AI Article Synopsis

  • A variety of biological agents can disrupt lipid membranes, including amyloid aggregates, antimicrobial peptides, and venom compounds, which are important for both diseases and therapeutic technologies.
  • The text introduces synthetic, DNA-based particles that can disrupt lipid membranes, designed with a core for adhesion and a protective outer layer that can be removed to enhance membrane interaction.
  • These particles can increase the permeability of lipid vesicles, leading to vesicle collapse, and can also form DNA aggregates that can trap bacteria, mimicking the immune response of trapping pathogens.

Article Abstract

Biology has evolved a variety of agents capable of permeabilizing and disrupting lipid membranes, from amyloid aggregates, to antimicrobial peptides, to venom compounds. While often associated with disease or toxicity, these agents are also central to many biosensing and therapeutic technologies. Here, we introduce a class of synthetic, DNA-based particles capable of disrupting lipid membranes. The particles have finely programmable size, and self-assemble from all-DNA and cholesterol-DNA nanostructures, the latter forming a membrane-adhesive core and the former a protective hydrophilic corona. We show that the corona can be selectively displaced with a molecular cue, exposing the 'sticky' core. Unprotected particles adhere to synthetic lipid vesicles, which in turn enhances membrane permeability and leads to vesicle collapse. Furthermore, particle-particle coalescence leads to the formation of gel-like DNA aggregates that envelop surviving vesicles. This response is reminiscent of pathogen immobilisation through immune cells secretion of DNA networks, as we demonstrate by trapping E. coli bacteria.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8346484PMC
http://dx.doi.org/10.1038/s41467-021-24989-7DOI Listing

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