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Featured researches published by Robert C. Unfer.


Cancer Research | 2005

Effective Treatment of Preexisting Melanoma with Whole Cell Vaccines Expressing α(1,3)-Galactosyl Epitopes

Gabriela R. Rossi; Mario R. Mautino; Robert C. Unfer; Tatiana Seregina; Nicholas N. Vahanian; Charles J. Link

The hyperacute immune response in humans is a potent mechanism of xenograft rejection mediated by complement-fixing natural antibodies recognizing alpha(1,3)-galactosyl epitopes (alphaGal) not present on human cells. We exploited this immune mechanism to create a whole cell cancer vaccine to treat melanoma tumors. B16 melanoma vaccines genetically engineered to express alphaGal epitopes (B16alphaGal) effectively treated preexisting s.c. and pulmonary alphaGal-negative melanoma (B16Null) tumors in the alpha(1,3)-galactosyltransferase knockout mouse model. T cells from mice vaccinated with B16alphaGal recognized B16Null melanoma cells measured by detection of intracellular tumor necrosis factor-alpha. We showed successful adoptive transfer of immunity to recipient mice bearing lung melanoma metastasis. Mice receiving lymphocytes from donors previously immunized with B16alphaGal had reduced pulmonary metastases. The transfer of lymphocytes from mice vaccinated with control vaccine had no effect in the pulmonary metastasis burden. This study unequivocally establishes for the first time efficacy in the treatment of preexisting melanoma tumors using whole cell vaccines expressing alphaGal epitopes. Vaccination with B16alphagal induced strong long-lasting cell-mediated antitumor immunity extended to B16Null. These data formed the basis for the testing of this therapeutic strategy in human clinical trials currently under way.


Clinical Cancer Research | 2004

Rat Sodium Iodide Symporter for Radioiodide Therapy of Cancer

Elena Mitrofanova; Robert C. Unfer; Nick Vahanian; Wayne Daniels; Erica Roberson; Tatiana Seregina; Prem Seth; Charles J. Link

Design and development of new approaches for targeted radiotherapy of cancer and improvement of therapeutic index by more local radiation therapy are very important issues. Adenovirus-mediated delivery of the sodium iodide symporter (NIS) gene to cancer cells is a powerful technique to concentrate lethal radiation in tumor cells and eradicate tumors with increased therapeutic index. A replication-defective adenoviral vector expressing the rat NIS gene (Ad-rNIS) was used for in vitro gene delivery and into human prostate cancer xenografts to study antitumor effect. Robust function of the rat symporter was detected in DU145, T47D, and HCT-15 human cancer cell lines transduced with Ad-rNIS. All three cancer cell lines successfully transferred functionally active rat symporter to the plasma membrane, resulting in very high levels of iodine-125 accumulation. Three-dimensional multicellular tumor spheroids derived from DU145 human prostate cancer cells were transduced with Ad-rNIS and incubated with 131I for 24 hours. After treatment, spheroids rapidly decreased in size and disappeared within 10 days. In vivo data revealed an inhibition of tumor growth in athymic nude mice after intratumoral Ad-rNIS injection followed by 131I administration. Eighty-eight percent of experimental mice survived >30 days, whereas control groups had only 18% survival >30 days. This is the first report that demonstrates the rat NIS gene can effectively induce growth arrest of human tumor xenografts after in vivo adenoviral gene delivery and 131I administration. The data confirm our hypothesis that the rat NIS gene is an attractive suicide gene candidate for cancer treatment.


Journal of Controlled Release | 2005

Novel cationic pentablock copolymers as non-viral vectors for gene therapy.

Ankit Agarwal; Robert C. Unfer; Surya K. Mallapragada


Cancer Immunology, Immunotherapy | 2005

Complete protection against melanoma in absence of autoimmune depigmentation after rejection of melanoma cells expressing α(1,3)galactosyl epitopes

Gabriela R. Rossi; Robert C. Unfer; Tatiana Seregina; Charles J. Link


Biomaterials | 2008

Dual-role self-assembling nanoplexes for efficient gene transfection and sustained gene delivery

Ankit Agarwal; Robert C. Unfer; Surya K. Mallapragada


Cancer Research | 2003

Immunity to the α(1,3)galactosyl epitope provides protection in mice challenged with colon cancer cells expressing α(1,3)galactosyl-transferase: A novel suicide gene for cancer gene therapy

Robert C. Unfer; Daniel J. Hellrung; Charles J. Link


Journal of Controlled Release | 2007

Colloidally stable novel copolymeric system for gene delivery in complete growth media.

Ankit Agarwal; Rita Vilensky; Anne Stockdale; Yeshayahu Talmon; Robert C. Unfer; Surya K. Mallapragada


Journal of Biomedical Materials Research Part A | 2007

Investigation of in vitro biocompatibility of novel pentablock copolymers for gene delivery

Ankit Agarwal; Robert C. Unfer; Surya K. Mallapragada


Human Gene Therapy | 2005

Effective growth arrest of human colon cancer in mice, using rat sodium iodide symporter and radioiodine therapy.

Elena Mitrofanova; Robert C. Unfer; Nick Vahanian; Struan Kane; Martha Carvour; Charles J. Link


Cancer Research | 2006

Adipophilin induction, lipid accumulation, and anti-proliferation through PPAR-gamma activation in malignant melanoma

Simon K. Wright; Robert C. Unfer; Jason Shellnut

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Charles J. Link

National Foundation for Cancer Research

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Elena Mitrofanova

National Foundation for Cancer Research

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Tatiana Seregina

National Foundation for Cancer Research

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Gabriela R. Rossi

National Foundation for Cancer Research

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Martha Carvour

National Foundation for Cancer Research

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Prem Seth

Northwestern University

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Daniel J. Hellrung

National Foundation for Cancer Research

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