VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization

Hypoxia-induced VEGF governs both physiological retinal vascular development and pathological retinal neovascularization. In the current paper, the mechanisms of physiological and pathological neovascularization are compared and contrasted. During pathological neovascularization, both the absolute a...

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Autores principales: Ishida, Susumu, Usui, Tomohiko, Yamashiro, Kenji, Kaji, Yuichi, Amano, Shiro, Ogura, Yuichiro, Hida, Tetsuo, Oguchi, Yoshihisa, Ambati, Jayakrishna, Miller, Joan W., Gragoudas, Evangelos S., Ng, Yin-Shan, D'Amore, Patricia A., Shima, David T., Adamis, Anthony P.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2003
Materias:
Brief Definitive Report
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2194095/
https://www.ncbi.nlm.nih.gov/pubmed/12900522
http://dx.doi.org/10.1084/jem.20022027
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author Ishida, Susumu
Usui, Tomohiko
Yamashiro, Kenji
Kaji, Yuichi
Amano, Shiro
Ogura, Yuichiro
Hida, Tetsuo
Oguchi, Yoshihisa
Ambati, Jayakrishna
Miller, Joan W.
Gragoudas, Evangelos S.
Ng, Yin-Shan
D'Amore, Patricia A.
Shima, David T.
Adamis, Anthony P.
author_facet Ishida, Susumu
Usui, Tomohiko
Yamashiro, Kenji
Kaji, Yuichi
Amano, Shiro
Ogura, Yuichiro
Hida, Tetsuo
Oguchi, Yoshihisa
Ambati, Jayakrishna
Miller, Joan W.
Gragoudas, Evangelos S.
Ng, Yin-Shan
D'Amore, Patricia A.
Shima, David T.
Adamis, Anthony P.
author_sort Ishida, Susumu
collection PubMed
description Hypoxia-induced VEGF governs both physiological retinal vascular development and pathological retinal neovascularization. In the current paper, the mechanisms of physiological and pathological neovascularization are compared and contrasted. During pathological neovascularization, both the absolute and relative expression levels for VEGF(164) increased to a greater degree than during physiological neovascularization. Furthermore, extensive leukocyte adhesion was observed at the leading edge of pathological, but not physiological, neovascularization. When a VEGF(164)-specific neutralizing aptamer was administered, it potently suppressed the leukocyte adhesion and pathological neovascularization, whereas it had little or no effect on physiological neovascularization. In parallel experiments, genetically altered VEGF(164)-deficient (VEGF(120/188)) mice exhibited no difference in physiological neovascularization when compared with wild-type (VEGF(+/+)) controls. In contrast, administration of a VEGFR-1/Fc fusion protein, which blocks all VEGF isoforms, led to significant suppression of both pathological and physiological neovascularization. In addition, the targeted inactivation of monocyte lineage cells with clodronate-liposomes led to the suppression of pathological neovascularization. Conversely, the blockade of T lymphocyte–mediated immune responses with an anti-CD2 antibody exacerbated pathological neovascularization. These data highlight important molecular and cellular differences between physiological and pathological retinal neovascularization. During pathological neovascularization, VEGF(164) selectively induces inflammation and cellular immunity. These processes provide positive and negative angiogenic regulation, respectively. Together, new therapeutic approaches for selectively targeting pathological, but not physiological, retinal neovascularization are outlined.
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spelling pubmed-21940952008-04-11 VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization Ishida, Susumu Usui, Tomohiko Yamashiro, Kenji Kaji, Yuichi Amano, Shiro Ogura, Yuichiro Hida, Tetsuo Oguchi, Yoshihisa Ambati, Jayakrishna Miller, Joan W. Gragoudas, Evangelos S. Ng, Yin-Shan D'Amore, Patricia A. Shima, David T. Adamis, Anthony P. J Exp Med Brief Definitive Report Hypoxia-induced VEGF governs both physiological retinal vascular development and pathological retinal neovascularization. In the current paper, the mechanisms of physiological and pathological neovascularization are compared and contrasted. During pathological neovascularization, both the absolute and relative expression levels for VEGF(164) increased to a greater degree than during physiological neovascularization. Furthermore, extensive leukocyte adhesion was observed at the leading edge of pathological, but not physiological, neovascularization. When a VEGF(164)-specific neutralizing aptamer was administered, it potently suppressed the leukocyte adhesion and pathological neovascularization, whereas it had little or no effect on physiological neovascularization. In parallel experiments, genetically altered VEGF(164)-deficient (VEGF(120/188)) mice exhibited no difference in physiological neovascularization when compared with wild-type (VEGF(+/+)) controls. In contrast, administration of a VEGFR-1/Fc fusion protein, which blocks all VEGF isoforms, led to significant suppression of both pathological and physiological neovascularization. In addition, the targeted inactivation of monocyte lineage cells with clodronate-liposomes led to the suppression of pathological neovascularization. Conversely, the blockade of T lymphocyte–mediated immune responses with an anti-CD2 antibody exacerbated pathological neovascularization. These data highlight important molecular and cellular differences between physiological and pathological retinal neovascularization. During pathological neovascularization, VEGF(164) selectively induces inflammation and cellular immunity. These processes provide positive and negative angiogenic regulation, respectively. Together, new therapeutic approaches for selectively targeting pathological, but not physiological, retinal neovascularization are outlined. The Rockefeller University Press 2003-08-04 /pmc/articles/PMC2194095/ /pubmed/12900522 http://dx.doi.org/10.1084/jem.20022027 Text en Copyright © 2003, The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Brief Definitive Report
Ishida, Susumu
Usui, Tomohiko
Yamashiro, Kenji
Kaji, Yuichi
Amano, Shiro
Ogura, Yuichiro
Hida, Tetsuo
Oguchi, Yoshihisa
Ambati, Jayakrishna
Miller, Joan W.
Gragoudas, Evangelos S.
Ng, Yin-Shan
D'Amore, Patricia A.
Shima, David T.
Adamis, Anthony P.
VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization
title VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization
title_full VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization
title_fullStr VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization
title_full_unstemmed VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization
title_short VEGF(164)-mediated Inflammation Is Required for Pathological, but Not Physiological, Ischemia-induced Retinal Neovascularization
title_sort vegf(164)-mediated inflammation is required for pathological, but not physiological, ischemia-induced retinal neovascularization
topic Brief Definitive Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2194095/
https://www.ncbi.nlm.nih.gov/pubmed/12900522
http://dx.doi.org/10.1084/jem.20022027
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