Postoperative active specific immunization in colorectal cancer patients with virus-modified autologous tumor-cell vaccine. First clinical results with tumor-cell vaccines modified with live but avirulent newcastle disease virus

Bohle, W; Schlag, Peter M.; Liebrich, W.; Hohenberger, Peter; Manasterski, Maria; Möller, Peter; Schirrmacher, Volker

doi:10.1002/1097-0142(19901001)66:7<1517::aid-cncr2820660714>3.0.co;2-i

Cited by 48 publications

(18 citation statements)

References 12 publications

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“…Toxicity was mild, manifesting as flu-like symptoms and fevers of up to 38°C. [33][34][35] In the majority of treated patients skin responses were observed against the vaccine at the intradermal site of injection. In a significant proportion of patients, synergistic amplifying effects between the two components of the vaccine, ATV and NDV were seen in augmenting local skin reactivity.…”

Section: Figure 5 No Replication Of Ndv In Normal Resting Human T Celmentioning

confidence: 97%

“…After three vaccinations at 2-week intervals, delayed type hypersensitivity (DTH) responses were increased upon challenge at distant sites with autologous cancer cells (ATV) without the virus. 34,35 This augmented DTH reactivity after ASI treatment upon ATV challenge indicates an augmentation in the precursor frequency of tumor reactive T lymphocytes.…”

Section: Figure 5 No Replication Of Ndv In Normal Resting Human T Celmentioning

confidence: 99%

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Human tumor cell modification by virus infection: an efficient and safe way to produce cancer vaccine with pleiotropic immune stimulatory properties when using Newcastle disease virus

et al. 1999

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Section: Figure 5 No Replication Of Ndv In Normal Resting Human T Celmentioning

confidence: 97%

Section: Figure 5 No Replication Of Ndv In Normal Resting Human T Celmentioning

confidence: 99%

Human tumor cell modification by virus infection: an efficient and safe way to produce cancer vaccine with pleiotropic immune stimulatory properties when using Newcastle disease virus

et al. 1999

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“…Although many studies demonstrate DTH responses in vaccinated patients, very little immunologic data exists in humans to indicate a potential mechanism for the effectiveness of NDV-infected tumor-cell vaccines. In some patients, T-cell (principally CD4 þ ) infiltrates were seen at the site of vaccination [103], while in another study elevated levels of circulating NK cells were detected in the peripheral blood in response to vaccination [104].…”

Section: Viral Modification and Apoptosismentioning

confidence: 99%

Overview of Tumor Cell–Based Vaccines

Copier

Dalgleish

2006

International Reviews of Immunology

103

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Whole-cell tumor vaccines have been investigated for more than 20 years for their efficacy in both preclinical models and in clinical trials in humans. There are clear advantages of whole-cell/polyepitope vaccination over those types of immunotherapy that target specific epitopes. Multiple and unknown antigens may be targeted to both the innate and adaptive immune system, and this may be further augmented by genetic modification of the vaccine cells to provide cytokines and costimulation. In this review, we give an overview of the field including the preclinical and clinical advances using unmodified and modified tumor-cell vaccines.

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“…Furthermore, additional mechanisms have been reported to explain virus-induced tumor regression. Viral proteins associated with either tumor cell membrane fragments or intact cells may enhance the immunogenicity of tumor antigens, thereby augmenting host cellular-and humoralmediated destruction of the tumor [7,8,9]. Certain viruses may stimulate host production of cytokines, for example, interferon and tumor necrosis factor-α [10,11].…”

Section: Introductionmentioning

confidence: 99%

Replication-selective viruses for cancer therapy

Biederer¹,

Ries

Brandts

et al. 2001

J Mol Med

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Advances in our understanding of the molecular basis of cancer and the availability of technology to genetically engineer viruses have led to the development of replication-competent viruses to treat cancer. In theory, replication-selective viruses offer several appealing properties as biological agents for cancer therapy: they kill tumor cells selectively, and their replication leads to amplification of their oncolytic potential. Most preclinical experiments in tissue culture and in animal models support this notion. Clinical data on the first generation of replication-selective viruses are now rapidly accruing. The therapeutic index, and ultimately the clinical outcome, will depend on a complex balance between host and viral factors. This review discusses strategies to kill cancer cells based on our understanding of their molecular defects and the progress being made using replication-competent viruses for tumor therapy. We focus our discussion on a replication-selective adenovirus called ONYX-015 that has recently demonstrated encouraging results in clinical trials

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Postoperative active specific immunization in colorectal cancer patients with virus-modified autologous tumor-cell vaccine. First clinical results with tumor-cell vaccines modified with live but avirulent newcastle disease virus

Cited by 48 publications

References 12 publications

Human tumor cell modification by virus infection: an efficient and safe way to produce cancer vaccine with pleiotropic immune stimulatory properties when using Newcastle disease virus

Human tumor cell modification by virus infection: an efficient and safe way to produce cancer vaccine with pleiotropic immune stimulatory properties when using Newcastle disease virus

Overview of Tumor Cell–Based Vaccines

Replication-selective viruses for cancer therapy

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