Effects of Vascular Endothelial Growth Factor on the Lymphocyte-Endothelium Interactions: Identification of Caveolin-1 and Nitric Oxide as Control Points of Endothelial Cell Anergy

Bouzin, Caroline; Brouet, Agnès; Vriese, Joelle De; DeWever, Julie; Feron, Olivier

doi:10.4049/jimmunol.178.3.1505

Cited by 173 publications

(125 citation statements)

References 25 publications

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“…Where indicated, cells were transfected with siRNAs as previously reported (50) or with a shRNA according to the manufacturer's protocol (Invitrogen). Human MCT1-specific siRNA targeted AAGAG-GCTGACTTTTCCAAAT sequence, a scrambled siRNA (AACTCGCT-GAG-ATTTCGTTAT) served to control specificity, and sham-transfected cells were used as a negative control.…”

Section: Methodsmentioning

confidence: 99%

Targeting lactate-fueled respiration selectively kills hypoxic tumor cells in mice

Sonveaux¹,

Végran²,

Schroeder³

et al. 2008

J. Clin. Invest.

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1,108

1,612

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Tumors contain oxygenated and hypoxic regions, so the tumor cell population is heterogeneous. Hypoxic tumor cells primarily use glucose for glycolytic energy production and release lactic acid, creating a lactate gradient that mirrors the oxygen gradient in the tumor. By contrast, oxygenated tumor cells have been thought to primarily use glucose for oxidative energy production. Although lactate is generally considered a waste product, we now show that it is a prominent substrate that fuels the oxidative metabolism of oxygenated tumor cells. There is therefore a symbiosis in which glycolytic and oxidative tumor cells mutually regulate their access to energy metabolites. We identified monocarboxylate transporter 1 (MCT1) as the prominent path for lactate uptake by a human cervix squamous carcinoma cell line that preferentially utilized lactate for oxidative metabolism. Inhibiting MCT1 with α-cyano-4-hydroxycinnamate (CHC) or siRNA in these cells induced a switch from lactate-fueled respiration to glycolysis. A similar switch from lactate-fueled respiration to glycolysis by oxygenated tumor cells in both a mouse model of lung carcinoma and xenotransplanted human colorectal adenocarcinoma cells was observed after administration of CHC. This retarded tumor growth, as the hypoxic/glycolytic tumor cells died from glucose starvation, and rendered the remaining cells sensitive to irradiation. As MCT1 was found to be expressed by an array of primary human tumors, we suggest that MCT1 inhibition has clinical antitumor potential.

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Section: Methodsmentioning

confidence: 99%

Targeting lactate-fueled respiration selectively kills hypoxic tumor cells in mice

Sonveaux¹,

Végran²,

Schroeder³

et al. 2008

J. Clin. Invest.

Self Cite

1,108

1,612

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“…This is important for pathological angiogenesis, because NO has an inhibitory effect on leukocyte recruitment through downregulation of P-selectin, as a mechanism of decreasing inflammatory responses (2). Importantly, VEGFR2 and eNOS colocalize in caveolae, and this is the site of VEGF-A stimulated NO production (20). This is important for angiogenic activity because NO is a critical signaling molecule necessary for endothelial cell differentiation and motility.…”

Section: Angiogenic Mediators In Ibd and Experimental Colitismentioning

confidence: 99%

Pathogenic angiogenesis in IBD and experimental colitis: new ideas and therapeutic avenues

Chidlow

Shukla²,

Grisham³

et al. 2007

American Journal of Physiology-Gastrointestinal and Liver Physi

144

114

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Chidlow JH Jr, Shukla D, Grisham MB, Kevil CG. Pathogenic angiogenesis in IBD and experimental colitis: new ideas and therapeutic avenues. Am J Physiol Gastrointest Liver Physiol 293: G5-G18, 2007. First published April 26, 2007; doi:10.1152/ajpgi.00107.2007.-Angiogenesis is now understood to play a major role in the pathology of chronic inflammatory diseases and is indicated to exacerbate disease pathology. Recent evidence shows that angiogenesis is crucial during inflammatory bowel disease (IBD) and in experimental models of colitis. Examination of the relationship between angiogenesis and inflammation in experimental colitis shows that initiating factors for these responses simultaneously increase as disease progresses and correlate in magnitude. Recent studies show that inhibition of the inflammatory response attenuates angiogenesis to a similar degree and, importantly, that inhibition of angiogenesis does the same to inflammation. Recent data provide evidence that differential regulation of the angiogenic mediators involved in IBD-associated chronic inflammation is the root of this pathological angiogenesis. Many factors are involved in this phenomenon, including growth factors/cytokines, chemokines, adhesion molecules, integrins, matrix-associated molecules, and signaling targets. These factors are produced by various vascular, inflammatory, and immune cell types that are involved in IBD pathology. Moreover, recent studies provide evidence that antiangiogenic therapy is a novel and effective approach for IBD treatment. Here we review the role of pathological angiogenesis during IBD and experimental colitis and discuss the therapeutic avenues this recent knowledge has revealed. inflammation; T cells; growth factors; adhesion molecules; antiangiogenesis ANGIOGENESIS PLAYS AN IMPORTANT role in many chronic inflammatory diseases including but not limited to diabetic retinopathy, atherosclerosis, rheumatoid arthritis, hypercholesterolemia, and psoriasis. It has been suggested that the angiogenic components of these diseases contribute to and exacerbate disease conditions (26, 31). Recent findings, both clinical and experimental, indicate that angiogenesis also plays a crucial role in the inflammatory bowel diseases (IBD), consisting of Crohn's disease (CD) and ulcerative colitis (UC) (31,37,58,131,155). Development of new vasculature during chronic inflammation may play a negative "pathological" role by contributing to increased inflammatory responses due to dysfunctional new vessel architecture and increases in the recruitment of inflammatory cell types. Importantly, recent data have shown that angiogenic inhibition during chronic inflammatory diseases attenuates further inflammation and disease pathology (31, 37, 51). As such, expanding our knowledge of how pathological angiogenesis occurs during IBD will further our ability to treat patients with these diseases. IBD PathogenesisCD and UC are idiopathic inflammatory disorders of the intestine and/or colon in which patients suffer from rectal bleeding, severe...

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“…However, tumors have developed strategies to suppress the recruitment of T cells to the tumor site (231). Disruption of chemokines that attract T cells (232) and inhibition of adhesion molecule expression on vascular endothelium through angiogenic growth factors, such as VEGF (233), play a role in preventing successful transmigration through the tumor endothelial barrier. The combination of ipilimumab with the VEGF inhibitor bevacizumab was therefore evaluated in metastatic melanoma.…”

Section: T Cell Trafficking and Infiltration Into Tumorsmentioning

confidence: 99%

Coinhibitory Pathways in Immunotherapy for Cancer

Baumeister

Freeman

Dranoff

et al. 2016

Annu. Rev. Immunol.

789

777

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The immune system is capable of recognizing tumors and eliminates many early malignant cells. However, tumors evolve to evade immune attack, and the tumor microenvironment is immunosuppressive. Immune responses are regulated by a number of immunological checkpoints that promote protective immunity and maintain tolerance. T cell coinhibitory pathways restrict the strength and duration of immune responses, thereby limiting immune-mediated tissue damage, controlling resolution of inflammation, and maintaining tolerance to prevent autoimmunity. Tumors exploit these coinhibitory pathways to evade immune eradication. Blockade of the PD-1 and CTLA-4 checkpoints is proving to be an effective and durable cancer immunotherapy in a subset of patients with a variety of tumor types, and additional combinations are further improving response rates. In this review we discuss the immunoregulatory functions of coinhibitory pathways and their translation to effective immunotherapies for cancer.

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Effects of Vascular Endothelial Growth Factor on the Lymphocyte-Endothelium Interactions: Identification of Caveolin-1 and Nitric Oxide as Control Points of Endothelial Cell Anergy

Cited by 173 publications

References 25 publications

Targeting lactate-fueled respiration selectively kills hypoxic tumor cells in mice

Targeting lactate-fueled respiration selectively kills hypoxic tumor cells in mice

Pathogenic angiogenesis in IBD and experimental colitis: new ideas and therapeutic avenues

Coinhibitory Pathways in Immunotherapy for Cancer

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