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• W2028838686 abstract "CD95, TNFR1, TRAILR1 and TRAILR2 belong to a subgroup of TNF receptors which is characterized by a conserved cell death-inducing protein domain that connects these receptors to the apoptotic machinery of the cell. Activation of death receptors in malignant cells attracts increasing attention as a principle to fight cancer. Besides agonistic antibodies the major way to stimulate death receptors is the use of their naturally occurring death ligands CD95L, TNF and TRAIL. However, dependent from the concept followed to develop a death ligand-based therapy various limiting aspects have to be taken into consideration on the way to a bedside usable drug. Problems arise in particular from the cell associated transmembrane nature of the death ligands, the poor serum half life of the soluble fragments derived from the transmembrane ligands, the ubiquitous expression of the death receptors and the existence of additional non-death receptors of the death ligands. Here, we summarize strategies how these limitations can be overcome by genetic engineering." @default.
• W2028838686 created "2016-06-24" @default.
• W2028838686 creator A5041346050 @default.
• W2028838686 creator A5041527718 @default.
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• W2028838686 date "2013-05-01" @default.
• W2028838686 modified "2023-09-27" @default.
• W2028838686 title "Engineering death receptor ligands for cancer therapy" @default.
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• W2028838686 doi "https://doi.org/10.1016/j.canlet.2010.12.019" @default.
• W2028838686 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/21236560" @default.
• W2028838686 hasPublicationYear "2013" @default.
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