Issue 26, 2021
From the journal:

Journal of Materials Chemistry B

Understanding selectivity of metabolic labelling and click-targeting in multicellular environments as a route to tissue selective drug delivery

Angel Tan, ORCID logo *abc   Qingtao Liu,a   Dedy Septiadi,c   Shuiling Chu,c   Tianqing Liu,d   Sarah-Jane Richards, ORCID logo e   Barbara Rothen-Rutishauser, ORCID logo c   Alke Petri-Fink, ORCID logo c   Matthew I. Gibson ORCID logo ef  and  Ben J. Boyd ORCID logo *ab  

* Corresponding authors

a Drug Delivery, Disposition and Dynamics, Monash Institute of Pharmaceutical Sciences, Monash University, Parkville Campus, VIC 3052, Australia
E-mail: angel.tan@monash.edu, ben.boyd@monash.edu

b ARC Centre of Excellence in Convergent Bio-Nano Science and Technology, Monash University, Parkville, VIC 3052, Australia

c Adolphe Merkle Institute, University of Fribourg, Chemin des Verdiers 4, 1700 Fribourg, Switzerland

d NICM Health Research Institute, Western Sydney University, Westmead, NSW 2145, Australia

e Department of Chemistry, University of Warwick, Gibbet Hill Road, Coventry, UK

f Warwick Medical School, University of Warwick, Coventry, UK

Abstract

Cancer cells generally exhibit higher metabolic demands relative to that of normal tissue cells. This offers great possibilities to exploit metabolic glycoengineering in combination with bio-orthogonal chemistry reactions to achieve tumour site-targeted therapeutic delivery. This work addresses the selectivity of metabolic glycan labelling in diseased (i.e., cancer) versus normal cells grown in a multicellular environment. Dibenzocylooctyne (DBCO)-bearing acetylated-D-mannosamine (Ac4ManNDBCO) was synthesised to metabolically label three different types of cell lines originating from the human lung tissues: A549 adenocarcinomic alveolar basal epithelial cells, MeT5A non-cancerous mesothelial cells, and MRC5 non-cancerous fibroblasts. These cell lines displayed different labelling sensitivity, which trended with their doubling time in the following order: A549 ≈ MeT5A > MRC5. The higher metabolic labelling efficiency inherently led to a higher extent of specific binding and accumulation of the clickable N3-conjugated gold nanoparticles (N3-AuNps, core diameter = 30 nm) in the DBCO–glycan modified A549 and MeT5A cells, but to a less prominent effect in MRC5 cells. These findings demonstrate that relative rates of cell metabolism can be exploited using metabolic labelling to recruit nanotherapeutics whilst minimising non-specific targeting of surrounding tissues.

Graphical abstract: Understanding selectivity of metabolic labelling and click-targeting in multicellular environments as a route to tissue selective drug delivery

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Article information

DOI
https://doi.org/10.1039/D1TB00721A
Article type
Paper
Submitted
01 Apr 2021
Accepted
07 Jun 2021
First published
22 Jun 2021

J. Mater. Chem. B, 2021,9, 5365-5373

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Understanding selectivity of metabolic labelling and click-targeting in multicellular environments as a route to tissue selective drug delivery

A. Tan, Q. Liu, D. Septiadi, S. Chu, T. Liu, S. Richards, B. Rothen-Rutishauser, A. Petri-Fink, M. I. Gibson and B. J. Boyd, J. Mater. Chem. B, 2021, 9, 5365 DOI: 10.1039/D1TB00721A

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