Issue 47, 2021

Bacteriophage PRD1 as a nanoscaffold for drug loading

Abstract

Viruses are very attractive biomaterials owing to their capability as nanocarriers of genetic material. Efforts have been made to functionalize self-assembling viral protein capsids on their exterior or interior to selectively take up different payloads. PRD1 is a double-stranded DNA bacteriophage comprising an icosahedral protein outer capsid and an inner lipidic vesicle. Here, we report the three-dimensional structure of PRD1 in complex with the antipsychotic drug chlorpromazine (CPZ) by cryo-electron microscopy. We show that the jellyrolls of the viral major capsid protein P3, protruding outwards from the capsid shell, serve as scaffolds for loading heterocyclic CPZ molecules. Additional X-ray studies and molecular dynamics simulations show the binding modes and organization of CPZ molecules when complexed with P3 only and onto the virion surface. Collectively, we provide a proof of concept for the possible use of the lattice-like organisation and the quasi-symmetric morphology of virus capsomers for loading heterocyclic drugs with defined properties.

Graphical abstract: Bacteriophage PRD1 as a nanoscaffold for drug loading

Supplementary files

Article information

Article type
Communication
Submitted
27 Jun 2021
Accepted
06 Nov 2021
First published
01 Dec 2021
This article is Open Access
Creative Commons BY license

Nanoscale, 2021,13, 19875-19883

Bacteriophage PRD1 as a nanoscaffold for drug loading

H. M. E. Duyvesteyn, I. Santos-Pérez, F. Peccati, A. Martinez-Castillo, T. S. Walter, D. Reguera, F. M. Goñi, G. Jiménez-Osés, H. M. Oksanen, D. I. Stuart and N. G. A. Abrescia, Nanoscale, 2021, 13, 19875 DOI: 10.1039/D1NR04153C

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