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Cellular Uptake of A Taurine-Modified, Ester Bond-Decorated D-Peptide Derivative via Dynamin-Based Endocytosis and Macropinocytosis. | LitMetric

AI Article Synopsis

  • Most peptides usually have positive charges to help with cellular uptake, but a study found that taurine, which has negative charges, can enhance the uptake of D-peptides when linked via an ester bond.
  • Taurine promotes D-peptide self-assembly into nanofibers, reducing efflux and boosting intracellular accumulation, with evidence showing that blocking enzymes related to this process hinders uptake in mammalian cells.
  • Further research used knockout mice and Drosophila to confirm that multiple endocytosis pathways are involved in the uptake process, with electron microscopy revealing increased vesicle numbers inside cells due to the formation of aggregates at the cell surface.

Article Abstract

Most of the peptides used for promoting cellular uptake bear positive charges. In our previous study, we reported an example of taurine (bearing negative charges in physiological conditions) promoting cellular uptake of D-peptides. Taurine, conjugated to a small D-peptide via an ester bond, promotes the cellular uptake of this D-peptide. Particularly, intracellular carboxylesterase (CES) instructs the D-peptide to self-assemble and to form nanofibers, which largely disfavors efflux and further enhances the intracellular accumulation of the D-peptide, as supported by that the addition of CES inhibitors partially impaired cellular uptake of this molecule in mammalian cell lines. Using dynamin 1, 2, and 3 triple knockout (TKO) mouse fibroblasts, we demonstrated that cells took up this molecule via macropinocytosis and dynamin-dependent endocytosis. Imaging of Drosophila larval blood cells derived from endocytic mutants confirmed the involvement of multiple endocytosis pathways. Electron microscopy (EM) indicated that the precursors can form aggregates on the cell surface to facilitate the cellular uptake via macropinocytosis. EM also revealed significantly increased numbers of vesicles in the cytosol. This work provides new insights into the cellular uptake of taurine derivative for intracellular delivery and self-assembly of D-peptides.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5835119PMC
http://dx.doi.org/10.1016/j.ymthe.2017.11.020DOI Listing

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