Dual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast cancer

Ali Flores-Pérez; Laurence A. Marchat; Sergio Rodríguez-Cuevas; Verónica Bautista-Piña; Alfredo Hidalgo-Miranda; Elena Aréchaga Ocampo; Mónica Sierra Martínez; Carlos Palma-Flores; Miguel A. Fonseca-Sánchez; Horacio Astudillo-De La Vega; Erika Ruíz-García; Juan Antonio González-Barrios; Carlos Pérez-Plasencia; María L. Streber; César López-Camarillo

doi:10.1038/srep34504

Dual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast cancer

Ali Flores-Pérez, Laurence A. Marchat, Sergio Rodríguez-Cuevas, Verónica Bautista-Piña, Alfredo Hidalgo-Miranda, Elena Aréchaga Ocampo, Mónica Sierra Martínez, Carlos Palma-Flores, Miguel A. Fonseca-Sánchez, Horacio Astudillo-De La Vega, Erika Ruíz-García, Juan Antonio González-Barrios, Carlos Pérez-Plasencia, María L. Streber, César López-Camarillo

Escuela Nacional de Medicina y Homeopatía (ENMH)

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

59 Citas (Scopus)

Resumen

Deregulated 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.

Idioma original	Inglés
Número de artículo	34504
Publicación	Scientific Reports
Volumen	6
DOI	https://doi.org/10.1038/srep34504
Estado	Publicada - 5 oct. 2016

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Flores-Pérez, A., Marchat, L. A., Rodríguez-Cuevas, S., Bautista-Piña, V., Hidalgo-Miranda, A., Ocampo, E. A., Martínez, M. S., Palma-Flores, C., Fonseca-Sánchez, M. A., Astudillo-De La Vega, H., Ruíz-García, E., González-Barrios, J. A., Pérez-Plasencia, C., Streber, M. L., & López-Camarillo, C. (2016). Dual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast cancer. Scientific Reports, 6, Artículo 34504. https://doi.org/10.1038/srep34504

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title = "Dual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast cancer",

abstract = "Deregulated 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.",

author = "Ali Flores-P{\'e}rez and Marchat, {Laurence A.} and Sergio Rodr{\'i}guez-Cuevas and Ver{\'o}nica Bautista-Pi{\~n}a and Alfredo Hidalgo-Miranda and Ocampo, {Elena Ar{\'e}chaga} and Mart{\'i}nez, {M{\'o}nica Sierra} and Carlos Palma-Flores and Fonseca-S{\'a}nchez, {Miguel A.} and {Astudillo-De La Vega}, Horacio and Erika Ru{\'i}z-Garc{\'i}a and Gonz{\'a}lez-Barrios, {Juan Antonio} and Carlos P{\'e}rez-Plasencia and Streber, {Mar{\'i}a L.} and C{\'e}sar L{\'o}pez-Camarillo",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2016.",

year = "2016",

month = oct,

day = "5",

doi = "10.1038/srep34504",

language = "Ingl{\'e}s",

volume = "6",

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Flores-Pérez, A, Marchat, LA, Rodríguez-Cuevas, S, Bautista-Piña, V, Hidalgo-Miranda, A, Ocampo, EA, Martínez, MS, Palma-Flores, C, Fonseca-Sánchez, MA, Astudillo-De La Vega, H, Ruíz-García, E, González-Barrios, JA, Pérez-Plasencia, C, Streber, ML & López-Camarillo, C 2016, 'Dual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast cancer', Scientific Reports, vol. 6, 34504. https://doi.org/10.1038/srep34504

TY - JOUR

T1 - Dual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast cancer

AU - Flores-Pérez, Ali

AU - Marchat, Laurence A.

AU - Rodríguez-Cuevas, Sergio

AU - Bautista-Piña, Verónica

AU - Hidalgo-Miranda, Alfredo

AU - Ocampo, Elena Aréchaga

AU - Martínez, Mónica Sierra

AU - Palma-Flores, Carlos

AU - Fonseca-Sánchez, Miguel A.

AU - Astudillo-De La Vega, Horacio

AU - Ruíz-García, Erika

AU - González-Barrios, Juan Antonio

AU - Pérez-Plasencia, Carlos

AU - Streber, María L.

AU - López-Camarillo, César

PY - 2016/10/5

Y1 - 2016/10/5

N2 - Deregulated 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.

AB - Deregulated 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.

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U2 - 10.1038/srep34504

DO - 10.1038/srep34504

M3 - Artículo

C2 - 27703260

SN - 2045-2322

VL - 6

JO - Scientific Reports

JF - Scientific Reports

M1 - 34504

ER -

Dual targeting of ANGPT1 and TGFBR2 genes by miR-204 controls angiogenesis in breast cancer

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