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Literature DB >> 27161484

The Late Endosome and Its Lipid BMP Act as Gateways for Efficient Cytosolic Access of the Delivery Agent dfTAT and Its Macromolecular Cargos.

Alfredo Erazo-Oliveras¹, Kristina Najjar¹, Dat Truong¹, Ting-Yi Wang¹, Dakota J Brock¹, Austin R Prater¹, Jean-Philippe Pellois².

Abstract

Endosomal entrapment is a severely limiting bottleneck in the delivery of biologics into cells. The compound dfTAT was recently found to circumvent this problem by mediating endosomal leakage efficiently and without toxicity. Herein, we report on the mechanism of endosomal escape of this cell-penetrating peptide. By modulating the trafficking of the peptide within the endocytic pathway, we identify late endosomes as the organelles rendered leaky by dfTAT. We establish that dfTAT binds bis(monoacylglycero)phosphate (BMP), a lipid found in late endosomes, and that the peptide causes the fusion and leakage of bilayers containing BMP. Together, these data identify late endosomes as desirable gateways for cell penetration and BMP as a cellular factor that can be exploited for the development of future delivery agents.

Entities: Chemical Disease Gene Mutation Species

Keywords: cellular delivery; endosomal escape; figubis(monoacylglycero)phosphate; late endosomes; membrane leakage

Mesh：

Substances：

Year: 2016 PMID： 27161484 PMCID： PMC4874899 DOI： 10.1016/j.chembiol.2016.03.016

Source DB: PubMed Journal: Cell Chem Biol ISSN： 2451-9448 Impact factor: 8.116

62 in total

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Authors: Alfredo Erazo-Oliveras; Kristina Najjar; Laila Dayani; Ting-Yi Wang; Gregory A Johnson; Jean-Philippe Pellois
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24 in total

1. An l- to d-Amino Acid Conversion in an Endosomolytic Analog of the Cell-penetrating Peptide TAT Influences Proteolytic Stability, Endocytic Uptake, and Endosomal Escape.

Authors: Kristina Najjar; Alfredo Erazo-Oliveras; Dakota J Brock; Ting-Yi Wang; Jean-Philippe Pellois
Journal: J Biol Chem Date: 2016-12-06 Impact factor: 5.157

2. Cytosolic Delivery of Macromolecules in Live Human Cells Using the Combined Endosomal Escape Activities of a Small Molecule and Cell Penetrating Peptides.

Authors: Jason Allen; Kristina Najjar; Alfredo Erazo-Oliveras; Helena M Kondow-McConaghy; Dakota J Brock; Kristin Graham; Elizabeth C Hager; Andrea L J Marschall; Stefan Dübel; Rudolph L Juliano; Jean-Philippe Pellois
Journal: ACS Chem Biol Date: 2019-10-31 Impact factor: 5.100

The Late Endosome and Its Lipid BMP Act as Gateways for Efficient Cytosolic Access of the Delivery Agent dfTAT and Its Macromolecular Cargos.

Review 1. Rab proteins as membrane organizers.

2. Generation of endosomolytic reagents by branching of cell-penetrating peptides: tools for the delivery of bioactive compounds to live cells in cis or trans.

3. Role of the small GTPase Rab7 in the late endocytic pathway.

4. Endosome-to-cytosol transport of viral nucleocapsids.

Review 5. The distribution and function of phosphatidylserine in cellular membranes.

6. Rab11 regulates recycling through the pericentriolar recycling endosome.

Review 7. Cell-surface proteoglycans as molecular portals for cationic peptide and polymer entry into cells.

8. Rab7 associates with early endosomes to mediate sorting and transport of Semliki forest virus to late endosomes.

Review 9. Twenty years of cell-penetrating peptides: from molecular mechanisms to therapeutics.

10. Protein delivery into live cells by incubation with an endosomolytic agent.

1. An l- to d-Amino Acid Conversion in an Endosomolytic Analog of the Cell-penetrating Peptide TAT Influences Proteolytic Stability, Endocytic Uptake, and Endosomal Escape.

2. Cytosolic Delivery of Macromolecules in Live Human Cells Using the Combined Endosomal Escape Activities of a Small Molecule and Cell Penetrating Peptides.

Review 3. Endosomal Escape and Cytosolic Penetration of Macromolecules Mediated by Synthetic Delivery Agents.

4. HOPS-dependent endosomal fusion required for efficient cytosolic delivery of therapeutic peptides and small proteins.

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10. Impact of the Endosomal Escape Activity of Cell-Penetrating Peptides on the Endocytic Pathway.