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IFN-alpha and 5-Aza-2-deoxycytidine enhance the anti-tumor efficacy of a dendritic-cell targeting MIP3alpha-Gp100-Trp2 DNA vaccine by affecting T-cell recruitment …

biorxiv. 2019; 
View James T. Gordy,  Kun Luo,   View Richard B. Markham
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PCR Cloning and Subcloning The original plasmid encoded the MIP3α-hgp100 fusion sequence, where the antigen includes amino acids 25-235 of human gp100, as described4. A vaccine of mouse MIP3α fused to the combined antigens construct consisting of the hgp100 construct and mouse tyrosinase-related protein 2 (Trp2, amino acids 170-269) was created. The region of Trp2 included a 5’ spacer region (amino acids MEFNDAQAPKSLEA) and was flanked by XbaI restriction sites. This construct was synthesized by Genscript Biotech Corp (Piscataway Township, NJ) in the pUC57 cloning vector. Get A Quote

摘要

Background The chemokine MIP-3α (CCL20) binds to CCR6 found on immature dendritic cells. DNA vaccines fusing MIP-3α to melanoma-associated antigens have shown improved efficacy and immunogenicity in the B16F10 model. To optimize the therapy, our laboratory has added agents designed to overcome immunoregulatory mechanisms of the tumor microenvironment. Here, we report that the combination of type-I interferon therapy (IFNα) with 5-Aza-2’-deoxycitidine (Aza) profoundly enhanced the therapeutic anti-melanoma efficacy of a MIP-3α-Gp100-Trp2 DNA vaccine. Methods The current studies utilize the B16F10 syngeneic mouse melanoma model. The vaccine is administered intramuscularly (i.m.) followed by i.m. electropor... More

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