2016
DOI: 10.1016/j.ebiom.2016.11.013
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IDO1 is an Integral Mediator of Inflammatory Neovascularization

Abstract: The immune tolerogenic effects of IDO1 (indoleamine 2,3-dioxygenase 1) have been well documented and genetic studies in mice have clearly established the significance of IDO1 in tumor promotion. Dichotomously, the primary inducer of IDO1, the inflammatory cytokine IFNγ (interferon-γ), is a key mediator of immune-based tumor suppression. One means by which IFNγ can exert an anti-cancer effect is by decreasing tumor neovascularization. We speculated that IDO1 might contribute to cancer promotion by countering th… Show more

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Cited by 81 publications
(94 citation statements)
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“…To test the idea that IDO1 is important for supporting neovascularization outside other possible confounding effects within the tumor microenvironment, studies were conducted in a mouse OIR (oxygen-induced retinopathy) model, a well established, reproducibly quantifiable surrogate system for studying neovascularization (Palmer et al , 2012; Stahl et al , 2012). As predicted, Ido1 −/− mice exhibited a significant reduction in OIR-induced retinal neovascularization relative to their WT counterparts (Mondal et al, 2016). Loss of the related IDO2 isoform had no demonstrable effect on OIR-induced retinal neovascularization, indicating that the effect is specific to IDO1 (Mondal et al, 2016).…”
Section: Ido1 In Inflammatory Programming: Pathogenic Neovascularizatsupporting
confidence: 69%
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“…To test the idea that IDO1 is important for supporting neovascularization outside other possible confounding effects within the tumor microenvironment, studies were conducted in a mouse OIR (oxygen-induced retinopathy) model, a well established, reproducibly quantifiable surrogate system for studying neovascularization (Palmer et al , 2012; Stahl et al , 2012). As predicted, Ido1 −/− mice exhibited a significant reduction in OIR-induced retinal neovascularization relative to their WT counterparts (Mondal et al, 2016). Loss of the related IDO2 isoform had no demonstrable effect on OIR-induced retinal neovascularization, indicating that the effect is specific to IDO1 (Mondal et al, 2016).…”
Section: Ido1 In Inflammatory Programming: Pathogenic Neovascularizatsupporting
confidence: 69%
“…As predicted, Ido1 −/− mice exhibited a significant reduction in OIR-induced retinal neovascularization relative to their WT counterparts (Mondal et al, 2016). Loss of the related IDO2 isoform had no demonstrable effect on OIR-induced retinal neovascularization, indicating that the effect is specific to IDO1 (Mondal et al, 2016). No difference in the normal retinal vascularization that develops under normoxic conditions was observed between Ido1 −/− and WT groups and reduction of the avascular region (Mondal et al, 2016), indicative of normal revascularization, was actually higher in the Ido1 −/− animals indicative of an improvement in normal vascular regrowth occurring in mice lacking IDO1.…”
Section: Ido1 In Inflammatory Programming: Pathogenic Neovascularizatsupporting
confidence: 69%
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