A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy

BACKGROUND: GD2 is a mainstream biomarker for neuroblastoma (NB)-targeted therapy. Current anti-GD2 therapeutics exhibit several side effects since GD2 is also expressed at low levels on normal cells. Thus, current anti-GD2 therapeutics can be compromised by the coexistence of the target receptor on...

Descripción completa

Detalles Bibliográficos
Autores principales: Zhang, Liyu, Wang, Meng, Zhu, Zeen, Ding, Chenxi, Chen, Shengquan, Wu, Haibin, Yang, Ying, Che, Fengyu, Li, Qiao, Li, Hui
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Dove 2021
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8121684/
https://www.ncbi.nlm.nih.gov/pubmed/34007175
http://dx.doi.org/10.2147/IJN.S302450
_version_ 1783692418834497536
author Zhang, Liyu
Wang, Meng
Zhu, Zeen
Ding, Chenxi
Chen, Shengquan
Wu, Haibin
Yang, Ying
Che, Fengyu
Li, Qiao
Li, Hui
author_facet Zhang, Liyu
Wang, Meng
Zhu, Zeen
Ding, Chenxi
Chen, Shengquan
Wu, Haibin
Yang, Ying
Che, Fengyu
Li, Qiao
Li, Hui
author_sort Zhang, Liyu
collection PubMed
description BACKGROUND: GD2 is a mainstream biomarker for neuroblastoma (NB)-targeted therapy. Current anti-GD2 therapeutics exhibit several side effects since GD2 is also expressed at low levels on normal cells. Thus, current anti-GD2 therapeutics can be compromised by the coexistence of the target receptor on both cancer cells and normal cells. PROPOSE: Aptamers are promising and invaluable molecular tools. Because of the pH difference between tumor and normal cells, in this study, we constructed a pH-sensitive aptamer-mediated drug delivery system (IGD-Targeted). METHODS: In vivo Systematic Evolution of Ligands by Exponential Enrichment (SELEX) was used to generate a novel GD2 aptamer. Flow cytometry and molecular docking were applied to assess the binding specificities, affinities abilities of the aptamers. Confocal microscope, CCK8 assay, and BrdU assay were utilized to evaluate whether IGD-Targeted could only bind with GD2 at acidic environment. To evaluate whether IGD-Targeted could inhibit GD2-positive tumor and protect normal cells, in vivo living imaging, histomorphological staining, blood test, and RNA-sequencing were observed in animal model. RESULTS: GD2 aptamer termed as DB67 could bind with GD2-positive cells with high specificity, while has minimal cross-reactivities to other negative cells. It has been validated that the i-motif in IGD-Targeted facilitates the binding specificity and affinity of the GD2 aptamer to GD2-positive NB tumor cells but does not interfere with GD2-positive normal cells at the pH of the cellular microenvironment. In addition, IGD-Targeted is capable of delivering Dox to only GD2-positive NB tumor cells and not to normal cells in vivo and in vitro, resulting in precise inhibition of tumor cells and protection of normal cells. CONCLUSION: This study suggests that IGD-Targeted as a promising platform for NB therapy which could show greater tumor inhibition and fewer side effects to normal cells, regardless of the existence of the same receptor on the target and nontarget cells.
format Online
Article
Text
id pubmed-8121684
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Dove
record_format MEDLINE/PubMed
spelling pubmed-81216842021-05-17 A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy Zhang, Liyu Wang, Meng Zhu, Zeen Ding, Chenxi Chen, Shengquan Wu, Haibin Yang, Ying Che, Fengyu Li, Qiao Li, Hui Int J Nanomedicine Original Research BACKGROUND: GD2 is a mainstream biomarker for neuroblastoma (NB)-targeted therapy. Current anti-GD2 therapeutics exhibit several side effects since GD2 is also expressed at low levels on normal cells. Thus, current anti-GD2 therapeutics can be compromised by the coexistence of the target receptor on both cancer cells and normal cells. PROPOSE: Aptamers are promising and invaluable molecular tools. Because of the pH difference between tumor and normal cells, in this study, we constructed a pH-sensitive aptamer-mediated drug delivery system (IGD-Targeted). METHODS: In vivo Systematic Evolution of Ligands by Exponential Enrichment (SELEX) was used to generate a novel GD2 aptamer. Flow cytometry and molecular docking were applied to assess the binding specificities, affinities abilities of the aptamers. Confocal microscope, CCK8 assay, and BrdU assay were utilized to evaluate whether IGD-Targeted could only bind with GD2 at acidic environment. To evaluate whether IGD-Targeted could inhibit GD2-positive tumor and protect normal cells, in vivo living imaging, histomorphological staining, blood test, and RNA-sequencing were observed in animal model. RESULTS: GD2 aptamer termed as DB67 could bind with GD2-positive cells with high specificity, while has minimal cross-reactivities to other negative cells. It has been validated that the i-motif in IGD-Targeted facilitates the binding specificity and affinity of the GD2 aptamer to GD2-positive NB tumor cells but does not interfere with GD2-positive normal cells at the pH of the cellular microenvironment. In addition, IGD-Targeted is capable of delivering Dox to only GD2-positive NB tumor cells and not to normal cells in vivo and in vitro, resulting in precise inhibition of tumor cells and protection of normal cells. CONCLUSION: This study suggests that IGD-Targeted as a promising platform for NB therapy which could show greater tumor inhibition and fewer side effects to normal cells, regardless of the existence of the same receptor on the target and nontarget cells. Dove 2021-05-10 /pmc/articles/PMC8121684/ /pubmed/34007175 http://dx.doi.org/10.2147/IJN.S302450 Text en © 2021 Zhang et al. https://creativecommons.org/licenses/by-nc/3.0/This work is published and licensed by Dove Medical Press Limited. The full terms of this license are available at https://www.dovepress.com/terms.php and incorporate the Creative Commons Attribution – Non Commercial (unported, v3.0) License (http://creativecommons.org/licenses/by-nc/3.0/ (https://creativecommons.org/licenses/by-nc/3.0/) ). By accessing the work you hereby accept the Terms. Non-commercial uses of the work are permitted without any further permission from Dove Medical Press Limited, provided the work is properly attributed. For permission for commercial use of this work, please see paragraphs 4.2 and 5 of our Terms (https://www.dovepress.com/terms.php).
spellingShingle Original Research
Zhang, Liyu
Wang, Meng
Zhu, Zeen
Ding, Chenxi
Chen, Shengquan
Wu, Haibin
Yang, Ying
Che, Fengyu
Li, Qiao
Li, Hui
A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy
title A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy
title_full A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy
title_fullStr A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy
title_full_unstemmed A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy
title_short A Novel pH-Sensitive Multifunctional DNA Nanomedicine: An Enhanced and Harmless GD2 Aptamer-Mediated Strategy for Guiding Neuroblastoma Antitumor Therapy
title_sort novel ph-sensitive multifunctional dna nanomedicine: an enhanced and harmless gd2 aptamer-mediated strategy for guiding neuroblastoma antitumor therapy
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8121684/
https://www.ncbi.nlm.nih.gov/pubmed/34007175
http://dx.doi.org/10.2147/IJN.S302450
work_keys_str_mv AT zhangliyu anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT wangmeng anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT zhuzeen anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT dingchenxi anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT chenshengquan anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT wuhaibin anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT yangying anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT chefengyu anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT liqiao anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT lihui anovelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT zhangliyu novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT wangmeng novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT zhuzeen novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT dingchenxi novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT chenshengquan novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT wuhaibin novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT yangying novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT chefengyu novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT liqiao novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy
AT lihui novelphsensitivemultifunctionaldnananomedicineanenhancedandharmlessgd2aptamermediatedstrategyforguidingneuroblastomaantitumortherapy

Ejemplares similares