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      Anthracycline Drugs on Modified Surface of Quercetin-Loaded Polymer Nanoparticles: A Dual Drug Delivery Model for Cancer Treatment

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          Abstract

          Polymer nanoparticles are vehicles used for delivery of hydrophobic anti-cancer drugs, like doxorubicin, paclitaxel or chemopreventors like quercetin (Q). The present study deals with the synthesis and characterisation of nano formulations (NFs) from Q loaded PLGA (poly lactic-co-glycolic acid) nano particles (NPs) by surface modification. The surface of Q-loaded (NPs) is modified by coating with biopolymers like bovine serum albumin (BSA) or histones (His). Conventional chemotherapeutic drugs adriamycin (ADR) and mitoxantrone (MTX) are bound to BSA and His respectively before being coated on Q-loaded NPs to nano formulate NF1 and NF2 respectively. The sizes of these NFs are in the range 400–500 nm as ascertained by SEM and DLS measurements. Encapsulation of Q in polymer NPs is confirmed from shifts in FT-IR, TGA and DSC traces of Q-loaded NPs compared to native PLGA and Q. Surface modification in NFs is evidenced by three distinct regions in their TEM images; the core, polymer capsule and the coated surface. Negative zeta potential of Q-loaded NPs shifted to positive potential on surface modification in NF1 and NF2. In vitro release of Q from the NFs lasted up to twenty days with an early burst release. NF2 is better formulation than NF1 as loading of MTX is 85% compared to 23% loading of ADR. Such NFs are expected to overcome multi-drug resistance (MDR) by reaching and treating the target cancerous cells by virtue of size, charge and retention.

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          Most cited references28

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          Challenges in Development of Nanoparticle-Based Therapeutics

          Neil Desai (2012)
          In recent years, nanotechnology has been increasingly applied to the area of drug development. Nanoparticle-based therapeutics can confer the ability to overcome biological barriers, effectively deliver hydrophobic drugs and biologics, and preferentially target sites of disease. However, despite these potential advantages, only a relatively small number of nanoparticle-based medicines have been approved for clinical use, with numerous challenges and hurdles at different stages of development. The complexity of nanoparticles as multi-component three dimensional constructs requires careful design and engineering, detailed orthogonal analysis methods, and reproducible scale-up and manufacturing process to achieve a consistent product with the intended physicochemical characteristics, biological behaviors, and pharmacological profiles. The safety and efficacy of nanomedicines can be influenced by minor variations in multiple parameters and need to be carefully examined in preclinical and clinical studies, particularly in context of the biodistribution, targeting to intended sites, and potential immune toxicities. Overall, nanomedicines may present additional development and regulatory considerations compared with conventional medicines, and while there is generally a lack of regulatory standards in the examination of nanoparticle-based medicines as a unique category of therapeutic agents, efforts are being made in this direction. This review summarizes challenges likely to be encountered during the development and approval of nanoparticle-based therapeutics, and discusses potential strategies for drug developers and regulatory agencies to accelerate the growth of this important field.
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            Nanotechnology in cancer therapeutics: bioconjugated nanoparticles for drug delivery.

            Nanotechnology refers to the interactions of cellular and molecular components and engineered materials-typically, clusters of atoms, molecules, and molecular fragments into incredibly small particles-between 1 and 100 nm. Nanometer-sized particles have novel optical, electronic, and structural properties that are not available either in individual molecules or bulk solids. The concept of nanoscale devices has led to the development of biodegradable self-assembled nanoparticles, which are being engineered for the targeted delivery of anticancer drugs and imaging contrast agents. Nanoconstructs such as these should serve as customizable, targeted drug delivery vehicles capable of ferrying large doses of chemotherapeutic agents or therapeutic genes into malignant cells while sparing healthy cells. Such "smart" multifunctional nanodevices hold out the possibility of radically changing the practice of oncology, allowing easy detection and then followed by effective targeted therapeutics at the earliest stages of the disease. In this article, we briefly discuss the use of bioconjugated nanoparticles for the delivery and targeting of anticancer drugs.
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              Understanding and overcoming major barriers in cancer nanomedicine.

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                Author and article information

                Contributors
                Role: Editor
                Journal
                PLoS One
                PLoS ONE
                plos
                plosone
                PLoS ONE
                Public Library of Science (San Francisco, CA USA )
                1932-6203
                19 May 2016
                2016
                : 11
                : 5
                : e0155710
                Affiliations
                [001]Department of Biotechnology, Maulana Abul Kalam Azad University of Technology, BF-142, Salt Lake, Sector-I, Kolkata 700 064, West Bengal, India
                University of Quebec at Trois-Rivieres, CANADA
                Author notes

                Competing Interests: The authors have declared that no competing interests exist.

                Conceived and designed the experiments: CS. Performed the experiments: AK AD. Analyzed the data: CS. Contributed reagents/materials/analysis tools: SP DM. Wrote the paper: CS AK. Standardised the synthesis of polymer nano particles: SP.

                Article
                PONE-D-16-10972
                10.1371/journal.pone.0155710
                4873127
                27196562
                a41e3bb6-b0da-4542-bd53-7e5e374ed217
                © 2016 Saha et al

                This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

                History
                : 16 March 2016
                : 3 May 2016
                Page count
                Figures: 9, Tables: 0, Pages: 15
                Funding
                Funded by: Department of Science and Technology, New Delhi, India
                Award ID: WOS-A CS 49/12
                Award Recipient :
                This work was funded by Department of Science and Technology, India ( www.dst.gov.in; Dr Chabita Saha; WOS-A CS 49/12).
                Categories
                Research Article
                Medicine and Health Sciences
                Pharmaceutics
                Drug Delivery
                Engineering and Technology
                Nanotechnology
                Nanoparticles
                Medicine and Health Sciences
                Pharmaceutics
                Pharmaceutical Processing Technology
                Drug Synthesis
                Medicine and Health Sciences
                Oncology
                Cancer Treatment
                Research and Analysis Methods
                Microscopy
                Electron Microscopy
                Scanning Electron Microscopy
                Research and Analysis Methods
                Spectrum Analysis Techniques
                Infrared Spectroscopy
                Fourier Transform Infrared Spectroscopy
                Medicine and Health Sciences
                Pharmacology
                Drug Interactions
                Physical Sciences
                Materials Science
                Materials by Attribute
                Coatings
                Engineering and Technology
                Manufacturing Processes
                Surface Treatments
                Coatings
                Custom metadata
                Data is available from Dryad (10.5061/dryad.5gf06).

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                Uncategorized

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