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Replicating viral vector platform exploits alarmin signals for potent CD8+ T cell-mediated tumour immunotherapy.

Nat Commun. 2017; 
Kallert SM, Darbre S, Bonilla WV, Kreutzfeldt M,, Page N, Müller P, Kreuzaler M, Lu M, Favre S, Kreppel F, Löhning M,, Luther SA, Zippelius A,, Merkler D,, Pinschewer DD.
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Gene Synthesis To create a Srec#1 expression plasmid, we substituted the IGR in pol-I-S-GPCtag for a synthetic cDNA fragment (Genscript) as described in Supplementary Fig. Get A Quote

摘要

Viral infections lead to alarmin release and elicit potent cytotoxic effector T lymphocyte (CTLeff) responses. Conversely, the induction of protective tumour-specific CTLeff and their recruitment into the tumour remain challenging tasks. Here we show that lymphocytic choriomeningitis virus (LCMV) can be engineered to serve as a replication competent, stably-attenuated immunotherapy vector (artLCMV). artLCMV delivers tumour-associated antigens to dendritic cells for efficient CTL priming. Unlike replication-deficient vectors, artLCMV targets also lymphoid tissue stroma cells expressing the alarmin interleukin-33. By triggering interleukin-33 signals, artLCMV elicits CTLeff responses of higher magnitude and funct... More

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