Comparing Soluble Ferric Pyrophosphate to Common Iron Salts and Chelates as Sources of Bioavailable Iron in a Caco-2 Cell Culture Model

Comparing Soluble Ferric Pyrophosphate to Common Iron Salts and Chelates as Sources of Bioavailable Iron in a Caco-2 Cell Culture Model

Iron bioavailability from supplements and fortificants varies depending upon the form of the iron and the presence or absence of iron absorption enhancers and inhibitors. Our objectives were to compare the effects of pH and selected enhancers and inhibitors and food matrices on the bioavailability o...

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Veröffentlicht in:Journal of agricultural and food chemistry 2009-06, Vol.57 (11), p.5014-5019
Hauptverfasser: Zhu, Le, Glahn, Raymond P, Nelson, Deanna, Miller, Dennis D
Format: Artikel
Sprache:eng
Schlagworte:
ascorbic acid
Biological and medical sciences
Biological Availability
Caco-2 Cells
calcium
chelating agents
citric acid
cultured cells
dietary mineral supplements
dietary minerals
Diphosphates - chemistry
Diphosphates - pharmacokinetics
ferritin
food additives
Food Chemistry/Biochemistry
food fortification
Food industries
food matrix
Fundamental and applied biological sciences. Psychology
human cell lines
Humans
iron
Iron - chemistry
Iron - pharmacokinetics
Iron Chelating Agents - chemistry
Iron Chelating Agents - pharmacokinetics
iron phosphates
Iron, Dietary - pharmacokinetics
magnesium
model food systems
Models, Biological
nutrient availability
nutrient-nutrient interactions
phytic acid
Phytic Acid - chemistry
Solubility
soluble ferric pyrophosphate
sulfates
tannins
Tannins - chemistry
zinc
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Zusammenfassung:Iron bioavailability from supplements and fortificants varies depending upon the form of the iron and the presence or absence of iron absorption enhancers and inhibitors. Our objectives were to compare the effects of pH and selected enhancers and inhibitors and food matrices on the bioavailability of iron in soluble ferric pyrophosphate (SFP) to other iron fortificants using a Caco-2 cell culture model with or without the combination of in vitro digestion. Ferritin formation was the highest in cells treated with SFP compared to those treated with other iron compounds or chelates. Exposure to pH 2 followed by adjustment to pH 7 markedly decreased FeSO4 bioavailability but had a smaller effect on bioavailabilities from SFP and sodium iron(III) ethylenediaminetetraacetate (NaFeEDTA), suggesting that chelating agents minimize the effects of pH on iron bioavailabilty. Adding ascorbic acid (AA) and cysteine to SFP in a 20:1 molar ratio increased ferritin formation by 3- and 2-fold, respectively, whereas adding citrate had no significant effect on the bioavailability of SFP. Adding phytic acid (10:1) and tannic acid (1:1) to iron decreased iron bioavailability from SFP by 91 and 99%, respectively. The addition of zinc had a marked inhibitory effect on iron bioavailability. Calcium and magnesium also inhibited iron bioavailability but to a lesser extent. Incorporating SFP in rice greatly reduced iron bioavailability from SFP, but this effect can be partially reversed with the addition of AA. SFP and FeSO4 were taken up similarly when added to nonfat dry milk. Our results suggest that dietary factors known to enhance and inhibit iron bioavailability from various iron sources affect iron bioavailability from SFP in similar directions. However, the magnitude of the effects of iron absorption inhibitors on SFP iron appears to be smaller than on iron salts, such as FeSO4 and FeCl3. This supports the hypothesis that SFP is a promising iron source for food fortification and dietary supplements.
ISSN:0021-8561
1520-5118
DOI:10.1021/jf900328t