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In vitro and in vivo assessment of vitamin A encapsulation in a liposome–protein delivery system

Thumbnail
Autor
Rovoli M., Pappas I., Lalas S., Gortzi O., Kontopidis G.
Fecha
2019
Language
en
DOI
10.1080/08982104.2018.1502314
Materia
beta lactoglobulin
liposome
membrane protein
phospholipid
retinol
sterol
antioxidant
lactoglobulin
liposome
phospholipid
retinol
sterol
absorption
adult
animal experiment
antioxidant activity
area under the curve
Article
biochemistry
comparative study
controlled study
drug bioavailability
drug blood level
drug clearance
drug half life
drug solubility
encapsulation
in vitro study
in vivo study
limit of detection
limit of quantitation
lipid composition
liposomal delivery
male
maximum concentration
mouse
nonhuman
priority journal
retention time
time to maximum plasma concentration
animal
bioavailability
C57BL mouse
CBA mouse
chemistry
drug stability
oxidation reduction reaction
solubility
Animals
Antioxidants
Biological Availability
Drug Stability
Lactoglobulins
Liposomes
Male
Mice, Inbred C57BL
Mice, Inbred CBA
Oxidation-Reduction
Phospholipids
Solubility
Sterols
Vitamin A
Taylor and Francis Ltd
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Resumen
Vitamin A (VA) is an essential nutrient needed in small amounts by humans and supports a wide range of biological actions. Retinol, the most common and most biologically active form of VA has also been found to inhibit peroxidation processes in membranes and it has been widely used as an ingredient with pharmaceutical and nutritional applications. VA is a lipophilic molecule, sensitive to air, oxidizing agents, ultraviolet light and low pH levels. For these reasons, it is necessary for VA to be protected against oxidation. Another disadvantage in the application of VA is its low solubility in aqueous media. Both issues (sensitivity and solubility) can be solved by employing encapsulation techniques. Liposomes can efficiently encapsulate lipid-soluble materials, such as VA. The encapsulated materials are protected from environmental and chemical changes. A new liposome/β-lactoglobulin formulation has been developed as a stable delivery system for VA. The aim of this study was the encapsulation of VA into β-lactoglobulin–liposome complexes, recently developed in our laboratory. The in vivo bioavailability characterization of VA was tested after administration in laboratory animals (mice). In this report, we demonstrate that VA could be efficiently entrapped and delivered in a phospholipid–sterol–protein membrane resembling system, a newly synthesized promising carrier. Based on this finding, the phospholipid–sterol–protein membrane resembling system may be one of the promising approaches to enhance VA absorption and to overcome the formulation difficulties associated with lipophilic means. The carrier system described here has huge potential in food fortification applications to treat VA deficiency. © 2018, © 2018 Informa UK Limited, trading as Taylor & Francis Group.
URI
http://hdl.handle.net/11615/78612
Colecciones
  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ. [19735]

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