Down-modulation of TNFSF15 in ovarian cancer by VEGF and MCP-1 is a pre-requisite for tumor neovascularization

Deng, Weimin; Gu, Xiaohong; Lü, Yi; Gu, Chao; Zheng, Yangyang; Zhang, Zhisong; Chen, Li; Yao, Zhi; Li, Luyuan

doi:10.1007/s10456-011-9244-y

Cited by 47 publications

(73 citation statements)

References 54 publications

(66 reference statements)

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“…We also demonstrated that tumor cells are capable of stimulating such modified Th2 responses, featuring production of IL-10 and IL-4 and secretion of IgG4 by B cells. Also consistent with a tumor-associated inflammatory environment, VEGF, known to polarize Th2-biased cytokine production by PBMCs through induction of IL-10-secreting cells such as Tregs (53), along with well-described tumor-induced inflammatory mediators IL-6 and MCP-1 (53)(54)(55)(56), was found at significantly increased levels (P < 0.001; Supplemental Figure 3A Figure 8. n = 33.…”

Section: Discussionmentioning

confidence: 65%

IgG4 subclass antibodies impair antitumor immunity in melanoma

Karagiannis

Gilbert²,

Josephs³

et al. 2013

J. Clin. Invest.

183

211

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Section: Discussionmentioning

confidence: 65%

IgG4 subclass antibodies impair antitumor immunity in melanoma

Karagiannis

Gilbert²,

Josephs³

et al. 2013

J. Clin. Invest.

183

211

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“…We showed previously that TNFSF15 gene expression in EC is down-regulated by VEGF produced by ovarian cancer cells (42). This indicates that the actions of a positive modulator of angiogenesis, namely VEGF, may lead to the removal from tumor microenvironment of a negative modulator of angiogenesis, namely TNFSF15, which would otherwise functions as an obstacle in the initiation or continuation of tumor angiogenesis.…”

Section: Discussionmentioning

confidence: 86%

“…It also inhibits Lin − -Sca-1 + EPC differentiation into EC (6) and EPC incorporation into tumor vasculature in murine models (10). TNFSF15 expression is absent or marginal in tumor vasculatures in various cancers (40)(41)(42), increased in irritable bowel syndrome (43), and down-regulated in wound tissues (44). TNFSF15 down-regulation in ovarian cancer is facilitated by VEGF secreted by cancer cells as well as by other inflammatory cytokines (42).…”

mentioning

confidence: 99%

“…TNFSF15 expression is absent or marginal in tumor vasculatures in various cancers (40)(41)(42), increased in irritable bowel syndrome (43), and down-regulated in wound tissues (44). TNFSF15 down-regulation in ovarian cancer is facilitated by VEGF secreted by cancer cells as well as by other inflammatory cytokines (42). Death domaincontaining receptor 3 (DR3) (TNFRSF25), a member of the TNF receptor superfamily, has been shown to be the receptor of TNFSF15 in T cells and dendritic cells (45,46).…”

mentioning

confidence: 99%

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TNFSF15 inhibits vasculogenesis by regulating relative levels of membrane-bound and soluble isoforms of VEGF receptor 1

Qin

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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Mouse bone marrow-derived Lin − -Sca-1 + endothelial progenitor cell (EPC) has pluripotent abilities such as supporting neovascularization. Vascular endothelial growth factor (VEGF) receptor 1 (VEGFR1) (Flt1) recognizes various VEGF isoforms and is critically implicated in a wide range of physiological and pathological settings, including vasculogenesis. Mouse EPC expresses two isoforms of VEGFR1: mFlt1, which transmits ligand-induced signals; and sFlt1, which acts as a negative regulator by sequestering ligands of VEGF receptors. How the relative levels of mFlt1 and sFlt1 are regulated is not yet clear. We report here that tumor necrosis factor superfamily 15 (TNFSF15) (also known as VEGI or TL1A), an endothelial cell-secreted cytokine, simultaneously promotes mFlt1 degradation and up-regulates sFlt1 expression in EPC, giving rise to disruption of VEGF-or PlGF-induced activation of eNOS and MAPK p38 and effective inhibition of VEGF-driven, EPC-supported vasculogenesis in a murine Matrigel implant model. TNFSF15 treatment of EPC cultures facilitates Akt deactivationdependent, ubiquitin-assisted degradation of mFlt1 and stimulates sFlt1 expression by activating the PKC, Src, and Erk1/2 signaling pathway. Additionally, TNFSF15 promotes alternative splicing of the Flt1 gene in favor of sFlt1 production by down-regulating nuclear protein Jumonji domain-containing protein 6 (Jmjd6), thus alleviating Jmjd6-inhibited sFlt1 expression. These findings indicate that TNFSF15 is a key component of a molecular mechanism that negatively modulates EPC-supported vasculogenesis through regulation of the relative levels of mFlt1 and sFlt1 in EPC.

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“…Nevertheless, treatment with a peptide that interferes with G-protein coupled receptors, X1/2pal-i3 pepducin, hindered PAR1 activation by MMP1 (74). Recent findings suggest that specific modulators that impede angiogenesis, such as tumor necrosis factor superfamily-15 (TNFSF15), are downregulated by VEGF and CCL2, which are not only released by cancer cells, and therefore, emphasize the importance of contributing cell populations to neoangiogenesis (75).…”

Section: Angiogenic Vasculature Is Required For Tumor Growthmentioning

confidence: 99%

Revisiting the Complexity of the Ovarian Cancer Microenvironment—Clinical Implications for Treatment Strategies

Musrap

Diamandis

2012

Molecular Cancer Research

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Epithelial ovarian cancer (EOC) is the leading cause of death among gynecological malignancies in North American women. Given that EOC encompasses a broad class of tumors consisting of a variety of different histologic and molecular subtypes, which generates genetically and etiologically distinct tumors, several challenges arise during treatment of patients with this disease. Overlaying this complexity is the contribution of supporting cells, particularly stromal components such as fibroblasts and immune infiltrates that collectively create a microenvironment that promotes and enhances cancer progression. A notable example is the induction of angiogenesis, which occurs through the secretion of pro-angiogenic factors by both tumor and tumor-associated cells. The recent development of angiogenic inhibitors targeting tumor vasculature, which have been shown to improve patient outcome when combined with standard therapy, has launched a paradigm shift on how cancer patients should be treated. It is evident that future clinical practices will focus on the incorporation of therapies that antagonize the protumoral effects of such microenvironment contributors. Herein, an overview of the varying tumor-host interactions that influence tumor behavior will be discussed, in addition to the recent efforts undertaken to target these interactions and their potential to revolutionize EOC patient care.

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Down-modulation of TNFSF15 in ovarian cancer by VEGF and MCP-1 is a pre-requisite for tumor neovascularization

Cited by 47 publications

References 54 publications

IgG4 subclass antibodies impair antitumor immunity in melanoma

IgG4 subclass antibodies impair antitumor immunity in melanoma

TNFSF15 inhibits vasculogenesis by regulating relative levels of membrane-bound and soluble isoforms of VEGF receptor 1

Revisiting the Complexity of the Ovarian Cancer Microenvironment—Clinical Implications for Treatment Strategies

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