NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINE
Naringenin (NAR), a natural flavonoid aglycone of naringin has been extensively investigated for its pharmacological activities, including anti-tumor effects. However, its poor bioavailability has been identified as the single most important challenge in oral drug delivery. Based in this condition,...
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doaj-153f4d6bf8864c1c8fb853b75d17b68b2020-11-24T22:01:42ZengUniversitas Gadjah MadaIndonesian Journal of Pharmacy2338-94272338-94862015-09-0126314715710.14499/indonesianjpharm26iss3pp147NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINELusia Oktora Ruma Kumala Sari0Agung Endro Nugroho1Dept of Pharmaceutics, Faculty of Pharmacy, University of Jember, Jember 68121, Indonesia;Dept of Pharmacology and Clinical Pharmacy, Faculty of Pharmacy, Universitas Gadjah Mada, Yogyakarta 55281, Indonesia.Naringenin (NAR), a natural flavonoid aglycone of naringin has been extensively investigated for its pharmacological activities, including anti-tumor effects. However, its poor bioavailability has been identified as the single most important challenge in oral drug delivery. Based in this condition, it is used nanoencapsulation to increase the effectiveness of NAR as anti-cancer. The objectives of this research were to develop the formulation of NAR-loaded nanoparticles (NARNPs) as well as to evaluate its potential as anti-cancer against T47D breast cancer cells line. NARNPs is prepared through the method of ionic gelation, meanwhile its characteristic is evaluated through photon correlation spectroscopy (PCS), transmission electron microscopy (TEM), fourier transform infra-red spectroscopy (FTIR), and different scanning calorimeter (DSC). The result of MTT test and cellular uptake indicate that NARNPs increase cytotoxicity and internalization of NAR to the cells compared to that of free NAR. The result of qualitative apoptosis study using fluorescence microscope indicates that both free NAR and NARNPs were able to induce apoptosis. It can be conclude that Chitosan nanoparticles–TPP conjugates have the capability to encapsulate naringenin hence increase the cellular uptake and cytotoxcicity of naringenin against T47D cell line. NARNPs also could induce the apoptosis effect.http://indonesianjpharm.farmasi.ugm.ac.id/index.php/3/article/view/814NARChitosan (CS)ionic gelationnanoparticles |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Lusia Oktora Ruma Kumala Sari Agung Endro Nugroho |
spellingShingle |
Lusia Oktora Ruma Kumala Sari Agung Endro Nugroho NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINE Indonesian Journal of Pharmacy NAR Chitosan (CS) ionic gelation nanoparticles |
author_facet |
Lusia Oktora Ruma Kumala Sari Agung Endro Nugroho |
author_sort |
Lusia Oktora Ruma Kumala Sari |
title |
NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINE |
title_short |
NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINE |
title_full |
NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINE |
title_fullStr |
NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINE |
title_full_unstemmed |
NARINGENIN-LOADED CHITOSAN NANOPARTICLES FORMULATION, AND ITS IN VITRO EVALUATION AGAINST T47D BREAST CANCER CELL LINE |
title_sort |
naringenin-loaded chitosan nanoparticles formulation, and its in vitro evaluation against t47d breast cancer cell line |
publisher |
Universitas Gadjah Mada |
series |
Indonesian Journal of Pharmacy |
issn |
2338-9427 2338-9486 |
publishDate |
2015-09-01 |
description |
Naringenin (NAR), a natural flavonoid aglycone of naringin has been extensively investigated for its pharmacological activities, including anti-tumor effects. However, its poor bioavailability has been identified as the single most important challenge in oral drug delivery. Based in this condition, it is used nanoencapsulation to increase the effectiveness of NAR as anti-cancer. The objectives of this research were to develop the formulation of NAR-loaded nanoparticles (NARNPs) as well as to evaluate its potential as anti-cancer against T47D breast cancer cells line. NARNPs is prepared through the method of ionic gelation, meanwhile its characteristic is evaluated through photon correlation spectroscopy (PCS), transmission electron microscopy (TEM), fourier transform infra-red spectroscopy (FTIR), and different scanning calorimeter (DSC). The result of MTT test and cellular uptake indicate that NARNPs increase cytotoxicity and internalization of NAR to the cells compared to that of free NAR. The result of qualitative apoptosis study using fluorescence microscope indicates that both free NAR and NARNPs were able to induce apoptosis. It can be conclude that Chitosan nanoparticles–TPP conjugates have the capability to encapsulate naringenin hence increase the cellular uptake and cytotoxcicity of naringenin against T47D cell line. NARNPs also could induce the apoptosis effect. |
topic |
NAR Chitosan (CS) ionic gelation nanoparticles |
url |
http://indonesianjpharm.farmasi.ugm.ac.id/index.php/3/article/view/814 |
work_keys_str_mv |
AT lusiaoktorarumakumalasari naringeninloadedchitosannanoparticlesformulationanditsinvitroevaluationagainstt47dbreastcancercellline AT agungendronugroho naringeninloadedchitosannanoparticlesformulationanditsinvitroevaluationagainstt47dbreastcancercellline |
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