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Mechanisms of Nanoparticle Mediated siRNA Transfection by Melittin-Derived Peptides

ACS Nano.. 2013-09; 
Hou KK, Pan H, Ratner L, Schlesinger PH, Wickline SA. Department of Cell Biology and Physiology, Washington University School of Medicine, St.Louis, MO. 63108, USA.
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Abstract

Traditional peptide-mediated siRNA transfection via peptide transduction domains exhibits limited cytoplasmic delivery of siRNA due to endosomal entrapment. This work overcomes these limitations with the use of membrane-destabilizing peptides derived from melittin for the knockdown of NFkB signaling in a model of adult T-Cell leukemia/lymphoma. While the mechanism of siRNA delivery into the cytoplasmic compartment by peptide transduction domains has not been well studied, our analysis of melittin derivatives indicates that concurrent nanocomplex disassembly and peptide-mediated endosomolysis are crucial to siRNA transfection. Importantly, in the case of the most active derivative, p5RHH, this process is initiat... More

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