
<ns0:uwmetadata xmlns:ns0="http://phaidra.univie.ac.at/XML/metadata/V1.0" xmlns:ns1="http://phaidra.univie.ac.at/XML/metadata/lom/V1.0" xmlns:ns10="http://phaidra.univie.ac.at/XML/metadata/provenience/V1.0" xmlns:ns11="http://phaidra.univie.ac.at/XML/metadata/provenience/V1.0/entity" xmlns:ns12="http://phaidra.univie.ac.at/XML/metadata/digitalbook/V1.0" xmlns:ns13="http://phaidra.univie.ac.at/XML/metadata/etheses/V1.0" xmlns:ns2="http://phaidra.univie.ac.at/XML/metadata/extended/V1.0" xmlns:ns3="http://phaidra.univie.ac.at/XML/metadata/lom/V1.0/entity" xmlns:ns4="http://phaidra.univie.ac.at/XML/metadata/lom/V1.0/requirement" xmlns:ns5="http://phaidra.univie.ac.at/XML/metadata/lom/V1.0/educational" xmlns:ns6="http://phaidra.univie.ac.at/XML/metadata/lom/V1.0/annotation" xmlns:ns7="http://phaidra.univie.ac.at/XML/metadata/lom/V1.0/classification" xmlns:ns8="http://phaidra.univie.ac.at/XML/metadata/lom/V1.0/organization" xmlns:ns9="http://phaidra.univie.ac.at/XML/metadata/histkult/V1.0">
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    <ns1:identifier>o:755</ns1:identifier>
    <ns1:title language="sr">Uticaj signalnog puta IL-33/ST2 na razvoj nekroze kod karcinoma dojke</ns1:title>
    <ns2:alt_title language="sr">The role of IL-33/ST2 signaling pathway in development of breast carcinoma necrosis : doctoral dissertation</ns2:alt_title>
    <ns1:language>sr</ns1:language>
    <ns1:description language="sr">Interleukin-33 (IL-33)/IL-33 receptor (IL-33R, IL-RL1, ST2) signalni put promoviše
rast tumora i razvoj metastaza inhibicijom antitumorskog imunskog odgovora. IL-33 je protein sa anti- i proinflamatornom ulogom koji funkcioniše kao transkripcioni
faktor i klasičan citokin sa ulogom alarmina. Nekrotične ćelije sekretuju
imunoregulatorne citokina uključujući IL-33 koji je član IL-1 familije citokina.
Prethodne studije sugerišu da IL-33 promoviše ekspresiju i oslobađanje vaskularnog
endotelnog faktora rasta (VEGF) u mastocitima i ukazuju na njegovu proangiogenu ulogu
aktivacijom endotelnih ćelija preko IL-33R. Međutim, značaj aktivacije IL-33/IL-33R
signalnog puta u angiogenezi i tumorskoj nekrozi nije u potpunosti jasna.
Cilj naše studije je bio da se ispita uloga signalnog puta IL-33/IL-33R u tumorskoj
nekrozi i angiogenezi karcinoma dojke.
Delecija gena za IL-33R u BALB/c miševa pojačava tumorsku nekrozu u isporava rast
tumora u eksperimentalnom modelu 4T1 karcinoma dojke što je povezano sa smanjenom
ekspresijom vaskularnog endotelnog faktora rasta i IL-33 u ćelijama tumora dojke.
Ekspresija IL-33 u ćelijama karcinoma dojke raste tokom vremena u IL-33R+/+ ali ne i u
IL-33R-/-. Rezultat ukazuje na mehanizam pozitivne povratne sprege IL-33/IL-33R osovine.
Analizirali smo ekspresije IL-33. IL-33R, i VEGF.a, kao i mikrovaskularnu gustinu
(MVD) u tumorima 40 pacijenkinja sa karcinomom dojke sa prisutnom ili odsutnom
nekrozom u tkivu tumora. Detektovali smo značajno veću ekspresiju IL-33. IL-33R i
VEGF-a u tkivu karcinoma dojke bez detektabilne nekroze. Ekspresije IL-33 i IL-33R
koreliraju sa ekspresijom VEGF-a u tumorskim ćelijama. Takođe, ekspresija VEGF je
bila u pozitivnoj korelaciji sa MVD u perinekrotičnom rubu tumora.
IL-33 poput IL-1β pokauje proangiogenu ulogu i kontroliše produkciju VEGF-a. IL-1β
pojačava ekspresiju VEGF-a i njegovih receptora na endotelnim ćelijama a zajedno sa
VEGF-om promoviše tumorsku angiogenezu. Kao i IL-1, IL-33 aktivira IL-1R3 (IL-1RAcP)
ukazujuć da inhibicija ovog protein primenom anti-IL-1R3 antitela inhibira
angiogenezu tumora i pojačava tumorsku nekrozu u tkivu carcinoma dojke usled gubitka
vaskularne podpore. Na osnovu ovih rezultata smatramo da IL-33 oslobođen iz
nekrotičnih ćelija facilitira ekspresiju VEGF-a u okolnim tumorskim ćelijama
promovišući angiogenezu što je potvrđeno većom MVD u perinekrotičnoj zoni humanog
carcinoma dojke. Naši rezultati ukazuju da IL-33/IL-33R signalni put igra važnu ulogu
u rastu tumora pojačavanjem ekspresije proangiogenog VEGF-a i inhibicijom tumorske
nekroze. U dodatku na ranija istraživanja, naši rezultati ukazuju na suprotnu ulogu
intracelularnog i sekretovanog IL-33. Naša studija pokazuje dodatni mehanizam kojim
IL-33/IL-33R osovina učestvuje u karcinogenezi i daje racionalno objašnjenje za
potencijalnu blokadu IL-33 kao terapijskog modaliteta u lečenju humanog karcinoma
dojke.</ns1:description>
    <ns1:description language="en">Interleukin-33 (IL-33)/IL-33 receptor (IL-33R, IL-RL1, ST2) signaling pathway promotes
mammary cancer growth and metastasis by inhibiting anti-tumor immunity. IL-33 is dual
function protein with roles as a nuclear factor and a classical cytokine and functions as a
prototypic „alarmin”. Necrotic cells release immunoregulatory cytokines, including IL-33, a
member of the IL-1 family of cytokines. Previous studies suggest that IL-33 directly facilitated
vascular endothelial growth factor (VEGF) expression and secretion in primed mast and showed
proangiogenic role of IL-33 by inducing endothelial proangiogenic activity via IL-33R
expressed on endothelial cells.However, the role of IL-33/IL-33R axis in neoangiogenesis and
tumor necrosis is not elucidated.
Therefore, the aim of this study was to investigate the role of IL-33/IL-33R axis in mammary
tumor necrosis and angiogenesis.
Deletion of IL-33R gene in BALB/c mice enhanced tumor necrosis and attenuated tumor growth
in 4T1 breast cancer model, which was associated with markedly decreased expression of VEGF
and IL-33 in mammary tumor cells. IL-33 expression in mammary tumor cells significantly
increased over time in IL-33R+
/+ mice, but not in IL-33R-/- mice the findings that reflect positive
feedback mechanism in IL-33/IL-33R axis We next analyzed IL-33, IL-33R and VEGF
expression and microvascular density (MVD) in breast tumors from 40 female patients with
absent or present tumor necrosis. We found significantly higher expression of IL-33, IL-33R and
VEGF in breast cancer tissues with absent tumor necrosis. Both, IL-33 and IL-33R expression
correlated with VEGF expression in tumor cells. Further, VEGF expression positively correlated
with MVD in perinecrotic zone.
IL-33 is very much like IL-1 in that both IL-1β and IL-33 are proangiogenic and control the
production of VEGF. IL-1β increases expression of VEGF and its receptors on endothelial cells
and acts together with VEGF in promoting tumor mediated angiogenesis. Thus, the
neutralization of IL-1β reduced tumor growth and the tumor-induced angiogenesis. As IL-1 and
IL- 33 both use IL-1R3 (IL-1RAcP), it may be speculated that anti-IL-1R3 antibodies may
reduce angiogenesis and increase tumor necrosis in breast cancer due to loss of vascular supply.
On the basis of these observations we suggest that IL-33 released by necrotic cells may facilitate
VEGF expression on nearby tumor cells, which could lead to enhanced angiogenesis as
demonstrated by high-grade MVD in perinecrotic zone in human breast cancer tissue. Taking
together, our data indicate that IL-33/IL-33R pathway is critically involved in mammary tumor
growth by facilitating expression of pro-angiogenic VEGF in tumor cells and attenuating tumor
necrosis. Additionally, results indicate oposite functions of intracellular and secreted IL-33.
Thus, this study revealed an additional mechanism by which IL-33/IL-33R pathway may be
involved in tumorigenesis and provide rationale for blocking IL-33 as a therapeutic modality in
human breast carcinoma.</ns1:description>
    <ns1:description language="sr"></ns1:description>
    <ns2:identifiers>
      <ns2:identifier>ID=523723925 ; D-3013</ns2:identifier>
    </ns2:identifiers>
    <ns2:identifiers>
      <ns2:resource>91552101</ns2:resource>
      <ns2:identifier>4630</ns2:identifier>
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    <ns2:identifiers>
      <ns2:resource>91552100</ns2:resource>
      <ns2:identifier>523723925</ns2:identifier>
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  <ns1:lifecycle>
    <ns1:upload_date>2017-02-28T10:35:09.053Z</ns1:upload_date>
    <ns1:status>45</ns1:status>
    <ns2:peer_reviewed>no</ns2:peer_reviewed>
    <ns1:contribute seq="0">
      <ns1:role>46</ns1:role>
      <ns1:ext_role>mentor</ns1:ext_role>
      <ns1:entity seq="0">
        <ns3:firstname> Miloš Z., 1977- </ns3:firstname>
        <ns3:lastname>Milosavljević</ns3:lastname>
      </ns1:entity>
      <ns1:date>2017</ns1:date>
    </ns1:contribute>
    <ns1:contribute seq="1">
      <ns1:role>63</ns1:role>
      <ns1:ext_role>mentor</ns1:ext_role>
      <ns1:entity seq="0">
        <ns3:firstname> Ivan. </ns3:firstname>
        <ns3:lastname>Jovanović</ns3:lastname>
      </ns1:entity>
      <ns1:date>2017</ns1:date>
    </ns1:contribute>
    <ns1:contribute seq="2">
      <ns1:role>63</ns1:role>
      <ns1:ext_role>član komisije</ns1:ext_role>
      <ns1:entity seq="0">
        <ns3:firstname> Miodrag. </ns3:firstname>
        <ns3:lastname>Lukić</ns3:lastname>
      </ns1:entity>
      <ns1:date>2017</ns1:date>
    </ns1:contribute>
    <ns1:contribute seq="3">
      <ns1:role>63</ns1:role>
      <ns1:ext_role>član komisije</ns1:ext_role>
      <ns1:entity seq="0">
        <ns3:firstname> Slavica, 1957- </ns3:firstname>
        <ns3:lastname>Knežević Ušaj</ns3:lastname>
      </ns1:entity>
      <ns1:date>2017</ns1:date>
    </ns1:contribute>
    <ns1:contribute seq="4">
      <ns1:role>63</ns1:role>
      <ns1:ext_role>član komisije</ns1:ext_role>
      <ns1:entity seq="0">
        <ns3:firstname> Gordana, 1976- </ns3:firstname>
        <ns3:lastname>Radosavljević</ns3:lastname>
      </ns1:entity>
      <ns1:date>2017</ns1:date>
    </ns1:contribute>
  </ns1:lifecycle>
  <ns1:technical>
    <ns1:format>273 lista</ns1:format>
    <ns1:size>6491363</ns1:size>
    <ns1:location>http://phaidrabg.bg.ac.rs/o:755</ns1:location>
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  <ns1:rights>
    <ns1:cost>no</ns1:cost>
    <ns1:copyright>yes</ns1:copyright>
    <ns1:license>2</ns1:license>
  </ns1:rights>
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    <ns6:annotations>
      <ns6:date>2017-02-28T10:35:09.320Z</ns6:date>
    </ns6:annotations>
  </ns1:annotation>
  <ns1:classification>
    <ns1:purpose>70</ns1:purpose>
    <ns7:keyword language="sr" seq="1">IL-33, IL-33R, karcinom dojke,neoangiogeneza, nekroza</ns7:keyword>
    <ns7:keyword language="sr" seq="1">IL-33, IL-33R, breast neoplasm,neoangiogenesis, necrosis</ns7:keyword>
    <ns7:keyword language="sr" seq="1">616.18-006(043.3)</ns7:keyword>
    <ns7:keyword language="sr" seq="1">Dojka - Karcinom</ns7:keyword>
  </ns1:classification>
  <ns1:organization>
    <ns8:hoschtyp>1738</ns8:hoschtyp>
    <ns8:orgassignment>
      <ns8:faculty>34A05</ns8:faculty>
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  <ns12:digitalbook>
    <ns12:releaseyear>2017</ns12:releaseyear>
  </ns12:digitalbook>
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