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Gene gun application in the generation of effector T cells for adoptive immunotherapy
Authors:Keishi Tanigawa  Hua Yu  Rong Sun  Brian J. Nickoloff  Alfred E. Chang
Affiliation:(1) Division of Surgical Oncology, University of Michigan, 3302 Cancer Center, 1500 E. Medical Center Drive, Ann Arbor, MI 48109-0932, USA e-mail: aechang@umich.edu Tel.: +1-734-936-4392 Fax: +1-734-647-9647, US;(2) H. Lee Moffitt Cancer Center and Research Institute, University of South Florida, College of Medicine, Tampa, FL 33612, USA, US;(3) Department of Pathology, Loyola University Medical Center, Maywood, IL 00153, USA, US
Abstract:We utilized the gene gun to transfect subcutaneous D5 melanoma and MT-901 mammary carcinoma tumors in situ with a granulocyte/macrophage-colony-stimulating factor (GM-CSF) plasmid complexed to gold particles. There was diminished tumor growth following bombardment with GM-CSF plasmid, which was apparent only during the period of administration. Transgenic GM-CSF was produced by the skin overlying the tumors and not by the tumors themselves. GM-CSF plasmid bombardment resulted in increased cell yields within tumor-draining lymph nodes (TDLN) with at least a 12-fold increase in the percentage of dendritic cells (8.9%) compared to controls (0.7%). Secondarily activated TDLN cells from animals transfected with GM-CSF demonstrated enhanced cytokine release (interferon γ, GM-CSF and interleukin-10) in response to tumor stimulator cells compared to controls, and had an increased capacity to mediate tumor regression in adoptive immunotherapy. There was a small, but detectable, non-specific immune adjuvant effect observed with gold particle bombardment alone, which was less than with GM-CSF plasmid. The adjuvant effect of GM-CSF plasmid required peri-tumoral transgene expression since gene bombardment away from the tumor was ineffective. Received: 27 April 1999 / Accepted: 27 August 1999
Keywords:T cells  Gene therapy  Adoptive immunotherapy  Vaccines
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