Tools to enable the study and translation of supramolecular amphiphiles
Tools to enable the study and translation of supramolecular amphiphiles
This tutorial review focuses on providing a summary of the key techniques used for the characterisation of supramolecular amphiphiles and their self-assembled aggregates; from the understanding of low-level molecular interactions, to materials analysis, use of data to support computer-aided molecular design and finally, the translation of this class of compounds for real world application, specifically within the clinical setting. We highlight the common methodologies used for the study of traditional amphiphiles and build to provide specific examples that enable the study of specialist supramolecular systems. This includes the use of nuclear magnetic resonance spectroscopy, mass spectrometry, X-ray scattering techniques (small- and wide-angle X-ray scattering and single crystal X-ray diffraction), critical aggregation (or micelle) concentration determination methodologies, machine learning, and various microscopy techniques. Furthermore, this review provides guidance for working with supramolecular amphiphiles in in vitro and in vivo settings, as well as the use of accessible software programs, to facilitate screening and selection of druggable molecules. Each section provides: a methodology overview - information that may be derived from the use of the methodology described; a case study - examples for the application of these methodologies; and a summary section - providing methodology specific benefits, limitations and future applications.
6892-6917
Allam, Thomas
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Balderston, Dominick E.
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Chahal, Mandeep K.
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Hilton, Kira L.F.
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Hind, Charlotte K.
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Keers, Olivia B.
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Lilley, Rebecca J.
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Manwani, Chandni
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Overton, Alix
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Popoola, Precious I.A.
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Thompson, Lisa R.
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White, Lisa J.
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Hiscock, Jennifer R.
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Allam, Thomas
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Balderston, Dominick E.
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Chahal, Mandeep K.
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Hilton, Kira L.F.
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Hind, Charlotte K.
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Keers, Olivia B.
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Lilley, Rebecca J.
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Manwani, Chandni
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Overton, Alix
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Popoola, Precious I.A.
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Thompson, Lisa R.
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White, Lisa J.
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Hiscock, Jennifer R.
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Allam, Thomas, Balderston, Dominick E., Chahal, Mandeep K., Hilton, Kira L.F., Hind, Charlotte K., Keers, Olivia B., Lilley, Rebecca J., Manwani, Chandni, Overton, Alix, Popoola, Precious I.A., Thompson, Lisa R., White, Lisa J. and Hiscock, Jennifer R.
(2023)
Tools to enable the study and translation of supramolecular amphiphiles.
Chemical Society Reviews, 52 (20), .
(doi:10.1039/d3cs00480e).
Abstract
This tutorial review focuses on providing a summary of the key techniques used for the characterisation of supramolecular amphiphiles and their self-assembled aggregates; from the understanding of low-level molecular interactions, to materials analysis, use of data to support computer-aided molecular design and finally, the translation of this class of compounds for real world application, specifically within the clinical setting. We highlight the common methodologies used for the study of traditional amphiphiles and build to provide specific examples that enable the study of specialist supramolecular systems. This includes the use of nuclear magnetic resonance spectroscopy, mass spectrometry, X-ray scattering techniques (small- and wide-angle X-ray scattering and single crystal X-ray diffraction), critical aggregation (or micelle) concentration determination methodologies, machine learning, and various microscopy techniques. Furthermore, this review provides guidance for working with supramolecular amphiphiles in in vitro and in vivo settings, as well as the use of accessible software programs, to facilitate screening and selection of druggable molecules. Each section provides: a methodology overview - information that may be derived from the use of the methodology described; a case study - examples for the application of these methodologies; and a summary section - providing methodology specific benefits, limitations and future applications.
Text
d3cs00480e
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Submitted date: 19 June 2023
e-pub ahead of print date: 26 September 2023
Additional Information:
Funding Information:
The authors would like to thank Mariam Yacoub for her contribution towards making this review visually inclusive. TA would like to thank Prof. Jeremy Frey (University of Southampton), Prof. J. Mark Sutton (UKHSA) for PhD funding and supervisory support. RJL would like to thank Prof. Claire Peppiatt-Wildman (University of Kent) for supervisory support. CM, PIAP, OBK and LRT would like to thank Prof. Michelle Garrett (University of Kent) for supervisory support. DB, KLFH, PIAP, AO, RJL, LRT and JRH would like to thank the University of Kent for funding. CM would like to thank the Jane Irons Scholarship for funding. OBK would like to thank the SoCoBio DTP for funding. LRT would like to thank the Daphne Jackson Trust, BBSRC, AstraZeneca, UKHSA and Cancer Research Horizons for funding and support. LJW and JRH would like to thank the UKRI (MR/T020415/1) for funding.
Identifiers
Local EPrints ID: 483722
URI: http://eprints.soton.ac.uk/id/eprint/483722
ISSN: 0306-0012
PURE UUID: 703480cf-3a80-43d2-ab2c-0585fed611be
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Date deposited: 03 Nov 2023 18:00
Last modified: 05 Jun 2024 20:01
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Contributors
Author:
Thomas Allam
Author:
Dominick E. Balderston
Author:
Mandeep K. Chahal
Author:
Kira L.F. Hilton
Author:
Charlotte K. Hind
Author:
Olivia B. Keers
Author:
Rebecca J. Lilley
Author:
Chandni Manwani
Author:
Alix Overton
Author:
Precious I.A. Popoola
Author:
Lisa R. Thompson
Author:
Lisa J. White
Author:
Jennifer R. Hiscock
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