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Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging

Near-infrared (NIR) nanoprobes with fluorescence “Turn-On” property are advantageous in cancer diagnosis but, to the best of our knowledge, “smart” nanoprobe that simultaneously targets both biotin receptor and carboxylesterase (CES) for HepG2 tumor-dual targeted imaging has not been reported. Metho...

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Autores principales: Chen, Peiyao, Kuang, Wen, Zheng, Zhen, Yang, Shuye, Liu, Yaling, Su, Lanhong, Zhao, Kui, Liang, Gaolin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6831296/
https://www.ncbi.nlm.nih.gov/pubmed/31695773
http://dx.doi.org/10.7150/thno.37625
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author Chen, Peiyao
Kuang, Wen
Zheng, Zhen
Yang, Shuye
Liu, Yaling
Su, Lanhong
Zhao, Kui
Liang, Gaolin
author_facet Chen, Peiyao
Kuang, Wen
Zheng, Zhen
Yang, Shuye
Liu, Yaling
Su, Lanhong
Zhao, Kui
Liang, Gaolin
author_sort Chen, Peiyao
collection PubMed
description Near-infrared (NIR) nanoprobes with fluorescence “Turn-On” property are advantageous in cancer diagnosis but, to the best of our knowledge, “smart” nanoprobe that simultaneously targets both biotin receptor and carboxylesterase (CES) for HepG2 tumor-dual targeted imaging has not been reported. Methods: Using CBT-Cys click condensation reaction, we rationally designed a “smart” NIR fluorescence probe H(2)N-Cys(StBu)-Lys(Biotin)-Ser(Cy5.5)-CBT (NIR-CBT) and used it to facilely prepare the fluorescence-quenched nanoparticle NIR-CBT-NP. Results: In vitro results indicated that, after NIR-CBT-NP was incubated with CES for 6 h, its fluorescence was turned “On” by 69 folds. Cell experiments verified that NIR-CBT-NP was uptaken by HepG2 cells via biotin receptor-assisted endocytosis and its fluorescence was turned “On” by intracellular CES hydrolysis. Moreover, NIR-CBT-NP was successfully applied to image both biotin receptor- and CES-overexpressing HepG2 tumors. Conclusion: Fluorescence-quenched nanoparticle NIR-CBT-NP was facilely prepared to actively target biotin receptor-overexpressing HepG2 cancer cells and turn the fluorescence “On” by intracellular CES hydrolysis for tumor-dual targeted imaging. We anticipate that our fluorescence “Turn-On” nanoparticle could be applied for liver cancer diagnosis in clinic in the near future.
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spelling pubmed-68312962019-11-06 Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging Chen, Peiyao Kuang, Wen Zheng, Zhen Yang, Shuye Liu, Yaling Su, Lanhong Zhao, Kui Liang, Gaolin Theranostics Research Paper Near-infrared (NIR) nanoprobes with fluorescence “Turn-On” property are advantageous in cancer diagnosis but, to the best of our knowledge, “smart” nanoprobe that simultaneously targets both biotin receptor and carboxylesterase (CES) for HepG2 tumor-dual targeted imaging has not been reported. Methods: Using CBT-Cys click condensation reaction, we rationally designed a “smart” NIR fluorescence probe H(2)N-Cys(StBu)-Lys(Biotin)-Ser(Cy5.5)-CBT (NIR-CBT) and used it to facilely prepare the fluorescence-quenched nanoparticle NIR-CBT-NP. Results: In vitro results indicated that, after NIR-CBT-NP was incubated with CES for 6 h, its fluorescence was turned “On” by 69 folds. Cell experiments verified that NIR-CBT-NP was uptaken by HepG2 cells via biotin receptor-assisted endocytosis and its fluorescence was turned “On” by intracellular CES hydrolysis. Moreover, NIR-CBT-NP was successfully applied to image both biotin receptor- and CES-overexpressing HepG2 tumors. Conclusion: Fluorescence-quenched nanoparticle NIR-CBT-NP was facilely prepared to actively target biotin receptor-overexpressing HepG2 cancer cells and turn the fluorescence “On” by intracellular CES hydrolysis for tumor-dual targeted imaging. We anticipate that our fluorescence “Turn-On” nanoparticle could be applied for liver cancer diagnosis in clinic in the near future. Ivyspring International Publisher 2019-09-25 /pmc/articles/PMC6831296/ /pubmed/31695773 http://dx.doi.org/10.7150/thno.37625 Text en © The author(s) This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Chen, Peiyao
Kuang, Wen
Zheng, Zhen
Yang, Shuye
Liu, Yaling
Su, Lanhong
Zhao, Kui
Liang, Gaolin
Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging
title Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging
title_full Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging
title_fullStr Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging
title_full_unstemmed Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging
title_short Carboxylesterase-Cleavable Biotinylated Nanoparticle for Tumor-Dual Targeted Imaging
title_sort carboxylesterase-cleavable biotinylated nanoparticle for tumor-dual targeted imaging
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6831296/
https://www.ncbi.nlm.nih.gov/pubmed/31695773
http://dx.doi.org/10.7150/thno.37625
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