GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging

Tumor imaging tools with high specificity and sensitivity are needed to aid the boundary recognition in solid tumor diagnosis and surgical resection. In this study, we developed a near infra-red (NIR) probe (P6) for in vitro/in vivo tumor imaging on the basis of the dual strategy of cancer cell targ...

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Autores principales: Guo, Ruiying, Huang, Feng, Zhang, Bo, Yan, Youyou, Che, Jinxin, Jin, Yizhen, Zhuang, Yuxin, Dong, Rong, Li, Yangling, Tan, Biqin, Song, Rui, Hu, Yongzhou, Dong, Xiaowu, Li, Xin, Lin, Nengming
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6587172/
https://www.ncbi.nlm.nih.gov/pubmed/31281494
http://dx.doi.org/10.7150/thno.32742
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author Guo, Ruiying
Huang, Feng
Zhang, Bo
Yan, Youyou
Che, Jinxin
Jin, Yizhen
Zhuang, Yuxin
Dong, Rong
Li, Yangling
Tan, Biqin
Song, Rui
Hu, Yongzhou
Dong, Xiaowu
Li, Xin
Lin, Nengming
author_facet Guo, Ruiying
Huang, Feng
Zhang, Bo
Yan, Youyou
Che, Jinxin
Jin, Yizhen
Zhuang, Yuxin
Dong, Rong
Li, Yangling
Tan, Biqin
Song, Rui
Hu, Yongzhou
Dong, Xiaowu
Li, Xin
Lin, Nengming
author_sort Guo, Ruiying
collection PubMed
description Tumor imaging tools with high specificity and sensitivity are needed to aid the boundary recognition in solid tumor diagnosis and surgical resection. In this study, we developed a near infra-red (NIR) probe (P6) for in vitro/in vivo tumor imaging on the basis of the dual strategy of cancer cell targeting and stimulus-dependent activation. The selective imaging capacity towards cancer cells of P6 was thoroughly investigated, and the potential mechanisms of endocytosis were preliminary explored. Methods: GSH-activated biotin labelled NIR probe (P6) was designed, synthesized and characterized. The GSH responsive properties were systematically illustrated through UV-vis, fluorescent tests and LC-MS analysis. In vitro fluorescent imaging of probe P6 was collected in various living cancer cell lines (i.e. SW480, HGC-27, H460, BxPC-3, KHOS) and normal cell lines (i.e. BEAS-2B, HLF-1, THP1) under confocal laser scanning microscopy. Probe P6 was further applied to image primary human cancer cells which were freshly isolated from the peritoneal carcinoma and rectal cancer patients. Serial sections of human tumor tissues were collected and sent for H&E (hematoxylin-eosin) staining and P6 imaging. Live fluorescent and photoacoustic imaging were used to investigate the in vivo imaging of P6 in both tumor and normal tissues in HGC-27 and KHOS xenograft model. Results: Probe P6 could be recognized and transported into cancer cells by tumor specific biotin receptors and efficiently be triggered by GSH to release fluorophore 4. In fact, the cellular uptake of P6 could be partially blocked by the addition of free biotin. Furthermore, probe P6 could image various cancer cell lines, as well as primary cancer cells, exhibiting a ten-fold increase in fluorescence intensity over normal cells. In freshly dissected cancer tissues, P6 fluorescent imaging distinguished the cancerous area under confocal laser scanning microscopy, which was exact the same area as indicated by H&E staining. We also found that P6 exhibited superior selectivity against cancer tissues by local injection. Conclusion: In this study, we developed a dual-modal NIR probe P6 with enhanced cellular uptake into cancer cells and environmental stimulus triggered fluorescence. Our strategy provided a novel insight into the development of imaging tools that could be potentially used for fluorescent image-guided cancer boundary recognition and possibly cancer diagnosis.
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spelling pubmed-65871722019-07-05 GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging Guo, Ruiying Huang, Feng Zhang, Bo Yan, Youyou Che, Jinxin Jin, Yizhen Zhuang, Yuxin Dong, Rong Li, Yangling Tan, Biqin Song, Rui Hu, Yongzhou Dong, Xiaowu Li, Xin Lin, Nengming Theranostics Research Paper Tumor imaging tools with high specificity and sensitivity are needed to aid the boundary recognition in solid tumor diagnosis and surgical resection. In this study, we developed a near infra-red (NIR) probe (P6) for in vitro/in vivo tumor imaging on the basis of the dual strategy of cancer cell targeting and stimulus-dependent activation. The selective imaging capacity towards cancer cells of P6 was thoroughly investigated, and the potential mechanisms of endocytosis were preliminary explored. Methods: GSH-activated biotin labelled NIR probe (P6) was designed, synthesized and characterized. The GSH responsive properties were systematically illustrated through UV-vis, fluorescent tests and LC-MS analysis. In vitro fluorescent imaging of probe P6 was collected in various living cancer cell lines (i.e. SW480, HGC-27, H460, BxPC-3, KHOS) and normal cell lines (i.e. BEAS-2B, HLF-1, THP1) under confocal laser scanning microscopy. Probe P6 was further applied to image primary human cancer cells which were freshly isolated from the peritoneal carcinoma and rectal cancer patients. Serial sections of human tumor tissues were collected and sent for H&E (hematoxylin-eosin) staining and P6 imaging. Live fluorescent and photoacoustic imaging were used to investigate the in vivo imaging of P6 in both tumor and normal tissues in HGC-27 and KHOS xenograft model. Results: Probe P6 could be recognized and transported into cancer cells by tumor specific biotin receptors and efficiently be triggered by GSH to release fluorophore 4. In fact, the cellular uptake of P6 could be partially blocked by the addition of free biotin. Furthermore, probe P6 could image various cancer cell lines, as well as primary cancer cells, exhibiting a ten-fold increase in fluorescence intensity over normal cells. In freshly dissected cancer tissues, P6 fluorescent imaging distinguished the cancerous area under confocal laser scanning microscopy, which was exact the same area as indicated by H&E staining. We also found that P6 exhibited superior selectivity against cancer tissues by local injection. Conclusion: In this study, we developed a dual-modal NIR probe P6 with enhanced cellular uptake into cancer cells and environmental stimulus triggered fluorescence. Our strategy provided a novel insight into the development of imaging tools that could be potentially used for fluorescent image-guided cancer boundary recognition and possibly cancer diagnosis. Ivyspring International Publisher 2019-05-26 /pmc/articles/PMC6587172/ /pubmed/31281494 http://dx.doi.org/10.7150/thno.32742 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
Guo, Ruiying
Huang, Feng
Zhang, Bo
Yan, Youyou
Che, Jinxin
Jin, Yizhen
Zhuang, Yuxin
Dong, Rong
Li, Yangling
Tan, Biqin
Song, Rui
Hu, Yongzhou
Dong, Xiaowu
Li, Xin
Lin, Nengming
GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging
title GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging
title_full GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging
title_fullStr GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging
title_full_unstemmed GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging
title_short GSH Activated Biotin-tagged Near-Infrared Probe for Efficient Cancer Imaging
title_sort gsh activated biotin-tagged near-infrared probe for efficient cancer imaging
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6587172/
https://www.ncbi.nlm.nih.gov/pubmed/31281494
http://dx.doi.org/10.7150/thno.32742
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