Literature DB >> 19583242

Nitric oxide release in human aortic endothelial cells mediated by delivery of amphiphilic polysiloxane nanoparticles to caveolae.

Takehiro Nishikawa1, Norio Iwakiri, Yoshiro Kaneko, Akihiko Taguchi, Kazuhito Fukushima, Hidezo Mori, Nobuhiro Morone, Jun-ichi Kadokawa.   

Abstract

Microdomains such as lipid raft and caveolae are organized as functional compartments in plasma membrane of cells. In this study, we note the functional platform of caveolae with dual functions, internalization of external substances and cell signalings leading to nitric oxide release, and hypothesize that the switching of enzyme activity of endothelial nitric oxide synthase can be achieved by targeting caveolae with nanoparticles. We prepared polysiloxane nanoparticles and studied cellular uptake of the nanoparticles and its concomitant influence on the nitric oxide release in human aortic endothelial cells. We found that polysiloxane nanoparticles were endocytosed via caveolae in human aortic endothelial cells and that enhanced nitric oxide release was followed by the cellular uptake of the nanoparticles. Furthermore, we confirmed that endothelial nitric oxide synthase was activated during cellular uptake of the nanoparticles. These findings support our idea that delivery of the polymeric nanoparticles to endothelial cells can lead to the induction of nitric oxide release.

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Year:  2009        PMID: 19583242     DOI: 10.1021/bm900128x

Source DB:  PubMed          Journal:  Biomacromolecules        ISSN: 1525-7797            Impact factor:   6.988


  10 in total

1.  Dispersion and stability optimization of TiO2 nanoparticles in cell culture media.

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Journal:  Environ Sci Technol       Date:  2010-10-01       Impact factor: 9.028

Review 2.  Nanotechnology based solutions for anti-leishmanial impediments: a detailed insight.

Authors:  Humzah Jamshaid; Fakhar Ud Din; Gul Majid Khan
Journal:  J Nanobiotechnology       Date:  2021-04-15       Impact factor: 10.435

3.  In vitro platelet aggregation and oxidative stress caused by amorphous silica nanoparticles.

Authors:  Abderrahim Nemmar; Priya Yuvaraju; Sumaya Beegam; Javed Yasin; Rauda Al Dhaheri; Mohamed A Fahim; Badreldin H Ali
Journal:  Int J Physiol Pathophysiol Pharmacol       Date:  2015-03-20

Review 4.  Endocytosis of nanomedicines.

Authors:  Gaurav Sahay; Daria Y Alakhova; Alexander V Kabanov
Journal:  J Control Release       Date:  2010-03-10       Impact factor: 9.776

5.  Silica Nanoparticle-Endothelial Interaction: Uptake and Effect on Platelet Adhesion under Flow Conditions.

Authors:  Jiban Saikia; Raziye Mohammadpour; Mostafa Yazdimamaghani; Hannah Northrup; Vladimir Hlady; Hamidreza Ghandehari
Journal:  ACS Appl Bio Mater       Date:  2018-11-30

6.  Amorphous silica nanoparticles trigger nitric oxide/peroxynitrite imbalance in human endothelial cells: inflammatory and cytotoxic effects.

Authors:  J Jose Corbalan; Carlos Medina; Adam Jacoby; Tadeusz Malinski; Marek W Radomski
Journal:  Int J Nanomedicine       Date:  2011-11-09

7.  Silica nanoparticles induce oxidative stress, inflammation, and endothelial dysfunction in vitro via activation of the MAPK/Nrf2 pathway and nuclear factor-κB signaling.

Authors:  Caixia Guo; Yinye Xia; Piye Niu; Lizhen Jiang; Junchao Duan; Yang Yu; Xianqing Zhou; Yanbo Li; Zhiwei Sun
Journal:  Int J Nanomedicine       Date:  2015-02-20

Review 8.  Role of Physicochemical Properties in Nanoparticle Toxicity.

Authors:  Seung Won Shin; In Hyun Song; Soong Ho Um
Journal:  Nanomaterials (Basel)       Date:  2015-08-19       Impact factor: 5.076

9.  Amorphous silica nanoparticles aggregate human platelets: potential implications for vascular homeostasis.

Authors:  J Jose Corbalan; Carlos Medina; Adam Jacoby; Tadeusz Malinski; Marek W Radomski
Journal:  Int J Nanomedicine       Date:  2012-02-07

Review 10.  Insight into Cellular Uptake and Intracellular Trafficking of Nanoparticles.

Authors:  Parisa Foroozandeh; Azlan Abdul Aziz
Journal:  Nanoscale Res Lett       Date:  2018-10-25       Impact factor: 4.703

  10 in total

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