvodimenzionalnimi eksperimenti NMR ter z masno spektrometrijo. Eksperimentalno smo vrednotili njihove fizikalno-kemijske lastnosti (topnost in porazdelitveni koeficient) ter jim s programom SwissADME napovedali farmakokinetične lastnosti. Spojine so pripravljene v količini in čistoti, ki omogočata tudi vrednotenje biološke aktivnosti v primerjavi z glutarimidnimi učinkovinami. Pripravili smo devet končnih spojin, ki imajo celokupno gledano boljše fizikalno-kemijske lastnosti kot glutarimidne učinkovine. Vse spojine so imele boljšo topnost v pufru pri pH 7,4 kot glutarimidni analogi. Pri seriji analogov pomalidomida smo opazili zanimiv trend in sicer, da imajo bioizosterni analogi višjo lipofilnost (logD7,4) in hkrati višjo topnost. Vsi bioizosterni analogi izkazujejo ugodnejše napovedane farmakokinetične vrednosti, in sicer smo spremljali topološko polarno površino (TPSA), prehod skozi krvno možgansko pregrado, ali so spojine substrati za P-glikoprotein in inhibicijo CYP450. Med vsemi spojinami izkazujeta najboljše lastnosti oba diastereomera spojine 4, ki ima bioizosterno zamenjavo na mestu šest 2-aminoglutarimida in tetrafluoro substitucijo na ftalimidnem delu molekule. Vse spojine izkazujejo potencial za nadaljnji razvoj in bodo biološko vrednotene kot vezalci cereblona.

Language:Slovenian
Keywords:bioizoster, stereoselektivna sinteza, PROTAC, rak
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2025
PID:20.500.12556/RUL-169287 This link opens in a new window
Publication date in RUL:22.05.2025
Views:298
Downloads:74
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Secondary language

Language:English
Title:Synthesis of diastereomerically pure trifluoromethylated phthalimidopiperidones as mimetics of glutarimide-based bioactive agents
Abstract:
Immunomodulatory drugs containing active ingredients such as thalidomide, lenalidomide and pomalidomide are mainly used in the treatment of multiple myeloma. They are also used in proteolysis targeting chimera (PROTAC) technology due to their affinity to the E3 ligase cereblon. PROTAC are hetero-bifunctional molecules consisting of three parts: a ligand that binds to the E3 ubiquitin ligase, a suitable linker and a ligand that binds to the target protein. The formation of the three-component complex leads to ubiquitination of the target protein, followed by degradation by the proteasome. By targeting more than 30 different proteins, PROTAC is used to treat a variety of cancers, immune disorders and neurodegenerative diseases. For finetuning of bioactivity, non-glutarimide analogs of the immunomodulatory drugs are highly sought after. As part of the master's thesis, we prepared thalidomide and pomalidomide analogues in which one of the carbonyl groups of the glutarimide fragment is replaced by a bioisosteric trifluoroethyl group. The designed molecules have two chiral centers, therefore we have developed synthetic routes for the preparation of individual diastereomers. The structure of the compounds was confirmed by one- and two-dimensional NMR experiments and by mass spectrometry. Their physicochemical properties (solubility, partition coefficient) were evaluated experimentally and their pharmacokinetic properties were predicted using the SwissADME software. The compounds were prepared in amounts and purities enabling the evaluation of their bioactivity relative to the glutarimide agents. We prepared nine final compounds, which, in general, demonstrated better physicochemical properties than glutarimide active ingredients. All compounds had better solubility in buffer pH 7.4 than glutarimides. In the series of pomalidomide analogs an intriguing trend was observed: the bioisosteric analogs are more lipophilic (logD7,4) and at the same time exhibit better solubility. All analogues had better predicted pharmacokinetic properties, among which we checked topological polar surface area (TPSA), blood-brain barrier penetration, whether the compounds are substrates for P-glycoprotein and CYP450 inhibition. Among all compounds, both diastereomers of compound 4 with the bioisosteric replacement at position six of the 2-aminoglutarimide and with tetrafluoro substitution on the phthalimide moiety, had the best properties. All compounds show potential for further development and will be evaluated as cereblon binders.

Keywords:bioisostere, stereoselective synthesis, PROTAC, cancer

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