4.8 Article

Lipopeptisomes: Anticancer peptide-assembled particles for fusolytic oncotherapy

Journal

ACTA BIOMATERIALIA
Volume 80, Issue -, Pages 269-277

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.actbio.2018.09.025

Keywords

Peptide; Self-assembly; Drug delivery; Nanomedicine

Funding

  1. Pennsylvania State University
  2. Penn State Schreyer Honors College Independent Research Grant
  3. Penn State Student Engagement Network Grant

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Anticancer peptides (ACPs) are cationic amphiphiles that preferentially kill cancer cells through folding dependent membrane disruption. Although ACPs represent attractive therapeutic candidates, particularly against drug-resistant cancers, their successful translation into clinical practice has gone unrealized due to their poor bioavailability, serum instability and, most importantly, severe hemolytic toxicity. Here, we exploit the membrane-specific interactions of ACPs to prepare a new class of peptide-lipid particle, we term a lipopeptisome (LP). This design sequesters loaded ACPs within a lipid lamellar corona to avoid contact with red blood cells and healthy tissues, while affording potent lytic destruction of cancer cells following LP-membrane fusion. Biophysical studies show ACPs rapidly fold at, and integrate into, liposomal membranes to form stable LPs with high loading efficiencies (>80%). Rational design of the particles to possess lipid combinations mimicking that of the aberrant cancer cell outer leaflet allows LPs to rapidly fuse with tumor cell membranes and afford localized assembly of loaded ACPs within the bilayer. This leads to preferential fusolytic killing of cancer cells with minimal collateral toxicity towards non-cancerous cells and erythrocytes, thereby imparting clinically relevant therapeutic indices to otherwise toxic ACPs. Thus, integration of ACPs into self-assembled LPs represents a new delivery strategy to improve the therapeutic utility of oncolytic agents, and suggests this technology may be added to targeted combinatorial approaches in precision medicine. (C) 2018 Acta Materialia Inc. Published by Elsevier Ltd. All rights reserved.

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