Cytotoxic T lymphocyte and antibody responses generated in rhesus monkeys immunized with retroviral vector-transduced fibroblasts expressing human immunodeficiency virus type-1 IIIB ENV/REV proteins. NLM AIDSLINE Important note: Information in this article was accurate in 1995. The state of the art may have changed since the publication date.

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Cytotoxic T lymphocyte and antibody responses generated in rhesus monkeys immunized with retroviral vector-transduced fibroblasts expressing human immunodeficiency virus type-1 IIIB ENV/REV proteins.

Hum Gene Ther. 1994 Jul;5(7):853-62. Unique Identifier : AIDSLINE MED/95072131
Laube LS; Burrascano M; Dejesus CE; Howard BD; Johnson MA; Lee WT; Lynn AE; Peters G; Ronlov GS; Townsend KS; et al; Viagene, Inc., San Diego, CA 92121.

Abstract: The immune response against human immunodeficiency virus type-1 (HIV-1) is believed to play a role in controlling the early stages of disease progression. The cellular immune response, in particular cytotoxic T lymphocyte (CTL) activity, may be important for eliminating virally infected cells in HIV-1-infected individuals. Genetic immunization using retroviral vectors provides an effective means of introducing antigens into the antigen presentation pathways for T cell stimulation. A nonreplicating, amphotropic murine retroviral vector containing the HIV-1 IIIB env gene has been used to transduce primary rhesus monkey fibroblasts for the expression of HIV-1 antigenic determinants. Rhesus monkeys were immunized with four doses of either vector-transduced autologous fibroblasts (VTAF) expressing the HIV-1 IIIB ENV/REV proteins or nontransduced autologous fibroblasts (NTAF) administered at 2-week intervals. The animals were evaluated for both the induction of HIV-1-specific immune responses and potential toxicity associated with this ex vivo treatment. The VTAF-immunized monkeys generated CTL responses specific for HIV-1 ENV/REV expressing autologous target cells, whereas, NTAF-immunized monkeys showed negligible CTL activity. The cytotoxic activity was mediated by CD8+, major histocompatibility complex (MHC)-restricted CTL. In addition, antibody responses directed against the HIV-1 gp120 protein were also detected in the sera of VTAF-immunized monkeys. Clinical and histopathological evaluation of immunized monkeys showed no evidence of significant adverse events. Several animals that received either VTAF or NTAF had detectable anti-cytoplasmic antibodies, but were not positive for anti-nuclear antibodies or rheumatoid factor. Subsequent evaluation of renal, synovial, and hepatic tissue samples from these monkeys revealed no autoimmune disease-associated lesions. This study demonstrates the safety and ability of autologous retroviral vector-transduced cells expressing HIV-1 IIIB ENV/REV proteins to stimulate immune responses in a non-human primate model, and provides a basis for this form of genetic immunization in HIV-infected humans.
Keywords: Animal Antibodies, Antinuclear/ANALYSIS Autoimmune Diseases/ETIOLOGY *AIDS Vaccines B-Lymphocytes/IMMUNOLOGY Cell Line, Transformed Comparative Study Cross Reactions Cytomegalovirus/GENETICS Cytoplasm/IMMUNOLOGY Fibroblasts/*IMMUNOLOGY Gene Products, env/GENETICS/*IMMUNOLOGY Gene Products, rev/GENETICS/*IMMUNOLOGY Genes, Synthetic *Genetic Vectors Human HIV Antibodies/*BIOSYNTHESIS HIV-1/GENETICS/*IMMUNOLOGY Immunization/ADVERSE EFFECTS/*METHODS Liver Diseases/ETIOLOGY Macaca mulatta/IMMUNOLOGY Moloney Leukemia Virus/GENETICS Recombinant Fusion Proteins/GENETICS/*IMMUNOLOGY Rheumatoid Factor/ANALYSIS Safety T-Lymphocytes, Cytotoxic/*IMMUNOLOGY Transduction, Genetic JOURNAL ARTICLEKWDanimalantibodies,antinuclear/analysisautoimmunediseases/etiologyKWDaidsvaccinesb-lymphocytes/immunologycellline,transformedcomparativestudycrossreactionscytomegalovirus/geneticscytoplasm/immunologyfibroblasts/KWDimmunologygeneproducts,env/genetics/KWDimmunologygeneproducts,rev/genetics/KWDimmunologygenes,syntheticKWDgeneticvectorshumanhivantibodies/KWDbiosynthesishiv-1/genetics/KWDimmunologyimmunization/adverseeffects/KWDmethodsliverdiseases/etiologymacacamulatta/immunologymoloneyleukemiavirus/geneticsrecombinantfusionproteins/genetics/KWDimmunologyrheumatoidfactor/analysissafetyt-lymphocytes,cytotoxic/KWDimmunologytransduction,geneticjournalarticle
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Copyright © 1995 - National Library of Medicine. Reproduced under license with the National Library of Medicine, Bethesda, MD.

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