Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications

PR-104A is a dual hypoxia/nitroreductase gene therapy prodrug by virtue of its ability to undergo either one- or two-electron reduction to its cytotoxic species. It has been evaluated extensively in pre-clinical GDEPT studies, yet off-target human aldo-keto reductase AKR1C3-mediated activation has l...

Descripción completa

Detalles Bibliográficos
Autores principales: Ashoorzadeh, Amir, Mowday, Alexandra M., Guise, Christopher P., Silva, Shevan, Bull, Matthew R., Abbattista, Maria R., Copp, Janine N., Williams, Elsie M., Ackerley, David F., Patterson, Adam V., Smaill, Jeff B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8877822/
https://www.ncbi.nlm.nih.gov/pubmed/35215297
http://dx.doi.org/10.3390/ph15020185
_version_ 1784658510029520896
author Ashoorzadeh, Amir
Mowday, Alexandra M.
Guise, Christopher P.
Silva, Shevan
Bull, Matthew R.
Abbattista, Maria R.
Copp, Janine N.
Williams, Elsie M.
Ackerley, David F.
Patterson, Adam V.
Smaill, Jeff B.
author_facet Ashoorzadeh, Amir
Mowday, Alexandra M.
Guise, Christopher P.
Silva, Shevan
Bull, Matthew R.
Abbattista, Maria R.
Copp, Janine N.
Williams, Elsie M.
Ackerley, David F.
Patterson, Adam V.
Smaill, Jeff B.
author_sort Ashoorzadeh, Amir
collection PubMed
description PR-104A is a dual hypoxia/nitroreductase gene therapy prodrug by virtue of its ability to undergo either one- or two-electron reduction to its cytotoxic species. It has been evaluated extensively in pre-clinical GDEPT studies, yet off-target human aldo-keto reductase AKR1C3-mediated activation has limited its use. Re-evaluation of this chemical scaffold has previously identified SN29176 as an improved hypoxia-activated prodrug analogue of PR-104A that is free from AKR1C3 activation. However, optimization of the bystander effect of SN29176 is required for use in a GDEPT setting to compensate for the non-uniform distribution of therapeutic gene transfer that is often observed with current gene therapy vectors. A lipophilic series of eight analogues were synthesized from commercially available 3,4-difluorobenzaldehyde. Calculated octanol-water partition coefficients (LogD(7.4)) spanned > 2 orders of magnitude. 2D anti-proliferative and 3D multicellular layer assays were performed using isogenic HCT116 cells expressing E. coli NfsA nitroreductase (NfsA_Ec) or AKR1C3 to determine enzyme activity and measure bystander effect. A variation in potency for NfsA_Ec was observed, while all prodrugs appeared AKR1C3-resistant by 2D assay. However, 3D assays indicated that increasing prodrug lipophilicity correlated with increased AKR1C3 activation and NfsA_Ec activity, suggesting that metabolite loss from the cell of origin into media during 2D monolayer assays could mask cytotoxicity. Three prodrugs were identified as bono fide AKR1C3-negative candidates whilst maintaining activity with NfsA_Ec. These were converted to their phosphate ester pre-prodrugs before being taken forward into in vivo therapeutic efficacy studies. Ultimately, 2-(5-(bis(2-bromoethyl)amino)-4-(ethylsulfonyl)-N-methyl-2-nitrobenzamido)ethyl dihydrogen phosphate possessed a significant 156% improvement in median survival in mixed NfsA_Ec/WT tumors compared to untreated controls (p = 0.005), whilst still maintaining hypoxia selectivity comparable to PR-104A.
format Online
Article
Text
id pubmed-8877822
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-88778222022-02-26 Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications Ashoorzadeh, Amir Mowday, Alexandra M. Guise, Christopher P. Silva, Shevan Bull, Matthew R. Abbattista, Maria R. Copp, Janine N. Williams, Elsie M. Ackerley, David F. Patterson, Adam V. Smaill, Jeff B. Pharmaceuticals (Basel) Article PR-104A is a dual hypoxia/nitroreductase gene therapy prodrug by virtue of its ability to undergo either one- or two-electron reduction to its cytotoxic species. It has been evaluated extensively in pre-clinical GDEPT studies, yet off-target human aldo-keto reductase AKR1C3-mediated activation has limited its use. Re-evaluation of this chemical scaffold has previously identified SN29176 as an improved hypoxia-activated prodrug analogue of PR-104A that is free from AKR1C3 activation. However, optimization of the bystander effect of SN29176 is required for use in a GDEPT setting to compensate for the non-uniform distribution of therapeutic gene transfer that is often observed with current gene therapy vectors. A lipophilic series of eight analogues were synthesized from commercially available 3,4-difluorobenzaldehyde. Calculated octanol-water partition coefficients (LogD(7.4)) spanned > 2 orders of magnitude. 2D anti-proliferative and 3D multicellular layer assays were performed using isogenic HCT116 cells expressing E. coli NfsA nitroreductase (NfsA_Ec) or AKR1C3 to determine enzyme activity and measure bystander effect. A variation in potency for NfsA_Ec was observed, while all prodrugs appeared AKR1C3-resistant by 2D assay. However, 3D assays indicated that increasing prodrug lipophilicity correlated with increased AKR1C3 activation and NfsA_Ec activity, suggesting that metabolite loss from the cell of origin into media during 2D monolayer assays could mask cytotoxicity. Three prodrugs were identified as bono fide AKR1C3-negative candidates whilst maintaining activity with NfsA_Ec. These were converted to their phosphate ester pre-prodrugs before being taken forward into in vivo therapeutic efficacy studies. Ultimately, 2-(5-(bis(2-bromoethyl)amino)-4-(ethylsulfonyl)-N-methyl-2-nitrobenzamido)ethyl dihydrogen phosphate possessed a significant 156% improvement in median survival in mixed NfsA_Ec/WT tumors compared to untreated controls (p = 0.005), whilst still maintaining hypoxia selectivity comparable to PR-104A. MDPI 2022-02-01 /pmc/articles/PMC8877822/ /pubmed/35215297 http://dx.doi.org/10.3390/ph15020185 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Ashoorzadeh, Amir
Mowday, Alexandra M.
Guise, Christopher P.
Silva, Shevan
Bull, Matthew R.
Abbattista, Maria R.
Copp, Janine N.
Williams, Elsie M.
Ackerley, David F.
Patterson, Adam V.
Smaill, Jeff B.
Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications
title Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications
title_full Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications
title_fullStr Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications
title_full_unstemmed Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications
title_short Interrogation of the Structure–Activity Relationship of a Lipophilic Nitroaromatic Prodrug Series Designed for Cancer Gene Therapy Applications
title_sort interrogation of the structure–activity relationship of a lipophilic nitroaromatic prodrug series designed for cancer gene therapy applications
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8877822/
https://www.ncbi.nlm.nih.gov/pubmed/35215297
http://dx.doi.org/10.3390/ph15020185
work_keys_str_mv AT ashoorzadehamir interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT mowdayalexandram interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT guisechristopherp interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT silvashevan interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT bullmatthewr interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT abbattistamariar interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT coppjaninen interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT williamselsiem interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT ackerleydavidf interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT pattersonadamv interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications
AT smailljeffb interrogationofthestructureactivityrelationshipofalipophilicnitroaromaticprodrugseriesdesignedforcancergenetherapyapplications

Ejemplares similares