In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy

Rationale: Drug combination therapy for cancer treatment exerts a more potent antitumor effect. The targeted delivery and release of multiple drugs in a patient's body thus presents a more effective treatment approach, warranting further research. Methods: Two antitumor drugs (ICG: indocyanine...

Descripción completa

Detalles Bibliográficos
Autores principales: Jiang, Xinglu, Fan, Xiaobo, Zhang, Rui, Xu, Wei, Wu, Hailu, Zhao, Fengfeng, Xiao, Han, Zhang, Chen, Zhao, Chenggui, Wu, Guoqiu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2020
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7667678/
https://www.ncbi.nlm.nih.gov/pubmed/33204335
http://dx.doi.org/10.7150/thno.52000
_version_ 1783610358806609920
author Jiang, Xinglu
Fan, Xiaobo
Zhang, Rui
Xu, Wei
Wu, Hailu
Zhao, Fengfeng
Xiao, Han
Zhang, Chen
Zhao, Chenggui
Wu, Guoqiu
author_facet Jiang, Xinglu
Fan, Xiaobo
Zhang, Rui
Xu, Wei
Wu, Hailu
Zhao, Fengfeng
Xiao, Han
Zhang, Chen
Zhao, Chenggui
Wu, Guoqiu
author_sort Jiang, Xinglu
collection PubMed
description Rationale: Drug combination therapy for cancer treatment exerts a more potent antitumor effect. The targeted delivery and release of multiple drugs in a patient's body thus presents a more effective treatment approach, warranting further research. Methods: Two antitumor drugs (ICG: indocyanine green and THP: pirarubicin) were successfully screened to sequentially trigger self-assembling peptides (P60) to produce bacteria-sized particles (500-1000 nm, P60-ICG-THP). First, after mixing equal amount of P60 and ICG, trace amount of water (the mass ratio between P60 and water: 100:1) was used to trigger their assembly into P60-ICG. Subsequently, the assembly of P60-ICG and THP was further triggered by ultrasound treatment to produce P60-ICG-THP. Results: P60-ICG-THP constituted a cluster of several nanoparticles (50-100 nm) and possessed a negative charge. Owing to its size and charge characteristics, P60-ICG-THP could remain outside the cell membrane, avoiding the phagocytic clearance of blood and normal tissue cells in vivo. However, after localizing in the tumor, the size and charge switches of P60-ICG-THP, rapidly triggered by the low pH of the tumor microenvironment, caused P60-ICG-THP to segregate into two parts: (i) positively charged nanoparticles with a size of approximately 50 nm, and (ii) negatively charged particles of an uneven size. The former, mainly carrying THP (chemotherapeutic agent), could immediately cross the cell membrane and deliver pirarubicin into the nucleus of tumor cells. The latter, carrying ICG (used for photothermal therapy), could also enter the cell via the endocytosis pathway or accumulate in tumor blood vessels to selectively block the supply of nutrients and oxygen (cancer starvation). Both these particles could avoid the rapid excretion of ICG in the liver and were conducive to accumulation in the tumor tissue for photothermal therapy. Conclusion: Our drug delivery system not only achieves the precise subcellular delivery of two anticancer drugs due to their size and charge switches in the tumor site, but also provides a new strategy to combine chemotherapy, photothermal therapy, and cancer starvation therapy for the development of a highly efficient antitumor therapeutic regimen.
format Online
Article
Text
id pubmed-7667678
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-76676782020-11-16 In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy Jiang, Xinglu Fan, Xiaobo Zhang, Rui Xu, Wei Wu, Hailu Zhao, Fengfeng Xiao, Han Zhang, Chen Zhao, Chenggui Wu, Guoqiu Theranostics Research Paper Rationale: Drug combination therapy for cancer treatment exerts a more potent antitumor effect. The targeted delivery and release of multiple drugs in a patient's body thus presents a more effective treatment approach, warranting further research. Methods: Two antitumor drugs (ICG: indocyanine green and THP: pirarubicin) were successfully screened to sequentially trigger self-assembling peptides (P60) to produce bacteria-sized particles (500-1000 nm, P60-ICG-THP). First, after mixing equal amount of P60 and ICG, trace amount of water (the mass ratio between P60 and water: 100:1) was used to trigger their assembly into P60-ICG. Subsequently, the assembly of P60-ICG and THP was further triggered by ultrasound treatment to produce P60-ICG-THP. Results: P60-ICG-THP constituted a cluster of several nanoparticles (50-100 nm) and possessed a negative charge. Owing to its size and charge characteristics, P60-ICG-THP could remain outside the cell membrane, avoiding the phagocytic clearance of blood and normal tissue cells in vivo. However, after localizing in the tumor, the size and charge switches of P60-ICG-THP, rapidly triggered by the low pH of the tumor microenvironment, caused P60-ICG-THP to segregate into two parts: (i) positively charged nanoparticles with a size of approximately 50 nm, and (ii) negatively charged particles of an uneven size. The former, mainly carrying THP (chemotherapeutic agent), could immediately cross the cell membrane and deliver pirarubicin into the nucleus of tumor cells. The latter, carrying ICG (used for photothermal therapy), could also enter the cell via the endocytosis pathway or accumulate in tumor blood vessels to selectively block the supply of nutrients and oxygen (cancer starvation). Both these particles could avoid the rapid excretion of ICG in the liver and were conducive to accumulation in the tumor tissue for photothermal therapy. Conclusion: Our drug delivery system not only achieves the precise subcellular delivery of two anticancer drugs due to their size and charge switches in the tumor site, but also provides a new strategy to combine chemotherapy, photothermal therapy, and cancer starvation therapy for the development of a highly efficient antitumor therapeutic regimen. Ivyspring International Publisher 2020-10-27 /pmc/articles/PMC7667678/ /pubmed/33204335 http://dx.doi.org/10.7150/thno.52000 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
Jiang, Xinglu
Fan, Xiaobo
Zhang, Rui
Xu, Wei
Wu, Hailu
Zhao, Fengfeng
Xiao, Han
Zhang, Chen
Zhao, Chenggui
Wu, Guoqiu
In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy
title In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy
title_full In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy
title_fullStr In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy
title_full_unstemmed In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy
title_short In situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy
title_sort in situ tumor-triggered subcellular precise delivery of multi-drugs for enhanced chemo-photothermal-starvation combination antitumor therapy
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7667678/
https://www.ncbi.nlm.nih.gov/pubmed/33204335
http://dx.doi.org/10.7150/thno.52000
work_keys_str_mv AT jiangxinglu insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT fanxiaobo insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT zhangrui insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT xuwei insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT wuhailu insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT zhaofengfeng insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT xiaohan insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT zhangchen insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT zhaochenggui insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy
AT wuguoqiu insitutumortriggeredsubcellularprecisedeliveryofmultidrugsforenhancedchemophotothermalstarvationcombinationantitumortherapy

Ejemplares similares