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Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer

Tumor Endothelial Marker-1 (TEM1/CD248) is a tumor vascular marker with high therapeutic and diagnostic potentials. Immuno-imaging with TEM1-specific antibodies can help to detect cancerous lesions, monitor tumor responses, and select patients that are most likely to benefit from TEM1-targeted thera...

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Autores principales: Li, Chunsheng, Wang, Junying, Hu, Jia, Feng, Yi, Hasegawa, Kosei, Peng, Xiaohui, Duan, Xingmei, Zhao, Aizhi, Mikitsh, John L., Muzykantov, Vladimir R., Chacko, Ann-Marie, Pryma, Daniel A., Dunn, Steven M., Coukos, George
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4196179/
https://www.ncbi.nlm.nih.gov/pubmed/25051365
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author Li, Chunsheng
Wang, Junying
Hu, Jia
Feng, Yi
Hasegawa, Kosei
Peng, Xiaohui
Duan, Xingmei
Zhao, Aizhi
Mikitsh, John L.
Muzykantov, Vladimir R.
Chacko, Ann-Marie
Pryma, Daniel A.
Dunn, Steven M.
Coukos, George
author_facet Li, Chunsheng
Wang, Junying
Hu, Jia
Feng, Yi
Hasegawa, Kosei
Peng, Xiaohui
Duan, Xingmei
Zhao, Aizhi
Mikitsh, John L.
Muzykantov, Vladimir R.
Chacko, Ann-Marie
Pryma, Daniel A.
Dunn, Steven M.
Coukos, George
author_sort Li, Chunsheng
collection PubMed
description Tumor Endothelial Marker-1 (TEM1/CD248) is a tumor vascular marker with high therapeutic and diagnostic potentials. Immuno-imaging with TEM1-specific antibodies can help to detect cancerous lesions, monitor tumor responses, and select patients that are most likely to benefit from TEM1-targeted therapies. In particular, near infrared(NIR) optical imaging with biomarker-specific antibodies can provide real-time, tomographic information without exposing the subjects to radioactivity. To maximize the theranostic potential of TEM1, we developed a panel of all human, multivalent Fc-fusion proteins based on a previously identified single chain antibody (scFv78) that recognizes both human and mouse TEM1. By characterizing avidity, stability, and pharmacokinectics, we identified one fusion protein, 78Fc, with desirable characteristics for immuno-imaging applications. The biodistribution of radiolabeled 78Fc showed that this antibody had minimal binding to normal organs, which have low expression of TEM1. Next, we developed a 78Fc-based tracer and tested its performance in different TEM1-expressing mouse models. The NIR imaging and tomography results suggest that the 78Fc-NIR tracer performs well in distinguishing mouse- or human-TEM1 expressing tumor grafts from normal organs and control grafts in vivo. From these results we conclude that further development and optimization of 78Fc as a TEM1-targeted imaging agent for use in clinical settings is warranted.
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spelling pubmed-41961792014-10-21 Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer Li, Chunsheng Wang, Junying Hu, Jia Feng, Yi Hasegawa, Kosei Peng, Xiaohui Duan, Xingmei Zhao, Aizhi Mikitsh, John L. Muzykantov, Vladimir R. Chacko, Ann-Marie Pryma, Daniel A. Dunn, Steven M. Coukos, George Oncotarget Research Paper Tumor Endothelial Marker-1 (TEM1/CD248) is a tumor vascular marker with high therapeutic and diagnostic potentials. Immuno-imaging with TEM1-specific antibodies can help to detect cancerous lesions, monitor tumor responses, and select patients that are most likely to benefit from TEM1-targeted therapies. In particular, near infrared(NIR) optical imaging with biomarker-specific antibodies can provide real-time, tomographic information without exposing the subjects to radioactivity. To maximize the theranostic potential of TEM1, we developed a panel of all human, multivalent Fc-fusion proteins based on a previously identified single chain antibody (scFv78) that recognizes both human and mouse TEM1. By characterizing avidity, stability, and pharmacokinectics, we identified one fusion protein, 78Fc, with desirable characteristics for immuno-imaging applications. The biodistribution of radiolabeled 78Fc showed that this antibody had minimal binding to normal organs, which have low expression of TEM1. Next, we developed a 78Fc-based tracer and tested its performance in different TEM1-expressing mouse models. The NIR imaging and tomography results suggest that the 78Fc-NIR tracer performs well in distinguishing mouse- or human-TEM1 expressing tumor grafts from normal organs and control grafts in vivo. From these results we conclude that further development and optimization of 78Fc as a TEM1-targeted imaging agent for use in clinical settings is warranted. Impact Journals LLC 2014-07-08 /pmc/articles/PMC4196179/ /pubmed/25051365 Text en Copyright: © 2014 Li et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Li, Chunsheng
Wang, Junying
Hu, Jia
Feng, Yi
Hasegawa, Kosei
Peng, Xiaohui
Duan, Xingmei
Zhao, Aizhi
Mikitsh, John L.
Muzykantov, Vladimir R.
Chacko, Ann-Marie
Pryma, Daniel A.
Dunn, Steven M.
Coukos, George
Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer
title Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer
title_full Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer
title_fullStr Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer
title_full_unstemmed Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer
title_short Development, optimization, and validation of novel anti-TEM1/CD248 affinity agent for optical imaging in cancer
title_sort development, optimization, and validation of novel anti-tem1/cd248 affinity agent for optical imaging in cancer
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4196179/
https://www.ncbi.nlm.nih.gov/pubmed/25051365
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