Vývoj inhibitorů halogenalkandehalogenas Bakalářská práce Brno 2011 Tomáš Buryška Instituce
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Graf 2: Úbytek koncentrace cyklopropyl bromidu v čase. Šedá barva byla použita pro abiotický rozklad, černá pro reakci s LinB. V první fázi byly otestovány komerčně dostupné látky (Tabulka 4). Seznam nejlepších substrátů obsahoval také látky, které nejsou komerčně dostupné. Některé z nich byly vyhledány v databázi NCI (Národní rakovinný institut USA), objednány a jejich testování v současné době probíhá. Zbylé látky bude nutné připravit organickou syntézou. 6.3 Hodnocení inhibičního účinku druhé sady potenciálních inhibitorů Z předchozích měření vyplývá, že cyklopropyl bromid nelze enzymaticky pomocí halogenalkandehalogenas odbourat. Pro vysokou podobnost s molekulami běžných substrátů lze předpokládat vazbu do aktivního místa enzymů, čímž by mohla inhibovat enzymatickou reakci. Proto byl cyklopropyl bromid otestován stejným způsobem (Graf 3) jako molekuly první sady, aby bylo možné provést porovnání. Z experimentálního hodnocení specifických aktivit látek virtuálního screeningu (Tabulka 7) je dále patrné, že jedním ze substrátů s nejvyšší specifickou aktivitou je 1,2-dibrompropan. Je známo, že dibromované krátké alkany jsou substráty s vysokou specifickou aktivitou (Koudelakova, Chovancova et al. 2011). Dalším otestovaným potenciálním inhibitorem byl 1,3-difluorpropan, který je nereaktivním analogem tohoto typu sloučenin. Naměřený pokles specifické aktivity za přítomnosti 1,3-difluorpropanu je statisticky nevýznamný a pravděpodobně nezpůsobuje hledaný inhibiční účinek (Graf 3). Graf 3: Specifická aktivita LinB za přítomnosti a nepřítomnosti 1,3-difluorpropanu, respektive cyklopropyl bromidu. Tabulka 8: Relativní aktivity LinB za přítomnosti druhé sady potenciálních inhibitorů.
6.4 Hodnocení vazby cyklopropyl bromidu pomocí metody zastaveného toku Cílem měření bylo zjistit, zda se cyklopropyl bromid váže do aktivního místa enzymu a interaguje s halogenid-stabilizujícími rezidui. Tento fakt se projevuje jako pokles fluorescenčního signálu tryptofanů s rostoucí koncentrací cyklopropyl bromidu v aktivním místě enzymu. Koncentrace saturovaného roztoku cyklopropyl bromidu byla ověřena pomocí GC-MS. Experimenty ukázaly (Graf 4), že přítomnost cyklopropyl bromidu ovlivňuje fluorescenci. Graf 4: Relativní fluorescence tryptofanů v aktivním místě LinB za přítomnosti cyklopropyl bromidu. Fluorescenční data získaná metodou zastaveného toku byla proložena Stern-Volmerovým modelem s využitím programu OriginPro 8.5. Vypočtená hodnota rovnovážné vazebné konstanty cyklopropyl bromidu byla 1,4 ± 0,4 mM-1. Relativně nízká vazebná konstanta koresponduje se slabým inhibičním účinkem této látky na aktivitu haloalkandehalogenasy LinB (Graf 3). 7. Diskuze První částí této práce bylo měření reziduálních aktivit první sady potenciálních inhibitorů. Tři z těchto potenciálních inhibitorů jsou fluorované analogy dobrých substrátů. Využívají neschopnosti halogenalkandehalogenas štěpit kovalentní vazbu uhlík-fluor. Problémem by mohla být krátká vzdálenost atomu fluoru od uhlíku, čímž by nemuselo dojít k dostatečně silné interakci s nukleofilním kyslíkem aspartátu. Čtvrtá látka využívá konceptu prostorového uspořádání substituentů na uhlíkové kostře, které předpokládá bránění nukleofilnímu ataku. Všechny látky ukázaly významnou inhibici specifické aktivity halogenalkandehalogenas (Graf 5), nicméně s ohledem k vysokým koncentracím potřebným k pozorované inhibici lze předpokládat slabou vazbu těchto prvních inhibitorů do aktivního místa těchto enzymů. Graf 5: Srovnání relativních reziduálních aktivit potenciálních inhibitorů. Následně byl proveden virtuální screening k nalezení nových substrátů. Nejlepší potenciální substráty byly experimentálně otestovány s enzymy DbjA a LinB na jejich specifickou aktivitu. V případě, že se látka ukázala nereaktivní, bylo provedeno kontrolní měření na GC-MS pro detekci velmi pomalé enzymatické reakce. Do druhé sady experimentálně testovaných potenciálních inhibitorů byly zahrnuty dvě látky. První z nich byl nereaktivní cyklopropyl bromid. Druhou látkou je odpovídající nereaktivní strukturní analog nejlepších substrátů– 1,3-difluorpropan. Stejně jako v případě první sady inhibitorů nebyly pozorovány dostatečné silné inhibiční účinky (Graf 5). Jejich rovnovážná vazebná konstanta je odhadována v jednotkách až desítkách mM-1. Rovnovážné konstanty vazby používaných léčiv na jejich cílové receptory se pohybují v řádech nM-1 až pM-1 (Babine and Bender 1997; Livnah, Bayer et al. 1993). Tyto první identifikované inhibitory haloalkandehalogenas nesplňují parametry účinných léčiv, proto bude nutné pokračovat v navazajících projektech v hledání dalších možných kandidátů nebo modifikaci kandidátů stávajících. 8. Shrnutí
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