Specific active immunotherapy in patients with adenocarcinoma of the colon utilizing tumor-associated antigens (TAA). A phase I clinical trial

Hollinshead, Ariel C.; Elias, E. George; Arlen, Myron; Buda, Barbara; Mosley, Maria; Scherrer, Joseph

doi:10.1002/1097-0142(19850801)56:3<480::aid-cncr2820560312>3.0.co;2-2

Cited by 39 publications

(26 citation statements)

References 16 publications

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“…The idea behind immunotherapy of cancer is that transformed cells express antigens that, in principle, can be recognized by the immune system and can be targeted for specific elimination of tumor cells [54,55]. Potential tumor antigens are, for example, mutated oncogenes or tumor-suppressor genes that were causative for the tumor (for example the EVT6-AML1 fusion protein in lymphoblastic leukemia [56]) or proteins that are normally rarely expressed in differentiated cells but are expressed in the malignant tissue like expression of the melanoma antigen-encoding genes (MAGE) in melanoma cells [57] or carcinoembryonic antigen (CEA) [58].…”

Section: Immunotherapymentioning

confidence: 82%

Gene therapy and gastrointestinal cancer: concepts and clinical facts

Hauses¹,

Schackert²

1999

Langenbeck's Arch Surg

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Data on 22 clinical trials on malignancies of the gastrointestinal tract are available. They utilize a variety of gene-delivery methods and target cell populations, and there is considerable variety among their strategies. Gene transfer is performed by injection of naked plasmid DNA and by use of DNA-liposome complexes and viral vectors. In some cases, the gene transfer is carried out ex vivo and the patients receive genetically modified cells, whereas other approaches deliver the vector to the target cell population in vivo. The theoretical concepts of gene therapy can be divided into three groups. One approach makes use of suicide genes comprising bacterial or viral genes that convert a nontoxic prodrug into a highly cytotoxic chemotherapeutic agent at the tumor site. This approach aims at higher therapeutic specificity and fewer side effects than with the systemic delivery of cytotoxic agents. The second strategy makes an attempt to invoke the immune system to destroy malignant cells. Different strategies, such as immunization with genetically modified tumor cells or transfer of new genes to T cells, are considered to have clinical benefits. The major advantage of these immunotherapeutic approaches is the systemic effect both on the primary tumor and on metastases. The third strategy evolved from the insight that cancer is a genetic disease caused by activation of oncogenes or inactivation of tumor-suppressor genes. Compensation of genetic defects by the downregulation of activated oncogenes or the restoration of tumor-suppressor-gene functions may be able to revert the malignant phenotype of cancer cells. Of the 22 gene-therapy trials, 17 trials focus on immunotherapy. Only two trials make use of suicide genes and, in three trials, a functional copy of the p53 tumor-suppressor gene was reintroduced into malignant cells. Modalities for gene transfer and the strategies underlying gene therapy will be discussed in the context of gastrointestinal malignancies and the potential benefits for patients.

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Section: Immunotherapymentioning

confidence: 82%

Gene therapy and gastrointestinal cancer: concepts and clinical facts

Hauses¹,

Schackert²

1999

Langenbeck's Arch Surg

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“…Rather, the immune system for the most part only detects the presence of a relatively small level of tumor antigen, and exerts a minimal response through a process termed "tumor surveillance". In the original Hollinshead et al [4] vaccine trials, it was shown that an ideal response to tumor antigen occurred with the administration of a threshold level of approximately 750-1000 µg of antigen administered intradermally along with an adjuvant. In most malignancies the level of immunogen (TAA) expression rarely exceeds 30-50 µg.…”

Section: Discussionmentioning

confidence: 99%

“…They were first identified by Hollinshead et al [4] from pooled allogeneic tumor specimens obtained following surgery. Further purification by sephadex column chromatography and isoelectric focusing led to the identification of these tumor associated antigens.…”

Section: Introductionmentioning

confidence: 99%

The Clinical Detection of Pancreatic Carcinoma: A Comparison of the Standard Biomarkers to that of a Newer Class of Biomarkers used for both Diagnosis and Therapy

Arlen¹,

Arlen²,

X³

et al. 2012

Pancreat Disord Ther

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“…A biologic approach is currently being pursued to identify immunogenic functional neoantigens. Ensituximab is one of several monoclonal antibodies raised against an allogeneic colorectal cancer vaccine that had previously been tested in human clinical trials in the USA [14]. Surgical samples from dozens of patients with various stages of colorectal cancer including metastatic foci were obtained as a source for antigen screening.…”

mentioning

confidence: 99%

“…Surface membrane from pooled allogeneic tumor was fractionated and various molecular weight components were tested for immunogenic reactivity which was the basis of the initial vaccine. Results revealed safety of the vaccine, but clinical benefit that directly correlated with the ability of the patients' immune system to mount IgG responses against the vaccine [14]. Based on the results of these early studies, the original vaccine was used as the source of antigenic material to produce monoclonal antibodies that specifically reacted with colorectal cancer and could kill tumor via antibody-dependent, cell-mediated cytotoxicity.…”

mentioning

confidence: 99%

Neoantigens in the immuno-oncology space

Arlen¹

2017

Future Oncol.

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Specific active immunotherapy in patients with adenocarcinoma of the colon utilizing tumor-associated antigens (TAA). A phase I clinical trial

Cited by 39 publications

References 16 publications

Gene therapy and gastrointestinal cancer: concepts and clinical facts

Gene therapy and gastrointestinal cancer: concepts and clinical facts

The Clinical Detection of Pancreatic Carcinoma: A Comparison of the Standard Biomarkers to that of a Newer Class of Biomarkers used for both Diagnosis and Therapy

Neoantigens in the immuno-oncology space

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