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A supplementation study in human subjects with a combination of meso-zeaxanthin, (3R,3′R)-zeaxanthin and (3R,3′R,6′R)-lutein

Published online by Cambridge University Press:  01 December 2008

David I. Thurnham*
Affiliation:
Northern Ireland Centre for Food and Health (NICHE), University of Ulster, Coleraine BT51 4LA, UK
Aurélie Trémel
Affiliation:
Institut National Supérieur de Formation Agroalimentaire, 65 rue de St Brieuc, Rennes cedex CS 84215-35042, France
Alan N. Howard
Affiliation:
Downing College, University of Cambridge, Cambridge CB2 1DQ, UK
*
*Corresponding author: Professor D. I. Thurnham, fax +44 1223 437515, email di.thurnham@ulster.ac.uk
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Abstract

We measured the blood uptake of meso-zeaxanthin (MZ) from a mixture of macular pigments since its bioavailability in man has not been studied. Volunteers (ten men and nine women) were recruited and received one capsule of Lutein Plus®/d. Blood was taken at baseline, day 10 and day 22. One capsule contained 10·8 mg lutein, 1·2 mg (3R,3′R)-zeaxanthin and 8·0 mg MZ. Plasma lutein and total zeaxanthin concentrations were quantified using isocratic liquid chromatography and the eluting xanthophyll fractions were collected and re-chromatographed on a chiral column to assess the proportion of MZ. Plasma concentrations per mg dose at day 22 suggested that (3R,3′R)-zeaxanthin (0·088 μmol/l per mg) was about 50 % more actively retained by the body than lutein (0·056 μmol/l per mg) (although the difference was not significant in women) and 2·5–3·0 times more than MZ (0·026 μmol/l per mg). Concentrations of MZ at day 22 were 2·5 times higher in women than men. The plasma responses from lutein and (3R,3′R)-zeaxanthin in the Lutein Plus® were lower than literature values for the pure substances. That is, their uptake into plasma appeared to be slightly depressed by the presence of MZ. Plasma concentrations of β-carotene were depressed by about 50 % at day 10 and about 35 % at day 22. In conclusion, the lower plasma response to MZ compared with (3R,3′R)-zeaxanthin probably indicates that MZ is less well absorbed than (3R,3′R)-zeaxanthin but work with pure MZ will be needed to confirm that the lower plasma response was not due to the large amount of lutein in the Lutein Plus®.

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Type
Full Papers
Copyright
Copyright © The Authors 2008
Figure 0

Fig. 1 Structures of the three principal xanthophyll carotenoids found in the macular pigment of the eye.

Figure 1

Fig. 2 Chromatography of xanthophyll pigments in a plasma extract of a sample collected on day 22. In the Ultracarb system the peak elution times of lutein and total zeaxanthin were 8.6 and 9.4 min respectively. The total volume between 8.4 and 9.8 min was collected for rechromatography on the chiral column because of initial uncertainty of the identity of the substance eluting between the two main peaks.

Figure 2

Table 1 Plasma lutein and zeaxanthin concentrations at baseline, day 10 and day 21 in the male and female volunteers supplemented with a combination of meso-zeaxanthin (MZ), (3R,3′R)-zeaxanthin and lutein*(Mean values and standard deviations)

Figure 3

Table 2 Relative increases in plasma concentrations of lutein, meso-zeaxanthin (MZ) and 3R,3′R-zeaxanthin to doses of respective xanthophylls from Lutein Plus®*(Mean values and standard deviations)

Figure 4

Fig. 3 Plasma xanthophyll concentrations at plateau following 21 d supplementation with the doses shown. The increases in plasma concentrations are shown of lutein (•), (3R,3′R)-zeaxanthin (△) and meso-zeaxanthin (MZ; ○) following 21 d oral supplementation. * Indicates the responses from xanthophylls in Lutein Plus® (1·2 mg (3R,3′R)-zeaxanthin, 10·8 mg lutein and 8 mg MZ). The other data on lutein are from Thurmann et al.(23) and on (3R,3′R)-zeaxanthin from Hartmann et al.(24). Response lines are forced through zero.