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In Vitro Models for Studying Secondary Plant Metabolite Digestion and Bioaccessibility
Authors:M Alminger  A‐M Aura  T Bohn  C Dufour  SN El  A Gomes  S Karakaya  MC Martínez‐Cuesta  GJ McDougall  T Requena  CN Santos
Affiliation:1. Dept. of Chemical and Biological Engineering, Chalmers Univ. of Technology, , Gothenburg, Sweden;2. VTT Technical Research Centre of Finland, , P.O.Box 1000, Espoo, Finland;3. Environment and Agro‐biotechnologies Dept, Centre de Recherche Public – Gabriel Lippmann, , 4422 Belvaux, Luxembourg;4. INRA, UMR408 Safety and Quality of Plant Products F‐84000 Avignon, , France;5. Univ. of Avignon, UMR408 Safety and Quality of Plant Products F‐84000 Avignon, , France;6. Engineering Faculty Dept. of Food Engineering, , Turkey;7. Inst. de Biologia Experimental e Tecnológica, , Portugal;8. Inst. de Tecnologia Química e Biológica, Univ. Nova de Lisboa, , Portugal;9. Inst. de Investigación en Ciencias de la Alimentación CIAL (CSIC‐UAM), , Spain;10. The James Hutton Inst., Invergowrie, DD2 5DA, , Dundee, United Kingdom
Abstract:There is an increased interest in secondary plant metabolites, such as polyphenols and carotenoids, due to their proposed health benefits. Much attention has focused on their bioavailability, a prerequisite for further physiological functions. As human studies are time consuming, costly, and restricted by ethical concerns, in vitro models for investigating the effects of digestion on these compounds have been developed and employed to predict their release from the food matrix, bioaccessibility, and assess changes in their profiles prior to absorption. Most typically, models simulate digestion in the oral cavity, the stomach, the small intestine, and, occasionally, the large intestine. A plethora of models have been reported, the choice mostly driven by the type of phytochemical studied, whether the purpose is screening or studying under close physiological conditions, and the availability of the model systems. Unfortunately, the diversity of model conditions has hampered the ability to compare results across different studies. For example, there is substantial variability in the time of digestion, concentrations of salts, enzymes, and bile acids used, pH, the inclusion of various digestion stages; and whether chosen conditions are static (with fixed concentrations of enzymes, bile salts, digesta, and so on) or dynamic (varying concentrations of these constituents). This review presents an overview of models that have been employed to study the digestion of both lipophilic and hydrophilic phytochemicals, comparing digestive conditions in vitro and in vivo and, finally, suggests a set of parameters for static models that resemble physiological conditions.
Keywords:phytochemicals  carotenoids  polyphenols  gastrointestinal digestion  in vitro models  bioacessibility
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