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Vpliv zaviralcev katepsinov B in X na endocitozo tumorskih matičnih celic
ID Bernik, Teja (Author), ID Mitrović, Ana (Mentor) More about this mentor... This link opens in a new window, ID Pečar Fonović, Urša (Comentor)

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Abstract
Rak dojke predstavlja drugo najsmrtonosnejšo bolezen pri ženskah. Zahvaljujoč presejalnim programom in napredku pri diagnosticiranju ter zdravljenju bolezni se je smrtnost v zadnjih desetletjih zmanjšala. Največjo težavo pri uspešnem zdravljenju pa še vedno predstavljajo tumorske matične celice. Le te so zaradi svoje specifične sposobnosti samoobnavljanja in diferenciacije namreč odporne na večino trenutnih načinov zdravljenja. Po zaključku zdravljenja pogosto ostanejo v telesu, kjer se ponovno začnejo razmnoževati, diferencirati do rakavih celic in metastazirati, kar privede do ponovnega nastanka tumorja ter ponovitve bolezni. Zaradi teh specifičnih lastnosti tumorskih matičnih celic potrebujemo nove načine zdravljenja, ki bi učinkovito delovali tudi na to populacijo celic. Možnost novih terapevtskih tarč predstavljata cisteinska katepsina B in X, ki sta pri raku udeležena pri vseh stopnjah nastanka in napredovanja raka, ter sta njuno izražanje in aktivnost povečana tudi v tumorskih matičnih celicah. Tumorske matične celice smo v magistrski nalogi na podlagi sposobnosti tvorbe tumorskih sfer, izolirali iz celičnih linij MDA-MB-231, MCF-7 in MCF-10A neoT. Pri tem smo čistost izoliranih tumorskih matičnih celic povečali s pripravo sekundarnih tumorskih sfer. Na izoliranih tumorskih matičnih celicah smo preverili udeleženost zaviralcev katepsinov B in X pri endocitozi z uporabo njunih specifičnih zaviralcev nitroksolina in spojine Z9. Pokazali smo, da je endocitoza transferina v tumorskih matičnih celicah značilno manjša kot pri diferenciranih tumorskih celicah. Z uporabo zaviralcev smo potrdili udeleženost katepsina B pri endocitozi tumorskih matičnih celic in pokazali, da ima zaviranje katepsina X s spojino Z9 le manjši učinek na endocitozo tumorskih matičnih celic. Pokazali smo, da je sposobnost endocitoze pri tumorskih matičnih celicah ob zmanjšani aktivnosti katepsina B povečana, kot je to značilno za diferencirane tumorske celice. Z nasičenjem receptorjev za endocitozo s holotransferinom smo tudi potrdili, da v testiranih tumorskih matičnih celicah poteka z receptorji posredovana endocitoza transferina.

Language:Slovenian
Keywords:Rak, tumorske matične celice, endocitoza, katepsin B, katepsin X, nizko molekularni zaviralci
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2024
PID:20.500.12556/RUL-164715 This link opens in a new window
Publication date in RUL:08.11.2024
Views:104
Downloads:18
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Secondary language

Language:English
Title:The influence of cathepsin B and X inhibitors on the cancer stem cell endocytosis
Abstract:
Breast cancer is the second deadliest disease among women. Thanks to screening programs and advances in diagnostics and treatment, mortality rates have declined in recent decades. However, cancer stem cells remain the major challenge in effective treatment. Due to their unique abilities of self-renewal and differentiation, these cells are resistant to most current therapies, often persisting post-treatment, where they proliferate, differentiate, and metastasize, leading to reoccurrence. New treatments targeting these cells are needed. Cysteine cathepsins B and X, which are involved in all stages of cancer progression, show increased expression and activity in cancer stem cells. In this thesis, cancer stem cells were isolated from MDA-MB-231, MCF-7, and MCF-10A neoT cell lines based on their sphere-forming abilities. Secondary tumour spheres were prepared to increase purity. The role of cathepsin B and X inhibitors in endocytosis was assessed using nitroxoline and compound Z9. We showed that transferrin endocytosis is significantly lower in cancer stem cells than in differentiated cancer cells. Inhibition confirmed cathepsin B’s involvement in endocytosis, while cathepsin X inhibition had a lower effect. Reduced cathepsin B activity increased endocytosis capacity in cancer stem cells to levels typical of differentiated cells. Additionally, receptor-mediated transferrin endocytosis was confirmed in cancer stem cells by holotransferrin saturation.

Keywords:Cancer, cancer stem cells, endocytosis, cathepsin B, cathepsin X, small molecular inhibitors

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