VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A

BACKGROUND: Different isoforms of VEGF-A (mainly VEGF(121), VEGF(165 )and VEGF(189)) have been shown to display particular angiogenic properties in the generation of a functional tumor vasculature. Recently, a novel class of VEGF-A isoforms, designated as VEGF(xxx)b, generated through alternative sp...

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Autores principales: Catena, Raúl, Larzabal, Leyre, Larrayoz, Marta, Molina, Eva, Hermida, Jose, Agorreta, Jackeline, Montes, Ramon, Pio, Ruben, Montuenga, Luis M, Calvo, Alfonso
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3022671/
https://www.ncbi.nlm.nih.gov/pubmed/21194429
http://dx.doi.org/10.1186/1476-4598-9-320
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author Catena, Raúl
Larzabal, Leyre
Larrayoz, Marta
Molina, Eva
Hermida, Jose
Agorreta, Jackeline
Montes, Ramon
Pio, Ruben
Montuenga, Luis M
Calvo, Alfonso
author_facet Catena, Raúl
Larzabal, Leyre
Larrayoz, Marta
Molina, Eva
Hermida, Jose
Agorreta, Jackeline
Montes, Ramon
Pio, Ruben
Montuenga, Luis M
Calvo, Alfonso
author_sort Catena, Raúl
collection PubMed
description BACKGROUND: Different isoforms of VEGF-A (mainly VEGF(121), VEGF(165 )and VEGF(189)) have been shown to display particular angiogenic properties in the generation of a functional tumor vasculature. Recently, a novel class of VEGF-A isoforms, designated as VEGF(xxx)b, generated through alternative splicing, have been described. Previous studies have suggested that these isoforms may inhibit angiogenesis. In the present work we have produced recombinant VEGF(121/165)b proteins in the yeast Pichia pastoris and constructed vectors to overexpress these isoforms and assess their angiogenic potential. RESULTS: Recombinant VEGF(121/165)b proteins generated either in yeasts or mammalian cells activated VEGFR2 and its downstream effector ERK1/2, although to a lesser extent than VEGF(165). Furthermore, treatment of endothelial cells with VEGF(121/165)b increased cell proliferation compared to untreated cells, although such stimulation was lower than that induced by VEGF(165). Moreover, in vivo angiogenesis assays confirmed angiogenesis stimulation by VEGF(121/165)b isoforms. A549 and PC-3 cells overexpressing VEGF(121)b or VEGF(165)b (or carrying the PCDNA3.1 empty vector, as control) and xenotransplanted into nude mice showed increased tumor volume and angiogenesis compared to controls. To assess whether the VEGF(xxx)b isoforms are differentially expressed in tumors compared to healthy tissues, immunohistochemical analysis was conducted on a breast cancer tissue microarray. A significant increase (p < 0.05) in both VEGF(xxx)b and total VEGF-A protein expression in infiltrating ductal carcinomas compared to normal breasts was observed. A positive significant correlation (r = 0.404, p = 0.033) between VEGF(xxx)b and total VEGF-A was found. CONCLUSIONS: Our results demonstrate that VEGF(121/165)b are not anti-angiogenic, but weakly angiogenic isoforms of VEGF-A. In addition, VEGF(xxx)b isoforms are up-regulated in breast cancer in comparison with non malignant breast tissues. These results are to be taken into account when considering a possible use of VEGF(121/165)b-based therapies in patients.
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spelling pubmed-30226712011-01-19 VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A Catena, Raúl Larzabal, Leyre Larrayoz, Marta Molina, Eva Hermida, Jose Agorreta, Jackeline Montes, Ramon Pio, Ruben Montuenga, Luis M Calvo, Alfonso Mol Cancer Research BACKGROUND: Different isoforms of VEGF-A (mainly VEGF(121), VEGF(165 )and VEGF(189)) have been shown to display particular angiogenic properties in the generation of a functional tumor vasculature. Recently, a novel class of VEGF-A isoforms, designated as VEGF(xxx)b, generated through alternative splicing, have been described. Previous studies have suggested that these isoforms may inhibit angiogenesis. In the present work we have produced recombinant VEGF(121/165)b proteins in the yeast Pichia pastoris and constructed vectors to overexpress these isoforms and assess their angiogenic potential. RESULTS: Recombinant VEGF(121/165)b proteins generated either in yeasts or mammalian cells activated VEGFR2 and its downstream effector ERK1/2, although to a lesser extent than VEGF(165). Furthermore, treatment of endothelial cells with VEGF(121/165)b increased cell proliferation compared to untreated cells, although such stimulation was lower than that induced by VEGF(165). Moreover, in vivo angiogenesis assays confirmed angiogenesis stimulation by VEGF(121/165)b isoforms. A549 and PC-3 cells overexpressing VEGF(121)b or VEGF(165)b (or carrying the PCDNA3.1 empty vector, as control) and xenotransplanted into nude mice showed increased tumor volume and angiogenesis compared to controls. To assess whether the VEGF(xxx)b isoforms are differentially expressed in tumors compared to healthy tissues, immunohistochemical analysis was conducted on a breast cancer tissue microarray. A significant increase (p < 0.05) in both VEGF(xxx)b and total VEGF-A protein expression in infiltrating ductal carcinomas compared to normal breasts was observed. A positive significant correlation (r = 0.404, p = 0.033) between VEGF(xxx)b and total VEGF-A was found. CONCLUSIONS: Our results demonstrate that VEGF(121/165)b are not anti-angiogenic, but weakly angiogenic isoforms of VEGF-A. In addition, VEGF(xxx)b isoforms are up-regulated in breast cancer in comparison with non malignant breast tissues. These results are to be taken into account when considering a possible use of VEGF(121/165)b-based therapies in patients. BioMed Central 2010-12-31 /pmc/articles/PMC3022671/ /pubmed/21194429 http://dx.doi.org/10.1186/1476-4598-9-320 Text en Copyright ©2010 Catena et al; licensee BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (<url>http://creativecommons.org/licenses/by/2.0</url>), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Catena, Raúl
Larzabal, Leyre
Larrayoz, Marta
Molina, Eva
Hermida, Jose
Agorreta, Jackeline
Montes, Ramon
Pio, Ruben
Montuenga, Luis M
Calvo, Alfonso
VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A
title VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A
title_full VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A
title_fullStr VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A
title_full_unstemmed VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A
title_short VEGF(121)b and VEGF(165)b are weakly angiogenic isoforms of VEGF-A
title_sort vegf(121)b and vegf(165)b are weakly angiogenic isoforms of vegf-a
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3022671/
https://www.ncbi.nlm.nih.gov/pubmed/21194429
http://dx.doi.org/10.1186/1476-4598-9-320
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