Publication:
Release behavior and cytotoxicity of captopril-intercalated layered double hydroxide for an antihypertensive drug delivery system

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Date
2023
Authors
Jadam M.L.
Jubri Z.
Sarijo S.H.
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Springer
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Abstract
Intercalation of an antihypertensive drug, captopril (CPL) into zinc�aluminum-layered (ZAL) double hydroxide carrier was successfully accomplished via co-precipitation method. The resulting material was investigated by powder X-ray diffraction, Fourier transform infrared spectroscopy, thermogravimetric and differential thermogravimetric�(TGA/DTG) analysis, carbon, hydrogen, nitrogen, and sulfur (CHNS) analysis, field emission scanning electron microscopy, and accelerated surface area and porosity (ASAP) analysis. High loading percentage of CPL (61.6% [w/w]) in zinc�aluminum�captopril-layered double hydroxide (ZAC) with an interlayer spacing of 9.7 � suggested the successful intercalation of CPL into the ZAL interlayer. Release percentages of the drug into Na3PO4, Na2CO3, and NaCl solutions are 48%, 30%, and 24%, respectively. Pseudo-second order kinetic model with correlation coefficient, r2 > 0.9 best defined the release behavior of CPL from ZAC nanocomposite into the aqueous media. Cytotoxicity study reveals lower toxic nature of ZAC nanohybrid (IC50 > 200��g/mL) compared to pristine CPL drug (IC50 < 200��g/mL) when tested on HUVEC and 3T3 cells. For the work described in this research, the organic-inorganic hybrid nanocomposite, ZAC could have good application in slow releases formulation of the drug delivery system. � 2022, The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.
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Antihypertensive drug , Captopril , Controlled release , Drug delivery system , Zinc�aluminum-layered double hydroxide , Aluminum compounds , Controlled drug delivery , Drug products , Field emission microscopes , Fourier transform infrared spectroscopy , Nanocomposites , Precipitation (chemical) , Targeted drug delivery , Thermogravimetric analysis , Zinc , Antihypertensive drugs , Captopril , Controlled release , Coprecipitation method , Drug-delivery systems , Layered-double hydroxides , Release behaviors , Zinc aluminiums , Zinc-aluminum , Zinc�aluminum-layered double hydroxide , Scanning electron microscopy
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https://www.scopus.com/inward/record.uri?eid=2-s2.0-85137438305&doi=10.1007%2fs10934-022-01333-y&partnerID=40&md5=75938b3daa28293a31b8b1c28c71003e
 https://irepository.uniten.edu.my/handle/123456789/34410
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