Preclinical development of human granulocyte-macrophage colony-stimulating factor-transfected melanoma cell vaccine using established canine cell lines and normal dogs

Gs, Hogge; Jk, Burkholder; Culp, Jerilyn; Mr, Albertini; Rr, Dubielzig; Yang, Ning; Eg, MacEwen

doi:10.1038/sj.cgt.7700015

Cited by 46 publications

(12 citation statements)

References 33 publications

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“…In canine cells, it has been shown that a radiation dose between 15 and 100 Gy is sufficient to block completely the cloning capacity of the tumor cells. 23 We confirmed that a single dose of 30 Gy on D17 and Abrams cell lines inhibited cell proliferation (data not shown). Consequently, canine cell lines were inactivated with a single dose of 30 Gy after infection and viral replication was assessed.…”

Section: Neutralization Assayssupporting

confidence: 69%

“…Biodistribution analysis was performed as previously described. 23 Briefly, frozen tissues were ground to a fine powder using a pestle and mortar and processed according to manufacturer instructions (Promega, Madison, WI). Luciferase enzyme activity in supernatants was assessed using luciferase assay reagent (Promega) and normalized to total protein content.…”

Section: Neutralization Assaysmentioning

confidence: 99%

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Osteosarcoma cells as carriers to allow antitumor activity of canine oncolytic adenovirus in the presence of neutralizing antibodies

et al. 2010

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Osteosarcoma (OSA) is the most common bone tumor affecting the dog. The veterinary options for therapeutic management of OSA are limited and prognosis for such patients is poor. Oncolytic adenoviruses are attractive tools for experimental therapeutics as they can replicate and spread within tumors to directly induce tumor destruction. However, a major impediment to systemic oncolytic adenoviruses injection is the presence of pre-existing neutralizing antibodies (Nabs). In this study, we investigated the effect of a replication-selective canine adenovirus (OCCAV) to treat OSA in the presence of Nabs and the use of canine OSA cells as carrier vehicles for evading Nabs. Our systemic biodistribution data indicated that canine tumor cells could successfully reach the tumor site and deliver OCCAV to tumor cells in an immunized mice model. Furthermore, the use of carrier cells also reduced adenovirus uptake by the liver. Importantly, OCCAV alone was not effective to control tumor growth in a pre-immunized xenograft mouse model. On the contrary, systemic antitumoral activity of carrier-cell OCCAV was evident even in the presence of circulating antibodies, which is a relevant result from a clinical point of view. These findings are of direct translational relevance for the future design of canine clinical trials.

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Section: Neutralization Assayssupporting

confidence: 69%

Section: Neutralization Assaysmentioning

confidence: 99%

Osteosarcoma cells as carriers to allow antitumor activity of canine oncolytic adenovirus in the presence of neutralizing antibodies

et al. 2010

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“…Note the multiple roles of the tyrosinase enzyme. different vaccination strategy and injected healthy dogs with lethally irradiated CMM cells transfected with human GM-CSF resulting in increased numbers of macrophages, which may act as APCs, at the vaccination site compared to non-transfected tumour cell vaccines (Hogge et al, 1999). In a further trial, Finocchiaro and Gilkin combined autologous/allogeneic formolised tumour cells as a vaccine injected concomitantly with lethally irradiated xenogeneic cells producing human IL-2 and human GM-CSF to treat CMM patients .…”

Section: Whole Cell Vaccinationmentioning

confidence: 99%

Cancer immunology and canine malignant melanoma: A comparative review

Atherton

Morris

McDermott

et al. 2016

Veterinary Immunology and Immunopathology

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Canine melanoma as a model of human melanomaFor at least two decades, veterinary oncologists have advocated using spontaneously occurring tumours in companion animals as models for human cancer (Knapp and Waters, 1997;MacEwen, 1990). Several recent reviews have readdressed this approach identifying osteosarcoma, mammary tumours, head and neck cancers, bladder carcinomas, non-Hodgkin lymphoma, prostatic carcinoma, lung cancer and pertinently oral canine malignant melanoma (CMM) as good models for human neoplasms (Hansen and Khanna, 2004;Khanna and Hunter, 2005;Paoloni and Khanna, 2008). The major benefits of dogs as tumour models include the ability to study genetically outbred and immunologically intact animals in which cancers develop spontaneously and thus, more likely reflect the process of tumourigenesis compared to experimentally-induced neoplasms. As pets and owners share the same environment, they may be exposed to the same carcinogens, which, in part, drive tumour development. Regarding disease modelling, animal tumours often have similar clinical presentation, tumour biology and histopathological appearance to their human counterparts and usually progress more rapidly, thereby shortening data maturation times. In addition, few "standard of care" therapies exist for dogs meaning that within reason, trial therapeutics can be instigated at any point. Given these benefits, companion animal tumour models more accurately reflect the features of human cancers compared to rodent models with CMM being a desirable example of one such neoplasm. Conversely, the opportunity to translate the potential value of state of the art human therapeutics to the veterinary clinic also exists. Oral canine malignant melanoma (CMM) is a spontaneously occurring aggressive tumour with relatively few medical treatment options, which provides a suitable model for the disease in humans. Historically, multiple immunotherapeutic strategies aimed at provoking both innate and adaptive anti-tumour immune responses have been published with varying levels of activity against CMM. Recently, a plasmid DNA vaccine expressing human tyrosinase has been licensed for the adjunct treatment of oral CMM. This article reviews the immunological similarities between CMM and the human counterpart; mechanisms by which tumours evade the immune system; reasons why melanoma is an attractive target for immunotherapy; the premise of whole cell, dendritic cell (DC), viral and DNA vaccination strategies alongside preliminary clinical results in dogs. Current "gold standard" treatments for advanced human malignant melanoma are evolving quickly with remarkable results being achieved following the introduction of immune checkpoint blockade and adoptively transferred cell therapies. The rapidly expanding field of cancer immunology and immunotherapeutics means that rational targeting of this disease in both species should enhance treatment outcomes in veterinary and human clinics.

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“…Three independent trials have examined the delivery of IL-2 or GM-CSF DNA with histoincompatible cells, 5 in combination with staphylococcal enterotoxin B, 2 or in autologous tumor vaccines. 37,38 The objective response rates for these studies were 50, 33, and 20%, respectively. The first two approaches led to median survival times that exceeded the control group or the anticipated survival based on historical data (39 and 24 weeks, respectively).…”

Section: Discussionmentioning

confidence: 86%

Enhancing antimelanoma immune responses through apoptosis

et al. 2003

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We examined the feasibility of using tumor apoptosis at accessible sites to enhance antimelanoma immune responses in a model of spontaneous canine melanoma. We show that priming peripheral blood mononuclear cells with apoptotic melanoma cells significantly enhanced autologous and allogeneic lymphokine-activated killing of tumor cells. Since various pathways required for intrinsic apoptosis are often inactivated in melanoma, we used Fas ligand (FasL) overexpression to promote extrinsic apoptosis. FasL induced apoptosis in five of six cell lines. Each of the susceptible lines, but not the resistant one, expressed Fas mRNA. In addition, direct intratumoral administration of FasL DNA to tumor-bearing dogs was safe, with no adverse events reported over 7 days of observation. A reduction of tumor burden was seen in three of five dogs treated. The reduction of tumor volume was correlated with Fas expression by the tumors, although one dog with a Fas-negative tumor survived for 82 weeks after treatment. Our data show that overexpression of FasL is suitable to promote apoptosis of Fas + melanomas, and support the notion that priming immune responder cells with apoptotic tumor cells may enhance antitumor responses. The results also suggest that intratumoral administration of FasL offers a safe route for therapeutic gene delivery.

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Preclinical development of human granulocyte-macrophage colony-stimulating factor-transfected melanoma cell vaccine using established canine cell lines and normal dogs

Cited by 46 publications

References 33 publications

Osteosarcoma cells as carriers to allow antitumor activity of canine oncolytic adenovirus in the presence of neutralizing antibodies

Osteosarcoma cells as carriers to allow antitumor activity of canine oncolytic adenovirus in the presence of neutralizing antibodies

Cancer immunology and canine malignant melanoma: A comparative review

Enhancing antimelanoma immune responses through apoptosis

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