A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers

Novel anticancer drugs targeting key apoptosis regulators have been developed and are undergoing clinical trials. Pharmacodynamic biomarkers to define the optimum dose of drug that provokes tumor apoptosis are in demand; acquisition of longitudinal tumor biopsies is a significant challenge and minim...

Descripción completa

Detalles Bibliográficos
Autores principales: Simpson, K L, Cawthorne, C, Zhou, C, Hodgkinson, C L, Walker, M J, Trapani, F, Kadirvel, M, Brown, G, Dawson, M J, MacFarlane, M, Williams, K J, Whetton, A D, Dive, C
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2013
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3674346/
https://www.ncbi.nlm.nih.gov/pubmed/23640455
http://dx.doi.org/10.1038/cddis.2013.137
_version_ 1782272356853481472
author Simpson, K L
Cawthorne, C
Zhou, C
Hodgkinson, C L
Walker, M J
Trapani, F
Kadirvel, M
Brown, G
Dawson, M J
MacFarlane, M
Williams, K J
Whetton, A D
Dive, C
author_facet Simpson, K L
Cawthorne, C
Zhou, C
Hodgkinson, C L
Walker, M J
Trapani, F
Kadirvel, M
Brown, G
Dawson, M J
MacFarlane, M
Williams, K J
Whetton, A D
Dive, C
author_sort Simpson, K L
collection PubMed
description Novel anticancer drugs targeting key apoptosis regulators have been developed and are undergoing clinical trials. Pharmacodynamic biomarkers to define the optimum dose of drug that provokes tumor apoptosis are in demand; acquisition of longitudinal tumor biopsies is a significant challenge and minimally invasive biomarkers are required. Considering this, we have developed and validated a preclinical ‘death-switch' model for the discovery of secreted biomarkers of tumour apoptosis using in vitro proteomics and in vivo evaluation of the novel imaging probe [(18)F]ML-10 for non-invasive detection of apoptosis using positron emission tomography (PET). The ‘death-switch' is a constitutively active mutant caspase-3 that is robustly induced by doxycycline to drive synchronous apoptosis in human colorectal cancer cells in vitro or grown as tumor xenografts. Death-switch induction caused caspase-dependent apoptosis between 3 and 24 hours in vitro and regression of ‘death-switched' xenografts occurred within 24 h correlating with the percentage of apoptotic cells in tumor and levels of an established cell death biomarker (cleaved cytokeratin-18) in the blood. We sought to define secreted biomarkers of tumor apoptosis from cultured cells using Discovery Isobaric Tag proteomics, which may provide candidates to validate in blood. Early after caspase-3 activation, levels of normally secreted proteins were decreased (e.g. Gelsolin and Midkine) and proteins including CD44 and High Mobility Group protein B1 (HMGB1) that were released into cell culture media in vitro were also identified in the bloodstream of mice bearing death-switched tumors. We also exemplify the utility of the death-switch model for the validation of apoptotic imaging probes using [(18)F]ML-10, a PET tracer currently in clinical trials. Results showed increased tracer uptake of [(18)F]ML-10 in tumours undergoing apoptosis, compared with matched tumour controls imaged in the same animal. Overall, the death-switch model represents a robust and versatile tool for the discovery and validation of apoptosis biomarkers.
format Online
Article
Text
id pubmed-3674346
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Nature Publishing Group
record_format MEDLINE/PubMed
spelling pubmed-36743462013-06-06 A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers Simpson, K L Cawthorne, C Zhou, C Hodgkinson, C L Walker, M J Trapani, F Kadirvel, M Brown, G Dawson, M J MacFarlane, M Williams, K J Whetton, A D Dive, C Cell Death Dis Original Article Novel anticancer drugs targeting key apoptosis regulators have been developed and are undergoing clinical trials. Pharmacodynamic biomarkers to define the optimum dose of drug that provokes tumor apoptosis are in demand; acquisition of longitudinal tumor biopsies is a significant challenge and minimally invasive biomarkers are required. Considering this, we have developed and validated a preclinical ‘death-switch' model for the discovery of secreted biomarkers of tumour apoptosis using in vitro proteomics and in vivo evaluation of the novel imaging probe [(18)F]ML-10 for non-invasive detection of apoptosis using positron emission tomography (PET). The ‘death-switch' is a constitutively active mutant caspase-3 that is robustly induced by doxycycline to drive synchronous apoptosis in human colorectal cancer cells in vitro or grown as tumor xenografts. Death-switch induction caused caspase-dependent apoptosis between 3 and 24 hours in vitro and regression of ‘death-switched' xenografts occurred within 24 h correlating with the percentage of apoptotic cells in tumor and levels of an established cell death biomarker (cleaved cytokeratin-18) in the blood. We sought to define secreted biomarkers of tumor apoptosis from cultured cells using Discovery Isobaric Tag proteomics, which may provide candidates to validate in blood. Early after caspase-3 activation, levels of normally secreted proteins were decreased (e.g. Gelsolin and Midkine) and proteins including CD44 and High Mobility Group protein B1 (HMGB1) that were released into cell culture media in vitro were also identified in the bloodstream of mice bearing death-switched tumors. We also exemplify the utility of the death-switch model for the validation of apoptotic imaging probes using [(18)F]ML-10, a PET tracer currently in clinical trials. Results showed increased tracer uptake of [(18)F]ML-10 in tumours undergoing apoptosis, compared with matched tumour controls imaged in the same animal. Overall, the death-switch model represents a robust and versatile tool for the discovery and validation of apoptosis biomarkers. Nature Publishing Group 2013-05 2013-05-02 /pmc/articles/PMC3674346/ /pubmed/23640455 http://dx.doi.org/10.1038/cddis.2013.137 Text en Copyright © 2013 Macmillan Publishers Limited http://creativecommons.org/licenses/by-nc-nd/3.0/ This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivs 3.0 Unported License. To view a copy of this license, visit http://creativecommons.org/licenses/by-nc-nd/3.0/
spellingShingle Original Article
Simpson, K L
Cawthorne, C
Zhou, C
Hodgkinson, C L
Walker, M J
Trapani, F
Kadirvel, M
Brown, G
Dawson, M J
MacFarlane, M
Williams, K J
Whetton, A D
Dive, C
A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers
title A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers
title_full A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers
title_fullStr A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers
title_full_unstemmed A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers
title_short A caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers
title_sort caspase-3 ‘death-switch' in colorectal cancer cells for induced and synchronous tumor apoptosis in vitro and in vivo facilitates the development of minimally invasive cell death biomarkers
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3674346/
https://www.ncbi.nlm.nih.gov/pubmed/23640455
http://dx.doi.org/10.1038/cddis.2013.137
work_keys_str_mv AT simpsonkl acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT cawthornec acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT zhouc acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT hodgkinsoncl acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT walkermj acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT trapanif acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT kadirvelm acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT browng acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT dawsonmj acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT macfarlanem acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT williamskj acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT whettonad acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT divec acaspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT simpsonkl caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT cawthornec caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT zhouc caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT hodgkinsoncl caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT walkermj caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT trapanif caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT kadirvelm caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT browng caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT dawsonmj caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT macfarlanem caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT williamskj caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT whettonad caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers
AT divec caspase3deathswitchincolorectalcancercellsforinducedandsynchronoustumorapoptosisinvitroandinvivofacilitatesthedevelopmentofminimallyinvasivecelldeathbiomarkers

Ejemplares similares