2010
DOI: 10.1515/bc.2010.132
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The C2-streptavidin delivery system promotes the uptake of biotinylated molecules in macrophages and T-leukemia cells

Abstract: Macrophages are tightly associated with inflammatory diseases as well as carcinogenesis, and therefore represent promising targets for drug delivery and gene transfer. We have recently established a novel protein delivery system based on the binary C2 toxin of Clostridium botulinum and streptavidin, allowing the uptake of exogenous biotinylated molecules into mammalian cells. Here, we applied this C2-streptavidin delivery system to macrophages and other leukocytes. First, the effect of wild-type C2 toxin on di… Show more

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Cited by 17 publications
(16 citation statements)
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“…GST-C2IN-p53 accumulated in the cytosol after 5 h, but was no longer detectable after 24 h (data not shown). In consistency, a cytosolic degradation has also been reported for other C2IN-based fusion proteins, such as C2IN-C3 [36], C2IN-SpvB [37] and C2IN-streptavidin [38]. Upon internalization into HeLa and A549 cells GST-C2IN-p53 was primarily detected in the cytoplasm and less prominently in the nucleus as observed by confocal microscopy.…”
Section: Discussionsupporting
confidence: 79%
“…GST-C2IN-p53 accumulated in the cytosol after 5 h, but was no longer detectable after 24 h (data not shown). In consistency, a cytosolic degradation has also been reported for other C2IN-based fusion proteins, such as C2IN-C3 [36], C2IN-SpvB [37] and C2IN-streptavidin [38]. Upon internalization into HeLa and A549 cells GST-C2IN-p53 was primarily detected in the cytoplasm and less prominently in the nucleus as observed by confocal microscopy.…”
Section: Discussionsupporting
confidence: 79%
“…Mutants of our study may not able to catalyze ADP-ribosylation reaction owing to their poor ligand efficiency and binding affinity of NAD + to the binding core. Enzyme deficient mutants of these toxins have been used as drug delivery systems and molecular tools for studying many pathophysiological mechanisms, but no one has been evaluated them as vaccine candidates (Dmochewitz et al, 2013;Fahrer et al, 2010aFahrer et al, , 2010bRohrbeck et al, 2012). A single amino acid substitution/mutation reported as an evolutionary constraint that can change antigenicity of many bacterial and viral antigens (Foley, 2015;Koide et al, 2005;Liang et al, 2010;Meyer and Wilke, 2015;Yoo and Deregt, 2001).…”
Section: Discussionmentioning
confidence: 99%
“…Many of the reported examples, which mainly consist of the chimeric toxins constructed on the basis of the active component of C2 toxin, C2I are intensively reviewed elsewhere [9,318]. More recent reports describe genetically engineered chimeric C2IN-streptavidin complexes, which were designed to delivered biotin-labeled molecules into the cytosol of diverse eukaryotic cell lines by the binding/translocation subunit of the toxin [361,362,363]. The C2-streptavidin delivery system was used to internalize biotin-labeled p53 tumor suppressor into different mammalian cell lines, including human tumor cells [364].…”
Section: Discussionmentioning
confidence: 99%