High-throughput screening identification of novel immunomodulatory combinations for the generation of tolerogenic dendritic cells

高通量筛选鉴定用于产生耐受性树突状细胞的新型免疫调节组合

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作者:Sihan Jia #, Jeremiah Kim #, Aaron Palmer Esser-Kahn, Peter Deak

Discussion

These second-generation PPI formulations have significant potential to generate robust tolDCs and strong antigen specific Tregs.

Methods

Over 40,000 combinations of pathogen-associated molecular patterns (PAMPs) and immunomodulatory small molecules were screened using a modified murine macrophage line, RAW dual cells, to observe the effect of these combinations on two major immune regulatory transcription factors, NF-κB and IRF. Combinations were further screened for inflammatory cytokine activity using a human monocyte cell line, THP-1, then on murine DCs. Leading candidates were co-cultured with T cells to assess antigen specific T cell responses.

Results

From this data, we identified 355 combinations that showed low or moderate IRF activity, low NF-κB activity, low inflammatory cytokine generation and good viability: all hallmarks of tolerogenic potential. We further screened these 355 combinations using bone marrow derived DCs (BMDCs) and identified 10 combinations that demonstrated high IL-10 (tolerogenic) and low TNF-α (inflammatory) secretion. After further optimizing these combinations, we identified two combinations that generate robust tolDCs from BMDCs ex vivo. We further show that these PPI-tolDCs can also generate antigen specific Tregs but do not increase overall Treg populations.

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