The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death

PURPOSE: Most effective antitumor therapies induce tumor cell death. Non-invasive, rapid and accurate quantitative imaging of cell death is essential for monitoring early response to antitumor therapies. To facilitate this, we previously developed a biocompatible necrosis-avid near-infrared fluoresc...

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Autores principales: Stammes, Marieke A., Maeda, Azusa, Bu, Jiachuan, Scollard, Deborah A., Kulbatski, Iris, Medeiros, Philip J., Sinisi, Riccardo, Dubikovskaya, Elena A., Snoeks, Thomas J. A., van Beek, Ermond R., Chan, Alan B., Löwik, Clemens W. G. M., DaCosta, Ralph S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2016
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5073092/
https://www.ncbi.nlm.nih.gov/pubmed/27818949
http://dx.doi.org/10.3389/fonc.2016.00221
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author Stammes, Marieke A.
Maeda, Azusa
Bu, Jiachuan
Scollard, Deborah A.
Kulbatski, Iris
Medeiros, Philip J.
Sinisi, Riccardo
Dubikovskaya, Elena A.
Snoeks, Thomas J. A.
van Beek, Ermond R.
Chan, Alan B.
Löwik, Clemens W. G. M.
DaCosta, Ralph S.
author_facet Stammes, Marieke A.
Maeda, Azusa
Bu, Jiachuan
Scollard, Deborah A.
Kulbatski, Iris
Medeiros, Philip J.
Sinisi, Riccardo
Dubikovskaya, Elena A.
Snoeks, Thomas J. A.
van Beek, Ermond R.
Chan, Alan B.
Löwik, Clemens W. G. M.
DaCosta, Ralph S.
author_sort Stammes, Marieke A.
collection PubMed
description PURPOSE: Most effective antitumor therapies induce tumor cell death. Non-invasive, rapid and accurate quantitative imaging of cell death is essential for monitoring early response to antitumor therapies. To facilitate this, we previously developed a biocompatible necrosis-avid near-infrared fluorescence (NIRF) imaging probe, HQ4, which was radiolabeled with (111)Indium-chloride ((111)In-Cl(3)) via the chelate diethylene triamine pentaacetic acid (DTPA), to enable clinical translation. The aim of the present study was to evaluate the application of HQ4-DTPA for monitoring tumor cell death induced by radiation therapy. Apart from its NIRF and radioactive properties, HQ4-DTPA was also tested as a photoacoustic imaging probe to evaluate its performance as a multimodal contrast agent for superficial and deep tissue imaging. MATERIALS AND METHODS: Radiation-induced tumor cell death was examined in a xenograft mouse model of human breast cancer (MCF-7). Tumors were irradiated with three fractions of 9 Gy each. HQ4-DTPA was injected intravenously after the last irradiation, NIRF and photoacoustic imaging of the tumors were performed at 12, 20, and 40 h after injection. Changes in probe accumulation in the tumors were measured in vivo, and ex vivo histological analysis of excised tumors was performed at experimental endpoints. In addition, biodistribution of radiolabeled [(111)In]DTPA-HQ4 was assessed using hybrid single-photon emission computed tomography–computed tomography (SPECT–CT) at the same time points. RESULTS: In vivo NIRF imaging demonstrated a significant difference in probe accumulation between control and irradiated tumors at all time points after injection. A similar trend was observed using in vivo photoacoustic imaging, which was validated by ex vivo tissue fluorescence and photoacoustic imaging. Serial quantitative radioactivity measurements of probe biodistribution further demonstrated increased probe accumulation in irradiated tumors. CONCLUSION: HQ4-DTPA has high specificity for dead cells in vivo, potentiating its use as a contrast agent for determining the relative level of tumor cell death following radiation therapy using NIRF, photoacoustic imaging and SPECT in vivo. Initial preclinical results are promising and indicate the need for further evaluation in larger cohorts. If successful, such studies may help develop a new multimodal method for non-invasive and dynamic deep tissue imaging of treatment-induced cell death to quantitatively assess therapeutic response in patients.
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spelling pubmed-50730922016-11-04 The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death Stammes, Marieke A. Maeda, Azusa Bu, Jiachuan Scollard, Deborah A. Kulbatski, Iris Medeiros, Philip J. Sinisi, Riccardo Dubikovskaya, Elena A. Snoeks, Thomas J. A. van Beek, Ermond R. Chan, Alan B. Löwik, Clemens W. G. M. DaCosta, Ralph S. Front Oncol Oncology PURPOSE: Most effective antitumor therapies induce tumor cell death. Non-invasive, rapid and accurate quantitative imaging of cell death is essential for monitoring early response to antitumor therapies. To facilitate this, we previously developed a biocompatible necrosis-avid near-infrared fluorescence (NIRF) imaging probe, HQ4, which was radiolabeled with (111)Indium-chloride ((111)In-Cl(3)) via the chelate diethylene triamine pentaacetic acid (DTPA), to enable clinical translation. The aim of the present study was to evaluate the application of HQ4-DTPA for monitoring tumor cell death induced by radiation therapy. Apart from its NIRF and radioactive properties, HQ4-DTPA was also tested as a photoacoustic imaging probe to evaluate its performance as a multimodal contrast agent for superficial and deep tissue imaging. MATERIALS AND METHODS: Radiation-induced tumor cell death was examined in a xenograft mouse model of human breast cancer (MCF-7). Tumors were irradiated with three fractions of 9 Gy each. HQ4-DTPA was injected intravenously after the last irradiation, NIRF and photoacoustic imaging of the tumors were performed at 12, 20, and 40 h after injection. Changes in probe accumulation in the tumors were measured in vivo, and ex vivo histological analysis of excised tumors was performed at experimental endpoints. In addition, biodistribution of radiolabeled [(111)In]DTPA-HQ4 was assessed using hybrid single-photon emission computed tomography–computed tomography (SPECT–CT) at the same time points. RESULTS: In vivo NIRF imaging demonstrated a significant difference in probe accumulation between control and irradiated tumors at all time points after injection. A similar trend was observed using in vivo photoacoustic imaging, which was validated by ex vivo tissue fluorescence and photoacoustic imaging. Serial quantitative radioactivity measurements of probe biodistribution further demonstrated increased probe accumulation in irradiated tumors. CONCLUSION: HQ4-DTPA has high specificity for dead cells in vivo, potentiating its use as a contrast agent for determining the relative level of tumor cell death following radiation therapy using NIRF, photoacoustic imaging and SPECT in vivo. Initial preclinical results are promising and indicate the need for further evaluation in larger cohorts. If successful, such studies may help develop a new multimodal method for non-invasive and dynamic deep tissue imaging of treatment-induced cell death to quantitatively assess therapeutic response in patients. Frontiers Media S.A. 2016-10-21 /pmc/articles/PMC5073092/ /pubmed/27818949 http://dx.doi.org/10.3389/fonc.2016.00221 Text en Copyright © 2016 Stammes, Maeda, Bu, Scollard, Kulbatski, Medeiros, Sinisi, Dubikovskaya, Snoeks, van Beek, Chan, Löwik and DaCosta. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Stammes, Marieke A.
Maeda, Azusa
Bu, Jiachuan
Scollard, Deborah A.
Kulbatski, Iris
Medeiros, Philip J.
Sinisi, Riccardo
Dubikovskaya, Elena A.
Snoeks, Thomas J. A.
van Beek, Ermond R.
Chan, Alan B.
Löwik, Clemens W. G. M.
DaCosta, Ralph S.
The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death
title The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death
title_full The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death
title_fullStr The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death
title_full_unstemmed The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death
title_short The Necrosis-Avid Small Molecule HQ4-DTPA as a Multimodal Imaging Agent for Monitoring Radiation Therapy-Induced Tumor Cell Death
title_sort necrosis-avid small molecule hq4-dtpa as a multimodal imaging agent for monitoring radiation therapy-induced tumor cell death
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5073092/
https://www.ncbi.nlm.nih.gov/pubmed/27818949
http://dx.doi.org/10.3389/fonc.2016.00221
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