1. Generation of Gene-Engineered Chimeric DNA Molecules for Specific Therapy of Autoimmune Diseases
- Author
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Andrey Tchorbanov, Maria Nikolova, Zsuzsanna Szekeres, Nikolina Mihaylova, Vera Gesheva, Iliyana Dimitrova, Anna Erdei, and József Prechl
- Subjects
Mice, Inbred MRL lpr ,Biology ,Applied Microbiology and Biotechnology ,law.invention ,Mice ,chemistry.chemical_compound ,Antigen ,immune system diseases ,law ,Genetics ,medicine ,Animals ,Lupus Erythematosus, Systemic ,Amino Acid Sequence ,skin and connective tissue diseases ,Research Articles ,Genetics (clinical) ,Pharmacology ,Systemic lupus erythematosus ,Lupus erythematosus ,medicine.disease ,Molecular biology ,Disease Models, Animal ,chemistry ,Naked DNA ,Antibodies, Antinuclear ,Immunoglobulin G ,Recombinant DNA ,biology.protein ,Cytokines ,Molecular Medicine ,Female ,DNA construct ,Antibody ,Genetic Engineering ,Peptides ,DNA ,Plasmids ,Single-Chain Antibodies - Abstract
Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by the development of self-reactive B and T cells and autoantibody production. In particular, double-stranded DNA-specific B cells play an important role in lupus progression, and their selective elimination is a reasonable approach for effective therapy of SLE. DNA-based vaccines aim at the induction of immune response against the vector-encoded antigen. Here, we are exploring, as a new DNA-based therapy of SLE, a chimeric DNA molecule encoding a DNA-mimotope peptide, and the Fv but not the immunogenic Fc fragment of an FcγRIIb-specific monoclonal antibody. This DNA construct was inserted in the expression vector pNut and used as a naked DNA vaccine in a mouse model of lupus. The chimeric DNA molecule can be expressed in eukaryotic cells and cross-links cell surface receptors on DNA-specific B cells, delivering an inhibitory intracellular signal. Intramuscular administration of the recombinant DNA molecule to lupus-prone MRL/lpr mice prevented increase in IgG anti-DNA antibodies and was associated with a low degree of proteinuria, modulation of cytokine profile, and suppression of lupus nephritis.
- Published
- 2012
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