Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical Trials
Traditional systemic chemotherapy involves the wide distribution of drug molecules in the body, causing toxic side effects in the healthy tissues and limiting the therapeutic dose required at the site of drug action. In order to decrease side effects and increase the drug efficacy, recent research...
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Canadian Society for Pharmaceutical Sciences
2020-05-01
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| Series: | Journal of Pharmacy & Pharmaceutical Sciences |
| Online Access: | https://journals.library.ualberta.ca/jpps/index.php/JPPS/article/view/30583 |
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doaj-16a602555a4c4b56884c11b63bde1c082020-11-25T04:05:20ZengCanadian Society for Pharmaceutical SciencesJournal of Pharmacy & Pharmaceutical Sciences1482-18262020-05-0123110.18433/jpps30583Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical TrialsZahra Eskandari0Fatemeh Bahadori1Burak Celik2Hayat Onyuksel3Department of Chemistry, Biochemistry Division, Faculty of Sciences and Arts, Yildiz Technical University, Istanbul, Turkey. & Department of Pharmaceutical Biotechnology, Faculty of Pharmacy, BezmialemVakif University, Istanbul, Turkey.Department of Pharmaceutical Biotechnology, Faculty of Pharmacy, BezmialemVakif University, Istanbul, Turkey.Department of Pharmaceutical Biotechnology, Faculty of Pharmacy, BezmialemVakif University, Istanbul, Turkey.Department of Biopharmaceutical Sciences, University of Illinois at Chicago, Chicago, IL USA. Traditional systemic chemotherapy involves the wide distribution of drug molecules in the body, causing toxic side effects in the healthy tissues and limiting the therapeutic dose required at the site of drug action. In order to decrease side effects and increase the drug efficacy, recent research on chemotherapy focuses on drug targeting. Targeted therapy can be achieved by several mechanisms including; 1) using an antibody as a drug that is specific to a disease biomarker, 2) using an antibody (or peptide) as a targeting agent conjugated to the drug molecule, 3) delivering the drug molecules to the target tissue in a nano-carrier with or without the targeting agent attached on its surface. The third approach involves the nanomedicines that can be targeted to diseased tissues by both passive (extravasating at diseased sites due to leaky vasculature) and active (specific interaction of the targeting agent with disease biomarker) targeting mechanisms. In this review we will cover the passively targeted nanomedicines prepared using nano drug carriers. Ideally the carrier particle should be in the right size (1-100nm), stable enough to prevent drug leakage during circulation, and safe not to cause any damage to healthy tissues. Competition for all these properties generated many different types of materials to be used as nanodrug delivery systems. After a brief review of most commonly used drug carriers, we discuss the clinical use of the targeted nanomedicines with regard to their pharmacokinetic and pharmacodynamics properties, and how these properties vary from conventional formulations providing free drugs in the circulation after administration. https://journals.library.ualberta.ca/jpps/index.php/JPPS/article/view/30583 |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Zahra Eskandari Fatemeh Bahadori Burak Celik Hayat Onyuksel |
| spellingShingle |
Zahra Eskandari Fatemeh Bahadori Burak Celik Hayat Onyuksel Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical Trials Journal of Pharmacy & Pharmaceutical Sciences |
| author_facet |
Zahra Eskandari Fatemeh Bahadori Burak Celik Hayat Onyuksel |
| author_sort |
Zahra Eskandari |
| title |
Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical Trials |
| title_short |
Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical Trials |
| title_full |
Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical Trials |
| title_fullStr |
Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical Trials |
| title_full_unstemmed |
Targeted Nanomedicines for Cancer Therapy, From Basics to Clinical Trials |
| title_sort |
targeted nanomedicines for cancer therapy, from basics to clinical trials |
| publisher |
Canadian Society for Pharmaceutical Sciences |
| series |
Journal of Pharmacy & Pharmaceutical Sciences |
| issn |
1482-1826 |
| publishDate |
2020-05-01 |
| description |
Traditional systemic chemotherapy involves the wide distribution of drug molecules in the body, causing toxic side effects in the healthy tissues and limiting the therapeutic dose required at the site of drug action. In order to decrease side effects and increase the drug efficacy, recent research on chemotherapy focuses on drug targeting. Targeted therapy can be achieved by several mechanisms including; 1) using an antibody as a drug that is specific to a disease biomarker, 2) using an antibody (or peptide) as a targeting agent conjugated to the drug molecule, 3) delivering the drug molecules to the target tissue in a nano-carrier with or without the targeting agent attached on its surface. The third approach involves the nanomedicines that can be targeted to diseased tissues by both passive (extravasating at diseased sites due to leaky vasculature) and active (specific interaction of the targeting agent with disease biomarker) targeting mechanisms. In this review we will cover the passively targeted nanomedicines prepared using nano drug carriers. Ideally the carrier particle should be in the right size (1-100nm), stable enough to prevent drug leakage during circulation, and safe not to cause any damage to healthy tissues. Competition for all these properties generated many different types of materials to be used as nanodrug delivery systems. After a brief review of most commonly used drug carriers, we discuss the clinical use of the targeted nanomedicines with regard to their pharmacokinetic and pharmacodynamics properties, and how these properties vary from conventional formulations providing free drugs in the circulation after administration.
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| url |
https://journals.library.ualberta.ca/jpps/index.php/JPPS/article/view/30583 |
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