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Conditional silencing of H-2Db class I molecule expression on dendritic cells modulates the protective and pathogenic kinetics of virus-antigen specific CD8 T cell …

biorxiv. 2019; 
Zachariah P. Tritz, Robin C. Orozco, Courtney S. Malo, Lila T Yokanovich, Katayoun Ayasoufi, Cori E. Fain, Roman H. Khadka, Megan L. Settell, Mike J. Hansen, Fang Jin, Aaron J Johnson
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Peptide Synthesis  Mice were euthanized for flow cytometric analysis, or induced to undergo PIFS, at 7, 14, or 28 dpi. The PIFS model employed by our group involves the tail vein injection of 100μL of a 1mg/mL solution of VP2121-130 peptide (FHAGSLLVFM) in PBS at either 7 or 14 days after the original TMEV infection (GenScript, Nanjing) [38-43]. Animals were observed until they became visibly distressed (hunched and unresponsive), and then were injected via tail vein with 100μL of a 100mg/mL FITC-albumin solution in PBS (Sigma-Aldrich, St. Louis, MO).  Get A Quote

摘要

Theiler’s murine encephalomyelitis virus (TMEV) infection of the central nervous system is rapidly cleared in C57BL/6 mice by an anti-viral CD8 T cell response restricted by the MHC class I molecule, H-2Db. While the CD8 T cell response against neurotropic viruses is well characterized, the identity and function of the antigen presenting cell(s) involved in this process is(are) less well defined. To address this gap in knowledge, we developed a novel C57BL/6 H-2Db conditional knockout mouse that expresses an H-2Db transgene in which the transmembrane domain locus is flanked by LoxP sites. We crossed these H-2Db LoxP mice with MHC class I-deficient mice expressing Cre-recombinase under either the CD11c or L... More

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