Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas

Rational: In a subset of cancers, arginine auxotrophy occurs due to the loss of expression of argininosuccinate synthetase 1 (ASS1). This loss of ASS1 expression makes cancers sensitive to arginine starvation that is induced by PEGylated arginine deiminase (ADI-PEG20). Although ADI-PEG20 treatment i...

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Autores principales: Prudner, Bethany Cheree, Sun, Fangdi, Kremer, Jeffrey Charles, Xu, Jinbin, Huang, Chaofeng, Sai, Kiran Kumar Solingapuram, Morgan, Zachary, Leeds, Hayden, McConathy, Jonathan, Van Tine, Brian Andrew
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5928874/
https://www.ncbi.nlm.nih.gov/pubmed/29721066
http://dx.doi.org/10.7150/thno.22083
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author Prudner, Bethany Cheree
Sun, Fangdi
Kremer, Jeffrey Charles
Xu, Jinbin
Huang, Chaofeng
Sai, Kiran Kumar Solingapuram
Morgan, Zachary
Leeds, Hayden
McConathy, Jonathan
Van Tine, Brian Andrew
author_facet Prudner, Bethany Cheree
Sun, Fangdi
Kremer, Jeffrey Charles
Xu, Jinbin
Huang, Chaofeng
Sai, Kiran Kumar Solingapuram
Morgan, Zachary
Leeds, Hayden
McConathy, Jonathan
Van Tine, Brian Andrew
author_sort Prudner, Bethany Cheree
collection PubMed
description Rational: In a subset of cancers, arginine auxotrophy occurs due to the loss of expression of argininosuccinate synthetase 1 (ASS1). This loss of ASS1 expression makes cancers sensitive to arginine starvation that is induced by PEGylated arginine deiminase (ADI-PEG20). Although ADI-PEG20 treatment is effective, it does have important limitations. Arginine starvation is only beneficial in patients with cancers that are ASS1-deficient. Also, these tumors may metabolically reprogram to express ASS1, transforming them from an auxotrophic phenotype to a prototrophic phenotype and thus rendering ADI-PEG20 ineffective. Due to these limitations of ADI-PEG20 treatment and the potential for developing resistance, non-invasive tools to monitor sensitivity to arginine starvation are needed. Methods: Within this study, we assess the utility of a novel positron emission tomography (PET) tracer to determine sarcomas reliant on extracellular arginine for survival by measuring changes in amino acid transport in arginine auxotrophic sarcoma cells treated with ADI-PEG20. The uptake of the (18)F-labeled histidine analogue, (S)-2-amino-3-[1-(2-[(18)F]fluoroethyl)-1H-[1,2,3]triazol-4-yl]propanoic acid (AFETP), was assessed in vitro and in vivo using human-derived sarcoma cell lines. In addition, we examined the expression and localization of cationic amino acid transporters in response to arginine starvation with ADI-PEG20. Results: In vitro studies revealed that in response to ADI-PEG20 treatment, arginine auxotrophs increase the uptake of L-[(3)H]arginine and [(18)F]AFETP due to an increase in the expression and localization to the plasma membrane of the cationic amino acid transporter CAT-1. Furthermore, in vivo PET imaging studies in mice with arginine-dependent osteosarcoma xenografts showed increased [(18)F]AFETP uptake in tumors 4 days after ADI-PEG20 treatment compared to baseline. Conclusion: CAT-1 transporters localizes to the plasma membrane as a result of arginine starvation with ADI-PEG20 in ASS1-deficient tumor cells and provides a mechanism for using cationic amino acid transport substrates such as [(18)F]AFETP for identifying tumors susceptible to ADI-PEG20 treatment though non-invasive PET imaging techniques. These findings indicate that [(18)F]AFETP-PET may be suitable for the early detection of tumor response to arginine depletion due to ADI-PEG20 treatment.
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spelling pubmed-59288742018-05-02 Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas Prudner, Bethany Cheree Sun, Fangdi Kremer, Jeffrey Charles Xu, Jinbin Huang, Chaofeng Sai, Kiran Kumar Solingapuram Morgan, Zachary Leeds, Hayden McConathy, Jonathan Van Tine, Brian Andrew Theranostics Research Paper Rational: In a subset of cancers, arginine auxotrophy occurs due to the loss of expression of argininosuccinate synthetase 1 (ASS1). This loss of ASS1 expression makes cancers sensitive to arginine starvation that is induced by PEGylated arginine deiminase (ADI-PEG20). Although ADI-PEG20 treatment is effective, it does have important limitations. Arginine starvation is only beneficial in patients with cancers that are ASS1-deficient. Also, these tumors may metabolically reprogram to express ASS1, transforming them from an auxotrophic phenotype to a prototrophic phenotype and thus rendering ADI-PEG20 ineffective. Due to these limitations of ADI-PEG20 treatment and the potential for developing resistance, non-invasive tools to monitor sensitivity to arginine starvation are needed. Methods: Within this study, we assess the utility of a novel positron emission tomography (PET) tracer to determine sarcomas reliant on extracellular arginine for survival by measuring changes in amino acid transport in arginine auxotrophic sarcoma cells treated with ADI-PEG20. The uptake of the (18)F-labeled histidine analogue, (S)-2-amino-3-[1-(2-[(18)F]fluoroethyl)-1H-[1,2,3]triazol-4-yl]propanoic acid (AFETP), was assessed in vitro and in vivo using human-derived sarcoma cell lines. In addition, we examined the expression and localization of cationic amino acid transporters in response to arginine starvation with ADI-PEG20. Results: In vitro studies revealed that in response to ADI-PEG20 treatment, arginine auxotrophs increase the uptake of L-[(3)H]arginine and [(18)F]AFETP due to an increase in the expression and localization to the plasma membrane of the cationic amino acid transporter CAT-1. Furthermore, in vivo PET imaging studies in mice with arginine-dependent osteosarcoma xenografts showed increased [(18)F]AFETP uptake in tumors 4 days after ADI-PEG20 treatment compared to baseline. Conclusion: CAT-1 transporters localizes to the plasma membrane as a result of arginine starvation with ADI-PEG20 in ASS1-deficient tumor cells and provides a mechanism for using cationic amino acid transport substrates such as [(18)F]AFETP for identifying tumors susceptible to ADI-PEG20 treatment though non-invasive PET imaging techniques. These findings indicate that [(18)F]AFETP-PET may be suitable for the early detection of tumor response to arginine depletion due to ADI-PEG20 treatment. Ivyspring International Publisher 2018-03-07 /pmc/articles/PMC5928874/ /pubmed/29721066 http://dx.doi.org/10.7150/thno.22083 Text en © Ivyspring International Publisher This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY-NC) license (https://creativecommons.org/licenses/by-nc/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Prudner, Bethany Cheree
Sun, Fangdi
Kremer, Jeffrey Charles
Xu, Jinbin
Huang, Chaofeng
Sai, Kiran Kumar Solingapuram
Morgan, Zachary
Leeds, Hayden
McConathy, Jonathan
Van Tine, Brian Andrew
Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas
title Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas
title_full Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas
title_fullStr Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas
title_full_unstemmed Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas
title_short Amino Acid Uptake Measured by [(18)F]AFETP Increases in Response to Arginine Starvation in ASS1-Deficient Sarcomas
title_sort amino acid uptake measured by [(18)f]afetp increases in response to arginine starvation in ass1-deficient sarcomas
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5928874/
https://www.ncbi.nlm.nih.gov/pubmed/29721066
http://dx.doi.org/10.7150/thno.22083
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