Open Access

Scientific Reports

, volume 10 , issue 1 , publication number 909

Characterization of chitosan/alginate/lovastatin nanoparticles and investigation of their toxic effects in vitro and in vivo

T Q Hoang ^{1, 2}

Chinh Thuy Nguyen ¹

Loc Thi Thach ³

Mai Thi Tran ¹

Huynh Duc Mai ¹

Trang Thi Thu Nguyen ¹

Giang Duc Le ³

Mao Van Can ⁴

Lam Dai Tran ^{1, 2}

Giang Long Bach ⁵

Kavitha Ramadass ⁶

C. I. Sathish ⁶

Quan Van Le ⁷

Hide authors affiliations Show authors affiliations: 7 affiliations

Institute for Tropical Technology, Vietnam Academy of Science and Technology, Cau Giay, Vietnam

Vietnam Academy of Science and Technology

Institute for Tropical Technology

Graduate University of Science and Technology, Vietnam Academy of Science and Technology, Cau Giay, Vietnam |

Vinh, University, Vinh, Vietnam |

⁴

Department of Pathophysiology, Vietnam Military Medical University, Ha Dong, Vietnam |

⁵

NTT Institute of High Technology, Nguyen Tat Thanh University, Ho Chi Minh city, Vietnam |

⁶

Global Innovative Center for Advanced Nanomaterials, Faculty of Engineering and Built Environment, The University of Newcastle, Callaghan, Australia |

⁷

Department of Functional Exploration, Military Hospital 103, Ha Dong, Vietnam |

Publication type: Journal Article

Publication date: 2020-01-22

Springer Nature

Scientific Reports

scimago Q1

wos Q1

SJR: 0.874

CiteScore: 6.7

Impact factor: 3.9

ISSN: 20452322

DOI: 10.1038/s41598-020-57666-8

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PubMed ID: 31969608

Multidisciplinary

Abstract

In this study, chitosan and alginate were selected to prepare alginate/chitosan nanoparticles to load the drug lovastatin by the ionic gelation method. The synthesized nanoparticles loaded with drug were characterized by Fourier transform infrared spectroscopy (FT-IR), scanning electron microscopy (SEM), laser scattering and differential scanning calorimetry (DSC) methods. The FTIR spectrum of the alginate/chitosan/lovastatin nanoparticles showed that chitosan and alginate interacted with lovastatin through hydrogen bonding and dipolar-dipolar interactions between the C-O, C=O, and OH groups in lovastatin, the C-O, NH, and OH groups in chitosan and the C-O, C=O, and OH groups in alginate. The laser scattering results and SEM images indicated that the alginate/chitosan/lovastatin nanoparticles have a spherical shape with a particle size in the range of 50–80 nm. The DSC diagrams displayed that the melting temperature of the alginate/chitosan/lovastatin nanoparticles was higher than that of chitosan and lower than that of alginate. This result means that the alginate and chitosan interact together, so that the nanoparticles have a larger crystal degree when compared with alginate and chitosan individually. Investigations of the in vitro lovastatin release from the alginate/chitosan/lovastatin nanoparticles under different conditions, including different alginate/chitosan ratios, different solution pH values and different lovastatin contents, were carried out by ultraviolet-visible spectroscopy. The rate of drug release from the nanoparticles is proportional to the increase in the solution pH and inversely proportional to the content of the loaded lovastatin. The drug release process is divided into two stages: a rapid stage over the first 10 hr, then the release becomes gradual and stable. The Korsmeyer-Peppas model is most suitable for the lovastatin release process from the alginate/chitosan/lovastatin nanoparticles in the first stage, and then the drug release complies with other models depending on solution pH in the slow release stage. In addition, the toxicity of alginate/chitosan/lovastatin (abbreviated ACL) nanoparticles was sufficiently low in mice in the acute toxicity test. The LD50 of the drug was higher than 5000 mg/kg, while in the subchronic toxicity test with treatments of 100 mg/kg and 300 mg/kg ACL nanoparticles, there were no abnormal signs, mortality, or toxicity in general to the function or structure of the crucial organs. The results show that the ACL nanoparticles are safe in mice and that these composite nanoparticles might be useful as a new drug carrier.

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1 citation

Manh Quoc

21 publications, 163 citations

h-index: 5

Thanh Do University

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Hoang T. Q. et al. Characterization of chitosan/alginate/lovastatin nanoparticles and investigation of their toxic effects in vitro and in vivo // Scientific Reports. 2020. Vol. 10. No. 1. 909

GOST all authors (up to 50) Copy

Hoang T. Q., Thuy Nguyen C., Thi Thach L., Thi Tran M., Duc Mai H., Thi Thu Nguyen T., Duc Le G., Van Can M., Dai Tran L., Long Bach G., Ramadass K., Sathish C. I., Van Le Q. Characterization of chitosan/alginate/lovastatin nanoparticles and investigation of their toxic effects in vitro and in vivo // Scientific Reports. 2020. Vol. 10. No. 1. 909

RIS |

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RIS Copy

TY - JOUR

DO - 10.1038/s41598-020-57666-8

UR - https://doi.org/10.1038/s41598-020-57666-8

TI - Characterization of chitosan/alginate/lovastatin nanoparticles and investigation of their toxic effects in vitro and in vivo

T2 - Scientific Reports

AU - Hoang, T Q

AU - Thuy Nguyen, Chinh

AU - Thi Thach, Loc

AU - Thi Tran, Mai

AU - Duc Mai, Huynh

AU - Thi Thu Nguyen, Trang

AU - Duc Le, Giang

AU - Van Can, Mao

AU - Dai Tran, Lam

AU - Long Bach, Giang

AU - Ramadass, Kavitha

AU - Sathish, C. I.

AU - Van Le, Quan

PY - 2020

DA - 2020/01/22

PB - Springer Nature

IS - 1

VL - 10

PMID - 31969608

SN - 2045-2322

ER -

BibTex

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BibTex (up to 50 authors) Copy

@article{2020_Hoang,

author = {T Q Hoang and Chinh Thuy Nguyen and Loc Thi Thach and Mai Thi Tran and Huynh Duc Mai and Trang Thi Thu Nguyen and Giang Duc Le and Mao Van Can and Lam Dai Tran and Giang Long Bach and Kavitha Ramadass and C. I. Sathish and Quan Van Le},

title = {Characterization of chitosan/alginate/lovastatin nanoparticles and investigation of their toxic effects in vitro and in vivo},

journal = {Scientific Reports},

year = {2020},

volume = {10},

publisher = {Springer Nature},

month = {jan},

url = {https://doi.org/10.1038/s41598-020-57666-8},

number = {1},

pages = {909},

doi = {10.1038/s41598-020-57666-8}

}

Publisher

Springer Nature

Journal

Scientific Reports

scimago Q1

wos Q1

SJR

0.874

CiteScore

6.7

Impact factor

3.9

ISSN

20452322 (Print, Electronic)