The endothelin B (ETB) receptor agonist IRL 1620 is highly vasoconstrictive in two syngeneic rat tumour lines: potential for selective tumour blood flow modification

Čemažar, Maja; Wilson, Ian A.; Prise, Vivien E.; Bell, Katrina M.; Hill, Sally A.; Tozer, G. M.

doi:10.1038/sj.bjc.6602672

Cited by 11 publications

(12 citation statements)

References 26 publications

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“…A similar observation of the reduction of response at higher dose has been reported for another ET B receptor agonist, sarafotoxin S6c in rats [62]. However, effect of IRL-1620 on tumor blood vessels in the HSN fibrosarcoma has been reported to be vasoconstrictive [63,64]. While, sarafotoxin S6c administration increased tumor blood flow (176%) compared to control animals in the same model [65].…”

Section: Discussionsupporting

confidence: 70%

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IRL‐1620, a tumor selective vasodilator, augments the uptake and efficacy of chemotherapeutic agents in prostate tumor rats

2007

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Section: Discussionsupporting

confidence: 70%

“…The Prostate DOI 10.1002/pros [67]. Rapid blood flow reduction observed with IRL-1620 in the P22 tumor and the HSN sarcoma [64] might be due to the existence of larger population of VSMCs in the sarcoma (muscle) tumor model employed for the study and/or may be attributed to doses of ET B receptor agonists used.…”

Section: Discussionmentioning

confidence: 99%

IRL‐1620, a tumor selective vasodilator, augments the uptake and efficacy of chemotherapeutic agents in prostate tumor rats

2007

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“…We never observed an autoimmunity of inflammation associated with ETBR blockade in mice, which contrasts with more robust immune therapies that can cause adverse events like autoimmunity [151]. ETBR blockade is likely to have also direct antiangiogenic effects through suppression of endothelial nitric oxide or tumor-derived VEGF, and although the antitumor effect of ETBR blockade, singly, may be modest, the combined use of ETBR antagonists with immunotherapy may act synergistically to inhibit angiogenesis [144,152].…”

Section: The Tumor Endothelial Barriermentioning

confidence: 78%

Tumor immune surveillance and ovarian cancer

Kandalaft

Motz

Duraiswamy

et al. 2011

Cancer Metastasis Rev

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In the past few years, cancer immunotherapies have produced promising results. Although traditionally considered unresponsive to immune therapy, increasing evidence indicates that ovarian cancers are, in fact, immunogenic tumors. This evidence comes from diverse epidemiologic and clinical data comprising evidence of spontaneous antitumor immune response and its association with longer survival in a proportion of ovarian cancer patients; evidence of tumor immune evasion mechanisms and their association with short survival in some ovarian cancer patients; and finally pilot data supporting the efficacy of immune therapy. Below we will discuss lessons learned on the biology underlying ovarian cancer immune rejection or tolerance and we will discuss its association with clinical outcome. We will discuss the role of angiogenesis and the tumor endothelium on regulation of the antitumor immune response with a special emphasis on the role of vascular endothelial growth factor (VEGF) in the suppression of immunological processes, which control tumor progression and its unique crosstalk with endothelin systems, and how their interactions may shape the antitumor immune response. In addition, we will discuss mechanisms of tumor tolerance through the suppression or exhaustion of effector cells and how these could be countered in the clinic. We believe that understanding these pathways in the tumor microenvironment will lead to novel strategies for enhancing ovarian cancer immunotherapy.

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“…Unlike in patients with sepsis (97), NO inhibition is safe and has been well tolerated in cancer patients (98). Although the anticancer effect of ET B R (or NO) blockade as monotherapy may be modest, the concomitant administration of immunotherapy may act synergistically against angiogenesis (86, 99). …”

Section: Clinical-translational Advancesmentioning

confidence: 99%

Endothelin B Receptor, a New Target in Cancer Immune Therapy

Kandalaft

Facciabene

Buckanovich

et al. 2009

Clinical Cancer Research

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The endothelins and their G protein-coupled receptors A and B have been implicated in numerous diseases and have recently emerged as pivotal players in a variety of malignancies. Tumors overexpress the endothelin 1 (ET-1) ligand and the endothelin-A-receptor (ET A R). Their interaction induces tumor growth and metastasis by promoting tumor cell survival and proliferation, angiogenesis, and tissue remodeling. On the basis of results from xenograft models, drug development efforts have focused on antagonizing the autocrine-paracrine effects mediated by ET-1/ET A R. In this review, we discuss a novel role of the endothelin-B-receptor (ET B R) in tumorigenesis and the effect of its blockade during cancer immune therapy.We highlight key characteristics of the B receptor such as its specific overexpression in the tumor compartment; and specifically, in the tumor endothelium, where its activation by ET-1suppressesT-cell adhesion and homing to tumors. We also review our recent findings on the effects of ET B R-specific blockade in increasing T-cell homing to tumors and enhancing the efficacy of otherwise ineffective immunotherapy.

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The endothelin B (ETB) receptor agonist IRL 1620 is highly vasoconstrictive in two syngeneic rat tumour lines: potential for selective tumour blood flow modification

Cited by 11 publications

References 26 publications

IRL‐1620, a tumor selective vasodilator, augments the uptake and efficacy of chemotherapeutic agents in prostate tumor rats

IRL‐1620, a tumor selective vasodilator, augments the uptake and efficacy of chemotherapeutic agents in prostate tumor rats

Tumor immune surveillance and ovarian cancer

Endothelin B Receptor, a New Target in Cancer Immune Therapy

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