B14 - Defining predictors of anti-viral immunity in the yellow fever vaccination model using gene polymorphisms and early innate response patterns

Cooperation of multiple nucleic acid sensors and antigen presenting cell (APC) subpopulations is thought to be critical for generating effective and long-lasting adaptive immunity to infection and vaccination. We use the live-attenuated yellow fever virus (YF17D) vaccination as a model of an acute self-limiting RNA virus infection in humans. We will apply (expression) quantitative trait loci (eQTL) analysis and single cell transciptome and epigenome analysis of circulating innate immune cells before and after YF17D vaccination. Thereby we will identify new factors that regulate nucleic acid sensing pathways and decipher the genetic basis of inter-individual variability in antiviral immunity.

Prof. Dr. Anne Krug Biomedical Center Munich (BMC), LMU Munich +49 (0)89 2180 - 75646 anne.krug@med.lmu.de External web links: Research webpage and CV	Prof. Dr. Simon Rothenfußer LMU Hospital, LMU Munich +49 (0)89 4400-57321 simon.rothenfusser@med.uni-muenchen.de External web links: Research webpage
Sandra Riemer Biomedical Center Munich (BMC), LMU Munich Sandra.Riemer@med.uni-muenchen.de	Magdalena Zaucha LMU Hospital, LMU Munich Magdalena.Zaucha@med.uni-muenchen.de

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B14 - Defining predictors of anti-viral immunity in the yellow fever vaccination model using gene polymorphisms and early innate response patterns

Prof. Dr. Anne Krug

Prof. Dr. Simon Rothenfußer

Sandra Riemer

Magdalena Zaucha

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