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Phase-separating peptides for direct cytosolic delivery and redox-activated release of macromolecular therapeutics
Phase-separating peptides for direct cytosolic delivery and redox-activated release of macromolecular therapeutics
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Phase-separating peptides for direct cytosolic delivery and redox-activated release of macromolecular therapeutics
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Phase-separating peptides for direct cytosolic delivery and redox-activated release of macromolecular therapeutics
Phase-separating peptides for direct cytosolic delivery and redox-activated release of macromolecular therapeutics
Journal Article

Phase-separating peptides for direct cytosolic delivery and redox-activated release of macromolecular therapeutics

2022
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Overview
Biomacromolecules are highly promising therapeutic modalities to treat various diseases. However, they suffer from poor cellular membrane permeability, limiting their access to intracellular targets. Strategies to overcome this challenge often employ nanoscale carriers that can get trapped in endosomal compartments. Here we report conjugated peptides that form pH- and redox-responsive coacervate microdroplets by liquid–liquid phase separation that readily cross the cell membrane. A wide range of macromolecules can be quickly recruited within the microdroplets, including small peptides, enzymes as large as 430 kDa and messenger RNAs (mRNAs). The therapeutic-loaded coacervates bypass classical endocytic pathways to enter the cytosol, where they undergo glutathione-mediated release of payload, the bioactivity of which is retained in the cell, while mRNAs exhibit a high transfection efficiency. These peptide coacervates represent a promising platform for the intracellular delivery of a large palette of macromolecular therapeutics that have potential for treating various pathologies (for example, cancers and metabolic diseases) or as carriers for mRNA-based vaccines. Coacervate microdroplets formed from pH- and redox-responsive peptides and self-assembled by liquid–liquid phase separation have been shown to quickly recruit macromolecular therapeutics—such as peptides, large proteins and mRNAs—and directly enter the cytosol of cells via a non-endocytic pathway. The subsequent release of therapeutic cargo is mediated by endogenic glutathione.