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dc.contributor.authorFLORES PEREZ, JOSE ALI-
dc.contributor.authorMARCHAT MARCHAU, LAURENCE ANIE-
dc.contributor.authorRODRIGUEZ CUEVAS, ARTURO SERGIO-
dc.contributor.authorBAUTISTA PIÑA, VERONICA-
dc.contributor.authorHIDALGO MIRANDA, ALFREDO-
dc.contributor.authorARECHAGA OCAMPO, ELENA-
dc.contributor.authorSIERRA MARTINEZ, MONICA-
dc.contributor.authorPALMA FLORES, CARLOS-
dc.contributor.authorFONSECA SANCHEZ, MIGUEL ANGEL-
dc.contributor.authorASTUDILLO DE LA VEGA, HORACIO-
dc.contributor.authorRUIZ GARCIA, ERIKA BETZABE-
dc.contributor.authorGONZALEZ BARRIOS, JUAN ANTONIO-
dc.contributor.authorPEREZ PLASENCIA, CARLOS GUADALUPE-
dc.contributor.authorSTREBER, MARIA-
dc.contributor.authorLOPEZ CAMARILLO, MARIO CESAR-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/330771">JOSE ALI FLORES PEREZ</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/19577">LAURENCE ANIE MARCHAT MARCHAU</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/15024">ARTURO SERGIO RODRIGUEZ CUEVAS</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/121473">ALFREDO HIDALGO MIRANDA</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/40111">ELENA ARECHAGA OCAMPO</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/306254">MONICA SIERRA MARTINEZ</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/215159">CARLOS PALMA FLORES</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/49800">MIGUEL ANGEL FONSECA SANCHEZ</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/31711">HORACIO ASTUDILLO DE LA VEGA</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/347106">ERIKA BETZABE RUIZ GARCIA</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/122257">JUAN ANTONIO GONZALEZ BARRIOS</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/201014">CARLOS GUADALUPE PEREZ PLASENCIA</dc:creator>-
dc.coverage.spatial<dc:creator id="info:eu-repo/dai/mx/cvu/31322">MARIO CESAR LOPEZ CAMARILLO</dc:creator>-
dc.coverage.temporal<dc:subject>info:eu-repo/classification/cti/3</dc:subject>-
dc.date.accessioned2021-06-01T23:56:44Z-
dc.date.available2021-06-01T23:56:44Z-
dc.date.issued2016-
dc.identifier.citationScientific Reports volume 6, Article number: 34504 (2016)en_US
dc.identifier.urihttp://ilitia.cua.uam.mx:8080/jspui/handle/123456789/850-
dc.description.abstractDeregulated expression of microRNAs has been associated with angiogenesis. Studying the miRNome of locally advanced breast tumors we unsuspectedly found a dramatically repression of miR-204, a small non-coding RNA with no previous involvement in tumor angiogenesis. Downregulation of miR-204 was confirmed in an independent cohort of patients and breast cancer cell lines. Gain-of-function analysis indicates that ectopic expression of miR-204 impairs cell proliferation, anchorage-independent growth, migration, invasion, and the formation of 3D capillary networks in vitro. Likewise, in vivo vascularization and angiogenesis were suppressed by miR-204 in a nu/nu mice model. Genome-wide profiling of MDA-MB-231 cells expressing miR-204 revealed changes in the expression of hundred cancer-related genes. Of these, we focused on the study of pro-angiogenic ANGPT1 and TGFβR2. Functional analysis using luciferase reporter and rescue assays confirmed that ANGPT1 and TGFβR2 are novel effectors downstream of miR-204. Accordingly, an inverse correlation between miR-204 and ANGPT1/TGFβR2 expression was found in breast tumors. Knockdown of TGFβR2, but not ANGPT1, impairs cell proliferation and migration whereas inhibition of both genes inhibits angiogenesis. Taken altogether, our findings reveal a novel role for miR-204/ANGPT1/TGFβR2 axis in tumor angiogenesis. We propose that therapeutic manipulation of miR-204 levels may represent a promising approach in breast cancer.en_US
dc.description.sponsorshipNature Publishing Groupen_US
dc.language.isoInglésen_US
dc.publisherReino Unido : Nature Publishing Groupen_US
dc.relation.haspart2045-2322-
dc.rightshttps://doi.org/10.1038/srep34504-
dc.rightshttps://www.nature.com/articles/srep34504.pdf-
dc.subjectCanceren_US
dc.subjectOncologíaen_US
dc.titleDual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast canceren_US
dc.typeArtículoen_US
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