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Vrednotenje endokrinih učinkov izbranih ftalatov in silico
ID Gajšek, Tea (Author), ID Sollner Dolenc, Marija (Mentor) More about this mentor... This link opens in a new window

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Abstract
Ftalati se nahajajo v številnih potrošniških izdelkih, vključno z izdelki za osebno nego, farmacevtskimi izdelki, kozmetiko in ovojnino za živila. Ftalati, ki jih uporabljamo kot mehčala, niso kemično vezani na plastične polimere, zato smo jim v veliki meri izpostavljeni zaradi odpuščanja iz izdelkov, ki vsebujejo tako pripravljeno plastiko, predstavljajo pa tudi nevarnost za okolje. V zadnjih letih se je povečalo raziskovanje vpliva potencialnih kemičnih motilcev endokrinega sistema. Škodljive učinke na endokrini sistem izkazujejo tudi ftalati, zato smo se v magistrski nalogi osredotočili na 26 izbranih ftalatov ter z in silico metodo vrednotili njihov endokrini potencial. Za vrednotenje smo uporabili prosto dostopen računalniški program Endocrine Disruptome (ED), ki omogoča sidranje spojin v aktivna mesta 18 struktur, ki pripadajo 14 različnim jedrnim hormonskim receptorjem. Pridobljene rezultate smo primerjali s podatki iz strokovne literature. Glede na pridobljene rezultate in dostopnost informacij v podatkovnih bazah smo ftalate uvrstili v štiri skupine. Predvsem smo želeli ugotoviti, ali program pravilno napove vezavo tistih ftaltov, ki so že biološko ovrednoteni. V prvo skupino sodijo ftalati, ki so uvrščeni na seznam potencialnih hormonskih motilcev, s programom pa smo napovedali srednjo ali veliko verjetnost interakcij z vsaj enim receptorjem. Ti ftalati so benzil butil ftalat (BBP), difenil ftalat (DPhP) in dicikloheksil ftalat (DCHP). V drugi skupini so tisti, ki so prav tako uvrščeni med potencialne motilce endokrinega sistema, ED pa zanje ni napovedal interakcij s srednjo ali visoko verjetnostjo. V to skupino smo uvrstili največ testiranih ftalatov, dimetil ftalat (DMP), dietil ftalat (DEP), dipropil ftalat (DPP), dibutil ftalat (DBP), diizobutil ftalat (DiBP), dimetoksietil ftalat (DMEP), dipentil ftalat (DPeP), diizopentil ftalat (DiPeP), diheksil ftalat (DHP), di-(2-etilheksil) ftalat (DEHP), dioktil ftalat (DOP), dinonil ftalat (DNP), diizononil ftalat (DiNP), diizodecil ftalat (DiDP) in ditridecil ftalat (DTDP). V tretji skupini so ftalati, ki glede na dostopne podatke ne povzročajo učinkov na endokrini sistem, niti ni njihovega škodljivega delovanja napovedal program. V tej skupini se nahajajo dialil ftalat (DAP), diheptil ftalat (DHpP), didecil ftalat (DDcP) in di-(2-propilheptil) ftalat (DPHP). V zadnji skupini pa so ftalati, ki glede na literaturne podatke ne delujejo na endokrin sistem, program pa je zanje napovedal škodljivo delovanje. Ti ftalati so: butil cikloheksil ftalat (BCHP), dibenzil ftalat (DBzP), dimetil cikloheksil ftalat (DMCHP) in cikloheksil isooktil ftalat (CHIOP). Metode in silico so enostavne za uporabo, toksičnost spojin pa lahko ocenimo še preden so te sintetizirane. Pri interpretaciji rezultatov se moramo zavedati, da zgolj z metodami in silico ne moremo potrditi delovanja spojin. Le-tega lahko potrdimo z nadaljnjimi študijami in vitro in in vivo, kar velja tudi za vezavo proučevanih ftalatov na izbrane receptorje in njihovo potencialno endokrino delovanje.

Language:Slovenian
Keywords:ftalati, kemični motilci endokrinega sistema, Endocrine Disruptome, jedrni hormonski receptorji, metode in silico
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2022
PID:20.500.12556/RUL-137133 This link opens in a new window
Publication date in RUL:02.06.2022
Views:763
Downloads:96
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Secondary language

Language:English
Title:In silico evaluation of endocrine activity of selected phthalates
Abstract:
Phthalates are found in many consumer products, including personal care products, pharmaceuticals, cosmetics and food packaging. Used as plasticizers are not chemically bound to plastic polymers. Therefore, we are largely exposed to them due to their leaking of products containing such prepared plastic. They also pose a danger to the environment. In the past years, research into the impact of potential chemical endocrine disruptors has increased. Phthalates also show harmful effects on the endocrine system, so in this master's thesis we focused on 26 selected phthalates and evaluated their endocrine disruption potential using in silico method. For evaluation, we used the freely available computer program Endocrine Disruptome (ED), which allows the docking of compounds to the active sites of 18 structures of 14 different nuclear hormone receptors. The obtained results were compared with data from the professional literature. According to the obtained results and the availability of information in databases, phthalates were classified into four groups. Above all, we wanted to determine whether the program correctly predicts the binding of those phthalates that are already biologically evaluated. The first group includes phthalates, which are included in the list of potential hormone disruptors and the program predicted a medium or high probability of interactions with at least one receptor. This phthalates are benzyl butyl phthalate (BBP), diphenyl phthalate (DPhP) and dicyclohexyl phthalate (DCHP). The second group includes does who are also classified as potential endocrine disruptors and Endocrine Disruptome did not predict their interactions with medium or high probability. The highest number of tested phthalates was included in this group, dimethyl phthalate (DMP), diethyl phthalate (DEP), dipropyl phthalate (DPP), dibutyl phthalate (DBP), diisobutyl phthalate (DiBP), dimethoxyethyl phthalate (DMEP), dipentyl phthalate (DPeP), diisopentyl phthalate (DiPeP), dihexyl phthalate (DHP), di-(2-ethylhexyl) phthalate (DEHP), dioctyl phthalate (DOP), dinonyl phthalate (DNP), diisononyl phthalate (DiNP), diisodecyl phthalate (DiDP) and ditridecyl phthalate (DTDP). The third group includes phthalates, which, according to the available data, do not cause effects on the endocrine system, nor have their harmful effects been predicted with the program. This group includes diallyl phthalate (DAP), diheptyl phthalate (DHpP), didecyl phthalate (DDcP) and di-(2-propylheptyl) phthalate (DPHP). In the last group are phthalates which according to the literature do not work on the endocrine system, but the program predicted harmful effects for them. These phthalates are: butyl cyclohexyl phthalate (BCHP), dibenzyl phthalate (DBzP), dimethyl cyclohexyl phthalate (DMCHP) and cyclohexyl isooctyl phthalate (CHIOP). The in silico methods are easy to use and the toxicity of the compounds can be assessed before they are even synthesized. When interpreting the results, we must be aware that the action of compounds cannot be confirmed by method in silico alone. This can be confirmed by further in vitro and in vivo studies, which also applies to the binding of the studied phthalates to selected receptors and their potential endocrine function.

Keywords:phthalates, chemical endocrine disruptors, Endocrine Disruptome, nuclear hormone receptors, method in silico

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