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Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems

Cancer cells have characteristics of acquired and intrinsic resistances to chemotherapy treatment—due to the hostile tumor microenvironment—that create a significant challenge for effective therapeutic regimens. Multidrug resistance, collateral toxicity to normal cells, and detrimental systemic side...

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Autores principales: Kydd, Janel, Jadia, Rahul, Velpurisiva, Praveena, Gad, Aniket, Paliwal, Shailee, Rai, Prakash
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5750652/
https://www.ncbi.nlm.nih.gov/pubmed/29036899
http://dx.doi.org/10.3390/pharmaceutics9040046
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author Kydd, Janel
Jadia, Rahul
Velpurisiva, Praveena
Gad, Aniket
Paliwal, Shailee
Rai, Prakash
author_facet Kydd, Janel
Jadia, Rahul
Velpurisiva, Praveena
Gad, Aniket
Paliwal, Shailee
Rai, Prakash
author_sort Kydd, Janel
collection PubMed
description Cancer cells have characteristics of acquired and intrinsic resistances to chemotherapy treatment—due to the hostile tumor microenvironment—that create a significant challenge for effective therapeutic regimens. Multidrug resistance, collateral toxicity to normal cells, and detrimental systemic side effects present significant obstacles, necessitating alternative and safer treatment strategies. Traditional administration of chemotherapeutics has demonstrated minimal success due to the non-specificity of action, uptake and rapid clearance by the immune system, and subsequent metabolic alteration and poor tumor penetration. Nanomedicine can provide a more effective approach to targeting cancer by focusing on the vascular, tissue, and cellular characteristics that are unique to solid tumors. Targeted methods of treatment using nanoparticles can decrease the likelihood of resistant clonal populations of cancerous cells. Dual encapsulation of chemotherapeutic drug allows simultaneous targeting of more than one characteristic of the tumor. Several first-generation, non-targeted nanomedicines have received clinical approval starting with Doxil(®) in 1995. However, more than two decades later, second-generation or targeted nanomedicines have yet to be approved for treatment despite promising results in pre-clinical studies. This review highlights recent studies using targeted nanoparticles for cancer treatment focusing on approaches that target either the tumor vasculature (referred to as ‘vascular targeting’), the tumor microenvironment (‘tissue targeting’) or the individual cancer cells (‘cellular targeting’). Recent studies combining these different targeting methods are also discussed in this review. Finally, this review summarizes some of the reasons for the lack of clinical success in the field of targeted nanomedicines.
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spelling pubmed-57506522018-01-10 Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems Kydd, Janel Jadia, Rahul Velpurisiva, Praveena Gad, Aniket Paliwal, Shailee Rai, Prakash Pharmaceutics Review Cancer cells have characteristics of acquired and intrinsic resistances to chemotherapy treatment—due to the hostile tumor microenvironment—that create a significant challenge for effective therapeutic regimens. Multidrug resistance, collateral toxicity to normal cells, and detrimental systemic side effects present significant obstacles, necessitating alternative and safer treatment strategies. Traditional administration of chemotherapeutics has demonstrated minimal success due to the non-specificity of action, uptake and rapid clearance by the immune system, and subsequent metabolic alteration and poor tumor penetration. Nanomedicine can provide a more effective approach to targeting cancer by focusing on the vascular, tissue, and cellular characteristics that are unique to solid tumors. Targeted methods of treatment using nanoparticles can decrease the likelihood of resistant clonal populations of cancerous cells. Dual encapsulation of chemotherapeutic drug allows simultaneous targeting of more than one characteristic of the tumor. Several first-generation, non-targeted nanomedicines have received clinical approval starting with Doxil(®) in 1995. However, more than two decades later, second-generation or targeted nanomedicines have yet to be approved for treatment despite promising results in pre-clinical studies. This review highlights recent studies using targeted nanoparticles for cancer treatment focusing on approaches that target either the tumor vasculature (referred to as ‘vascular targeting’), the tumor microenvironment (‘tissue targeting’) or the individual cancer cells (‘cellular targeting’). Recent studies combining these different targeting methods are also discussed in this review. Finally, this review summarizes some of the reasons for the lack of clinical success in the field of targeted nanomedicines. MDPI 2017-10-14 /pmc/articles/PMC5750652/ /pubmed/29036899 http://dx.doi.org/10.3390/pharmaceutics9040046 Text en © 2017 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Review
Kydd, Janel
Jadia, Rahul
Velpurisiva, Praveena
Gad, Aniket
Paliwal, Shailee
Rai, Prakash
Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems
title Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems
title_full Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems
title_fullStr Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems
title_full_unstemmed Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems
title_short Targeting Strategies for the Combination Treatment of Cancer Using Drug Delivery Systems
title_sort targeting strategies for the combination treatment of cancer using drug delivery systems
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5750652/
https://www.ncbi.nlm.nih.gov/pubmed/29036899
http://dx.doi.org/10.3390/pharmaceutics9040046
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