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Vpliv cistatina C in stefina B na prisotnost makrofagov pri mišjem modelu raka mlečne žleze MMTV-PyMT
ID Senica, Jerneja (Author), ID Turk, Boris (Mentor) More about this mentor... This link opens in a new window

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Abstract
Proteaze so encimi, ki so pomembno vključeni v številne biološke procese v celicah. S svojim delovanjem vplivajo na aktivnosti drugih proteinov, zato je nadvse pomembna njihova ustrezna regulacija. Med proteaze, ki za svoje delovanje potrebujejo reducirajoče okolje in jih primarno najdemo v lizosomih, sodijo cisteinski katepsini. Glavni inhibitorji delovanja cisteinskih katepsinov pa so cistatini, med katerimi sta ključna inhibitorja cistatin C in stefin B. Cistatini s svojim delovanjem regulirajo prekomerno aktivnost cisteinskih katepsinov. Oboji imajo pomemben vpliv na številna bolezenska stanja, tako imajo pomembno vlogo tudi pri napredovanja raka. Vloga cistatinov pa ni samo inhibicija cisteinskih katepsinov, študije so namreč pokazale, da cistatini pomembno vplivajo tudi na druge molekularne poti v celici, vključno s proliferacijo in diferenciacijo. Rak mlečne žleze oziroma rak dojke je eno izmed rakavih obolenj, ki je najbolj razširjeno med ženskami po vsem svetu. Zaradi velike podobnosti med mlečno žlezo pri človeku in miši študije bolezni potekajo na različnih transgenih mišjih modelih adenokarcinoma mlečne žleze, kot je MMTV-PyMT. Pomembno vlogo pri razvoju raka in nastanku metastaz ima tumorsko mikrookolje in celice v njem, predvsem makrofagi. V okviru magistrske naloge smo želeli preučiti vpliv cistatina C in stefina B na razširjenost makrofagov na mišjem modelu raka mlečne žleze MMTV-PyMT in na mišjih MMTV-PyMT modelih z utišanima genoma za cistatin C in stefin B. S tem smo želeli ovrednotiti njun vpliv na napredovanje raka. Rezine mišjih tumorjev smo barvali s F4-80 primarnimi protitelesi in substratnim sistemom DAB in jih opazovali pod mikroskopom. Ugotovili smo, da je najmanjše število makrofagov prisotno pri transgenih miših z utišanima genoma za oba cistatina. Na podlagi tega smo sklepali, da oba pomembno pripomoreta k napredovanju raka, vendar njuna točna vloga v teh procesih še ni opredeljena.

Language:Slovenian
Keywords:cistatin C, stefin B, rak mlečne žleze, MMTV-PyMT miši, makrofagi
Work type:Master's thesis/paper
Typology:2.09 - Master's Thesis
Organization:FKKT - Faculty of Chemistry and Chemical Technology
Year:2021
PID:20.500.12556/RUL-129654 This link opens in a new window
COBISS.SI-ID:76795651 This link opens in a new window
Publication date in RUL:06.09.2021
Views:1269
Downloads:60
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Secondary language

Language:English
Title:The role of cystatin C and stefin B on the presence of macrophages in the MMTV-PyMT mouse mammary cancer model
Abstract:
Proteases are enzymes which are significantly involved in many cellular processes. Proteases influence activity of many other proteins, so their adequate regulation is very important. Cysteine cathepsins are primarily found in lysosomes and require a reducing environment to function. The main inhibitors of cysteine cathepsins are cystatins, among which the key inhibitors are cystatin C and stefin B. Cystatins regulate excessive cysteine cathepsins activity. Both have a significant impact on the pathogenesis of cancer and other diseases. The role of cystatins, however, is not just to inhibit cysteine cathepsins activity. Several studies have suggested a significant effect of cystatins on other cellular pathways including proliferation and differentiation. Breast cancer is the most common cancer among women worldwide. The mouse has emerged as an important animal model for human breast cancer because the mammary glands of the two species are very similar. So research studies of human breast cancer are conducted on various transgenic mouse models of breast adenocarcinoma, such as MMTV-PyMT. In the master’s thesis we studied the effect of cystatin C and stefin B on the presence of macrophages in the MMTV-PyMT mouse mammary cancer model and in the transgenic MMTV-PyMT mouse mammary cancer models with knocked out genes for cystatin C and stefin B. We wanted to evaluate their impact on cancer progression. Tumour slices were stained with primary F4-80 antibodies and the DAB substrate system. We have found out that the lowest number of macrophages was present in transgenic mice with knocked out genes for both cystatins. We have concluded that both significantly contribute to cancer progression, but their exact role in the processes has not yet been defined.

Keywords:cystatin C, stefin B, mammary gland cancer, MMTV-PyMT mouse, macrophages

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