ADAM17 silencing in mouse colon carcinoma cells : the effect on tumoricidal cytokines and angiogenesis

2012
journal article
article
30
dc.abstract.enADAM17 (a disintegrin and metalloprotease 17) is a major sheddase for numerous growth factors, cytokines, receptors, and cell adhesion molecules and is often overexpressed in malignant cells. It is generally accepted that ADAM17 promotes tumor development via activating growth factors from the EGF family, thus facilitating autocrine stimulation of tumor cell proliferation and migration. Here we show, using MC38CEA murine colon carcinoma model, that ADAM17 also regulates tumor angiogenesis and cytokine profile. When ADAM17 was silenced in MC38CEA cells, in vivo tumor growth and in vitro cell motility were significantly diminished, but no effect was seen on in vitro cell proliferation. ADAM17-silencing was accompanied by decreased in vitro expression of vascular endothelial growth factor-A and matrix metalloprotease-9, which was consistent with the limited angiogenesis and slower growth seen in ADAM17-silenced tumors. Among the growth factors susceptible to shedding by ADAM17, neuregulin-1 was the only candidate to mediate the effects of ADAM17 on MC38CEA motility and tumor angiogenesis. Concentrations of TNF and IFNγ, cytokines that synergistically induced proapoptotic effects on MC38CEA cells, were significantly elevated in the lysates of ADAM17-silenced tumors compared to mock transfected controls, suggesting a possible role for ADAM17 in host immune suppression. These results introduce new, complex roles of ADAM17 in tumor progression, including its impact on the anti-tumor immune response.pl
dc.affiliationWydział Biochemii, Biofizyki i Biotechnologii : Zakład Biochemii Komórkipl
dc.affiliationWydział Biochemii, Biofizyki i Biotechnologii : Zakład Biologii Komórkipl
dc.contributor.authorDas, Sudiptapl
dc.contributor.authorCzarnek, Maria - 177708 pl
dc.contributor.authorBzowska, Monika - 127507 pl
dc.contributor.authorMężyk-Kopeć, Renata - 130487 pl
dc.contributor.authorStalińska, Krystyna - 132053 pl
dc.contributor.authorWyroba, Barbara - 170163 pl
dc.contributor.authorSroka, Jolanta - 132030 pl
dc.contributor.authorJucha, Jarosław - 110038 pl
dc.contributor.authorDeneka, Dawidpl
dc.contributor.authorStokłosa, Paulinapl
dc.contributor.authorOgonek, Justynapl
dc.contributor.authorSwartz, Melody A.pl
dc.contributor.authorMadeja, Zbigniew - 130173 pl
dc.contributor.authorBereta, Joanna - 127287 pl
dc.date.accessioned2016-05-20T12:15:21Z
dc.date.available2016-05-20T12:15:21Z
dc.date.issued2012pl
dc.date.openaccess0
dc.description.accesstimew momencie opublikowania
dc.description.number12pl
dc.description.versionostateczna wersja wydawcy
dc.description.volume7pl
dc.identifier.articleide50791pl
dc.identifier.doi10.1371/journal.pone.0050791pl
dc.identifier.eissn1932-6203pl
dc.identifier.projectROD UJ / Ppl
dc.identifier.urihttp://ruj.uj.edu.pl/xmlui/handle/item/26652
dc.languageengpl
dc.language.containerengpl
dc.rightsUdzielam licencji. Uznanie autorstwa 4.0 Międzynarodowa*
dc.rights.licenceCC-BY
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/legalcode.pl*
dc.share.typeotwarte czasopismo
dc.subtypeArticlepl
dc.titleADAM17 silencing in mouse colon carcinoma cells : the effect on tumoricidal cytokines and angiogenesispl
dc.title.journalPLoS ONEpl
dc.typeJournalArticlepl
dspace.entity.typePublication
dc.abstract.enpl
ADAM17 (a disintegrin and metalloprotease 17) is a major sheddase for numerous growth factors, cytokines, receptors, and cell adhesion molecules and is often overexpressed in malignant cells. It is generally accepted that ADAM17 promotes tumor development via activating growth factors from the EGF family, thus facilitating autocrine stimulation of tumor cell proliferation and migration. Here we show, using MC38CEA murine colon carcinoma model, that ADAM17 also regulates tumor angiogenesis and cytokine profile. When ADAM17 was silenced in MC38CEA cells, in vivo tumor growth and in vitro cell motility were significantly diminished, but no effect was seen on in vitro cell proliferation. ADAM17-silencing was accompanied by decreased in vitro expression of vascular endothelial growth factor-A and matrix metalloprotease-9, which was consistent with the limited angiogenesis and slower growth seen in ADAM17-silenced tumors. Among the growth factors susceptible to shedding by ADAM17, neuregulin-1 was the only candidate to mediate the effects of ADAM17 on MC38CEA motility and tumor angiogenesis. Concentrations of TNF and IFNγ, cytokines that synergistically induced proapoptotic effects on MC38CEA cells, were significantly elevated in the lysates of ADAM17-silenced tumors compared to mock transfected controls, suggesting a possible role for ADAM17 in host immune suppression. These results introduce new, complex roles of ADAM17 in tumor progression, including its impact on the anti-tumor immune response.
dc.affiliationpl
Wydział Biochemii, Biofizyki i Biotechnologii : Zakład Biochemii Komórki
dc.affiliationpl
Wydział Biochemii, Biofizyki i Biotechnologii : Zakład Biologii Komórki
dc.contributor.authorpl
Das, Sudipta
dc.contributor.authorpl
Czarnek, Maria - 177708
dc.contributor.authorpl
Bzowska, Monika - 127507
dc.contributor.authorpl
Mężyk-Kopeć, Renata - 130487
dc.contributor.authorpl
Stalińska, Krystyna - 132053
dc.contributor.authorpl
Wyroba, Barbara - 170163
dc.contributor.authorpl
Sroka, Jolanta - 132030
dc.contributor.authorpl
Jucha, Jarosław - 110038
dc.contributor.authorpl
Deneka, Dawid
dc.contributor.authorpl
Stokłosa, Paulina
dc.contributor.authorpl
Ogonek, Justyna
dc.contributor.authorpl
Swartz, Melody A.
dc.contributor.authorpl
Madeja, Zbigniew - 130173
dc.contributor.authorpl
Bereta, Joanna - 127287
dc.date.accessioned
2016-05-20T12:15:21Z
dc.date.available
2016-05-20T12:15:21Z
dc.date.issuedpl
2012
dc.date.openaccess
0
dc.description.accesstime
w momencie opublikowania
dc.description.numberpl
12
dc.description.version
ostateczna wersja wydawcy
dc.description.volumepl
7
dc.identifier.articleidpl
e50791
dc.identifier.doipl
10.1371/journal.pone.0050791
dc.identifier.eissnpl
1932-6203
dc.identifier.projectpl
ROD UJ / P
dc.identifier.uri
http://ruj.uj.edu.pl/xmlui/handle/item/26652
dc.languagepl
eng
dc.language.containerpl
eng
dc.rights*
Udzielam licencji. Uznanie autorstwa 4.0 Międzynarodowa
dc.rights.licence
CC-BY
dc.rights.uri*
http://creativecommons.org/licenses/by/4.0/legalcode.pl
dc.share.type
otwarte czasopismo
dc.subtypepl
Article
dc.titlepl
ADAM17 silencing in mouse colon carcinoma cells : the effect on tumoricidal cytokines and angiogenesis
dc.title.journalpl
PLoS ONE
dc.typepl
JournalArticle
dspace.entity.type
Publication
Affiliations

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