| Literature DB >> 20604937 |
Paul Kelly1, Tamara Shawa, Stayner Mwanamakondo, Rose Soko, Geoff Smith, G Robin Barclay, Ian R Sanderson.
Abstract
BACKGROUND: Although micronutrient supplementation can reduce morbidity and mortality due to diarrhoea, nutritional influences on intestinal host defence are poorly understood. We tested the hypothesis that micronutrient supplementation can enhance barrier function of the gut.Entities:
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Year: 2010 PMID: 20604937 PMCID: PMC2910659 DOI: 10.1186/1471-230X-10-72
Source DB: PubMed Journal: BMC Gastroenterol ISSN: 1471-230X Impact factor: 3.067
Composition of the micronutrient tablet
| Micronutrient | Amount | |
|---|---|---|
| β-carotene | 4.8 mg | 4.2 mg equivalent |
| Ascorbic acid (vitamin C) | 70 mg | 40 mg |
| Cholecalciferol (vitamin D3) | 5 μg | - |
| Tocopherol (vitamin E) | 10 mg | 4 mg (uncertain) |
| Thiamine (vitamin B1) | 1.4 mg | 1.0 mg |
| Riboflavin (vitamin B2) | 1.4 mg | 1.3 mg |
| Niacin | 18 mg | 17 mg |
| Pyridoxine (vitamin B6) | 1.9 mg | 1.4 mg |
| Cyanocobalamin (vitamin B12) | 2.6 μg | 1.5 μg |
| Folic acid | 400 μg | 200 μg |
| Iron | 30 mg | 14.8 mg (women), 8.7 mg (men) |
| Zinc | 15 mg | 9.5 mg |
| Copper | 2 mg | 1.2 mg |
| Selenium | 65 μg | 75 μg |
| Iodine | 150 μg | 140 μg |
Composition of the trial medication (one tablet was given each day) compared to the UK recommended nutrient intake (RNI). The RNI for vitamin D in healthy adults exposed to sunlight is zero if appropriate lipid precursors are present in the diet [37].
Demographic and clinical characteristics of study groups for the analysis of gastric acid and the analysis of permeability, translocation and immune activation
| Gastric acid sub-group | Translocation sub-group | |||
|---|---|---|---|---|
| MM | Placebo | MM | Placebo | |
| (n = 100) | (n = 103) | (n = 38) | (n = 49) | |
| Age (yrs) (median, 5th/95th centiles) | 31 (19-65) | 36 (20-62) | 41 (19-56) | 29 (18-51) |
| Sex Male | 35 | 48 | 8 | 14 |
| Female | 65 | 55 | 30 | 35 |
| BMI (kg/m2) (median, 5th/95th centiles) | 21.3 (17.9-31.7) | 21.9 (17.7-31.6) | 22.1 (18.3-36.3) | 23.2 (18.0-41.6) |
| MUAC (cm) (median, 5th/95th centiles) | 28.0 (24.0-38.0) | 27.4 (23.0-34.3) | 26.0 (22.5-37.0) | 26.8 (21.9-38.2) |
| HIV positive | 40 of 97 tested | 44 of 101 tested | 5 of 29 tested | 12 of 46 tested |
| CD4 count (median, 5th/95th centiles) | 382 (68-716) | 349 (161-659) | 362 (331-634) | 466 (190-936) |
| CD4 count < 200 cells/μL | 7/40 | 4/44 | 0/5 | 2/12 |
P values are not shown: none of the comparisons between MM and placebo were significant
Figure 1Gastric pH in relation to HIV status and anti-retroviral therapy. The difference across all groups was significantly different using the Kruskal-Wallis test (P = 0.0005).
Measures of intestinal permeability, absorptive capacity, bacterial translocation, and tumour necrosis factor receptor p55, analysed both by treatment allocation and by HIV status
| Measure | By treatment allocation | By HIV status* | ||||
|---|---|---|---|---|---|---|
| MM | Placebo | HIV positive | HIV negative | |||
| (n = 37) | (n = 49) | (n = 17) | (n = 57) | |||
| Xylose (%) | 21.4 (18.9-27.4) | 21.2 (16.3-26.4) | 0.49 | 20.3 (17.9-23.7) | 21.2 (15.4-27.4) | 0.94 |
| R:G | 0.35 (0.32-0.40) | 0.38 (0.34-0.42) | 0.23 | 0.39 (0.35-0.43) | 0.36 (0.32-0.41) | 0.12 |
| L:R | 0.057 (0.045-0.088) | 0.048 (0.036-0.071) | 0.12 | 0.059 (0.036-0.071) | 0.050 (0.036-0.077) | 0.49 |
| LPS (pg/ml) | 50.7 (24.8-115.1) | 51.6 (22.0-107.9) | 0.52 | 64.7 (29-113) | 51.6 (20-109) | 0.56 |
| anti-LPS IgM (units) | 95 (58-148) | 127 (100-175) | 0.047 | 117 (89-134) | 118 (66-190) | 0.46 |
| anti-LPS IgG (units) | 115 (63-201) | 152 (64-272) | 0.60 | 142 (98-293) | 153 (63-223) | 0.33 |
| TNFp55 (pg/ml) | 1.13 (1.01-1.40) | 1.22 (1.02-1.40) | 0.62 | 1.32 (0.99-1.64) | 1.14 (1.04-1.38) | 0.37 |
* HIV testing was declined by 12 participants. The units given for anti-LPS antibodies are in reference to Scottish blood donor median value (see Methods).
Figure 2Correlation between serum concentrations of TNFR55 and anti-LPS IgM. The correlation coefficient (r = 0.30, P = 0.006) was derived from log-transformed data.
Figure 3Gastric histology. Representative histological sections from gastric biopsies from a patient with (A) normal gastric histology and (B) the most severe gastric atrophy observed, which was classified as mild. No moderate or severe atrophy was seen.