Few studies have investigated the association between dietary intake and blood concentrations of water-soluble vitamins in patients with ulcerative colitis (UC). In the present study, vitamin concentrations were measured in the blood and urinary excretion of 23 outpatients with UC and compared against a control group of 20 healthy participants. A weighed food record procedure was used to ensure controlled macronutrient and vitamin intakes of the UC cohort. Individuals in the control group were given a semi-purified diet for 8 days prior to assessment. Multiple linear regression analysis was used to identify important differences in vitamin concentrations, independent of sex, age and other confounding variables. The blood concentrations of vitamins B2, C, niacin and folate were markedly lower in the patients with UC than those in the control group, and the renal clearance of vitamins B1, B6, B12 and folate was notably higher in the UC cohort. It was concluded that vitamins B2, C, niacin and folate were at significantly lower concentrations in patients with UC following adjustment for coexisting factors. The lower levels of niacin may be partially due to impaired reabsorption. Chronic inflammation, common in patients with UC, with may contribute to the lower levels of other vitamins by rendering amino acid and carbohydrate metabolism into a hypermetabolic state. As the role of vitamins in metabolic activity is constant and pervasive, nutritional management including the application of water-soluble vitamins appears important for patients suffering from UC.
Ulcerative colitis (UC) is a chronic inflammatory disease of the large intestine, the characteristic symptoms of which are abdominal pain and cramping, blood in stools, diarrhea, vomiting and weight loss (
Vitamins, in their presence as much as their absence, are important in the pathophysiology of IBD. The most serious problem associated with vitamins in IBD is anemia due to deficiencies in iron, vitamin B12 or folate. The causes of these deficiencies are different: Iron is depleted by chronic gastrointestinal blood loss; vitamin B12 is inhibited by malabsorption secondary to terminal ileitis; folate deficiency may occur as a result of sulfasalazine therapy (
Although there has been interest in the involvement of vitamins in the development and relapse of UC, there is limited data on the association between dietary intake and blood concentrations of water-soluble vitamins in patients with UC. With this in mind, the aim of the present study was to make a comprehensive comparison between the concentrations of water-soluble vitamins in the blood and urinary excretion of UC sufferers with a group of healthy control subjects.
A total of 23 patients (in remission, 8 men and 9 women; with active UC, 2 men and 4 women; mean age, 43.6 years; range: 20-74 years) who visited the outpatient clinic of Shiga University of Medical Science Hospital (Shiga, Japan) were enrolled in the present study. All patients were treated with medicines for UC, including salazosulfapyridine (SASP) and 5-ASA. A number of patients were treated with prednisolone or an immunosuppressant, including azathioprine. The study was fully explained to each patient and they provided informed consent. Patients with UC reporting a history of major abdominal surgery, including colectomy, or of other gastrointestinal illness, carcinoma or other inflammatory and infectious disorders were excluded. This part of the study was performed between August and December 2010, in accordance with the Helsinki Declaration (October 2000). The protocol for was approved by the Institutional Review Board of the Shiga University of Medical Science. (no. 22-41, 2010).
A total of 20 healthy, Japanese college students (10 men/10 women, mean age: 20.7 years, range 19-23 years), volunteered for the present study. The physical examination and blood tests performed prior to the experiment showed normal values. The study was reviewed and approved by the Ethical Committee of the Independent Administrative Agency, National Institute of Health and Nutrition (Tokyo, Japan). All participants were housed in the same facility for 8 days. A daily schedule imposed lights-out at 10:00 p.m. in order to promote sleep and wake-up at 06:00 a.m. The precise design of the experiment has been described elsewhere (
Fasting blood samples were collected in EDTA tubes. Whole blood and plasma samples were stored at -20˚C for later analysis. In addition 24-h urine samples were collected on the day prior to the blood tests. The urine samples were maintained on ice until they had been measured and were immediately analyzed in order to avoid the destruction of water-soluble vitamins. The method of analysis is described below under. Following analysis, the samples were stored at -20˚C.
The collection of 24-h urine samples was performed from the second urination on day 7 to the first urination on day 8. Following measurement of the urine samples, they were immediately treated following the same protocol as the patients with UC in the preceding paragraph. Blood samples were collected from a cubital vein at 08:30 a.m., prior to breakfast on day 8, were analyzed immediately to avoid the destruction of water-soluble vitamins and were then stored at -20˚C.
Food intake was recorded by each patient using a weighed food record procedure with supplemental use of photography at home. A registered dietician provided instructions on weighing and taking photographs. This regime was followed for 3 days prior to assessment. The validation of this method has been reported elsewhere (
The mealtimes were as follows: Breakfast at 08:00-09:00 a.m., lunch at 12:30-13:10 p.m., and dinner at 18:30-19:00 p.m. The subjects consumed a semi-purified diet based on Japanese Dietary Reference Intakes (
Thiamin hydrochloride, riboflavin, pyridoxine hydrochloride, pyridoxal phosphate monohydrate, cyanocobalamin, nicotinamide, folate (pteroylmonoglutamic acid), and L (+)-ascorbic acid were purchased from Wako Pure Chemical Industries (Osaka, Japan). 4-Pyridoxic acid was made by ICN Pharmaceuticals (Costa Mesa, CA, USA) and obtained from Wako Pure Chemical Industries. N1-Methylnicotinamide (MNA) chloride was purchased from Tokyo Chemical Industries (Tokyo, Japan).
The concentrations of total vitamin B1 in the whole blood and urine samples were measured using the high performance liquid chromatography (HPLC)-post-labeled fluorescence method of Kimura
The body surface area (BSA) was calculated using the following formula: BSA = 0.007184 x body weight (kg)0.425 x height (cm)0.725 (
SPSS Statistics version 23.0 (IBM Corp., Armonk, NY, USA) was used. The χ2 test was used to compare dichotomous variables among controls, patients with active UC, and patients with UC in remission. Student's t-test was used to confirm whether the means of two groups were statistically different from each other. One-way analysis of variance was used to compare the means of three groups, followed by post hoc application of the Tukey test when the F-value was significantly different at P<0.05. With the exception of vitamin B2, almost none of the means of variables in the patients with UC were statistically different when active and remission cases were compared. Coefficients for multiple linear regression models were used to examine the differences in blood vitamin concentrations between the UC cohorts and control groups (
The basic characteristics of members of the UC and control groups are tabulated in
The macronutrient and vitamin intakes for all participants are listed in
The urinary vitamin excretion values of the patients with UC and controls are listed in
The blood vitamin concentrations of the patients with UC and the controls are listed in
The vitamin clearance rates of the UC and the control groups are listed in
The principal finding of the present study investigating the association between dietary intake and blood concentrations of water-soluble vitamins in patients with UC was that concentrations of vitamin B2, vitamin C, niacin and folate were markedly lower in patients with UC than in healthy control subjects, independent of age, BMI, dietary intake, eGFR and other confounding factors; and that for renal clearance, only niacin was notably higher in patients with UC.
Individuals suffering from UC are usually advised to follow a diet rich in energy and protein, but restricted in fat which can stimulate the mucous membrane of the large intestine and cause diarrhea (
Vitamin deficiencies, if they occur in IBD, may not be attributed to a single cause (
Vitamin B2 (riboflavin) is an architectural component of flavin mononucleotide and flavin adenine dinucleotide, which serve as prosthetic groups in flavoproteins. For example, a flavoprotein, succinate dehydrogenase catalyzing the oxidation reaction of succinic acid to fumaric acid is a key enzyme in tricarboxylic acid cycle for energy production (
As vitamin B12 is important for the normal formation of red blood cells, its serum level was examined in relation to anemia among patients with IBD in Brazil (
In the present study, the blood concentration of vitamin C was markedly lower in the patients with UC than in the control subjects. Fernandez-Banares
Despite a sufficient dietary intake of niacin, its concentration was lower in the UC group than in the control group. By contrast, niacin renal clearance was markedly higher in the UC group than in the control group. The lower concentration of niacin was likely due to a high urinary clearance of niacin. In addition, the increased catabolic metabolism in UC may contribute to the lower level of niacin. Niacin is an architectural component of pyridine nucleotide coenzymes, including nicotinamide adenine dinucleotide and nicotinamide adenine dinucleotide phosphate. The reduced forms of the pyridine nucleotide coenzymes also have anti-inflammatory activity (
The lower concentrations of folate in patients with UC in the present study may be associated with medications taken by the patients. Interactions with SASP and 5-ASA, therapeutic agents for UC, are known to cause vitamin deficiency, particularly for folate. Hoshino
The key strengths of the present study were as follows: i) the comprehensive measurement of blood, urine, and dietary intakes of water-soluble vitamins of subjects; and ii) the standardized collection of samples that were immediately analyzed with high-quality laboratory measurements. The cross-sectional design of the study was identified as a weakness, and results require interpretation with caution when considering cause-effect relationships. As the age ranges differed widely between the patients suffering from UC and healthy subjects, statistical analyses may have been affected. However, as R2, the goodness-of-fit measure for all of the blood vitamin concentrations augmented considerably from Model 0 to Model 2, the appropriateness of the statistical method appears to have be confirmed. Data on urinary creatinine of NaCl was not collected from the patients with UC, nor was blood creatinine in the control subjects. The eGFR was used for the UC cohort and a rate of 100 ml/min was used for the control subjects. The total number of subjects, including patients (n=23) and controls (n=20), may be considered small. However, by remaining vigilant regarding the behavior of R2 in the analyses, and by checking R2 behavior against comparable studies in the field, the number of subjects is considered to be adequate.
In conclusion, the blood concentrations of vitamin B2, vitamin C, niacin and folate were significantly lower in patients with UC than in healthy subjects, independent of age and other confounding factors. Reductions in the blood concentrations of these vitamins in patients with UC may be of clinical significance, including in the forecasting, diagnosing and treatment of anemia in patients suffering from UC. Therefore, modifying the management of patients with UC, including adjustments in diet and/or vitamin supplementation, may be warranted when similar laboratory results are present.
Not applicable.
This study was supported by The University of Shiga Prefecture Grant for Special Research (grant no. 78).
The datasets used in the present study are available from the corresponding author on reasonable request.
HI, ToF and KS conceived and designed the experiments; HI, TsF and KS analyzed the data; HI and YD wrote the first draft of the manuscript; TsF, KS and MS contributed to the writing of the manuscript; HI, ToF, TsF, SB, MS, TT, YD, and KS agreed with manuscript results and conclusions. All the authors reviewed and approved the final manuscript.
All procedures performed in the study involving human participants were in accordance with the 1964 Helsinki Declaration and its later amendments or comparable ethical standards. The protocol for this study was approved by the Institutional Review Board of the Shiga University of Medical Science (no. 22-41, 2010). Written informed consent was obtained from the individual participants included in the study.
Not applicable.
The authors declare that they have no competing interests.
Background characteristics of participants.
| Characteristics | Control participants (n=20) | Patients with UC in remission (n=17) | Patients with active UC (n=6) | P-value |
|---|---|---|---|---|
| Age (years) | 20.7±0.9 | 41.8±14.9 |
44.7±15.7 |
<0.001 |
| Women (%) | 50 | 53 | 66 | 0.581 |
| BMI (kg/m2) | 21.4±1.7 | 21.9±3.6 | 22.4±4.2 |
0.020 |
| Hb (g/dl) | 14.1±1.5 | 11.2±3.7 | 0.124 | |
| Ht (%) | 41.5±3.7 | 39.5±5.0 | 0.285 | |
| WBC (x103/mm3) | 5.8±1.8 | 7.8±3.0 | 0.046 | |
| Alb (g/dl) | 4.2±0.4 | 3.8±0.7 | 0.077 | |
| TP (g/dl) | 7.0±0.5 | 7.1±0.6 | 0.841 | |
| T-Chol (mg/dl) | 195±25 | 188±49 | 0.639 | |
| CRP (mg/dl) | 0.1±0.2 | 1.8±4.2 | 0.063 | |
| CRE (mg/dl) | 0.8±0.2 | 0.9±0.4 | 0.300 | |
| eGFR (ml/min) | 78.1±15.4 | 73.6±22.4 | 0.578 |
Values are presented as the mean ± standard deviation or % (for women). The χ2 test was used to compare dichotomous variables (% women) among controls, patients with UC in remission phase, and patients with UC in active phase. Student's t-test was used to ascertain whether the means of two groups were statistically different from each other. Analysis of variance was used to compare the means of the three cohorts, followed a post-hoc Tukey HSD test when the F-value was significant at P<0.05. aP<0.05
bP<0.01 compared with the control by Tukey's post hoc analysis. UC, ulcerative colitis; BMI, body mass index; Hb, hemoglobin; Ht, hematocrit; WBC, white blood cell count; Alb, albumin; TP, total protein; T-chol, total cholesterol; CRP, C-reactive protein; CRE, creatinine; eGFR, estimated glomerular filtration rate.
Macronutrient and vitamin intakes of patients with UC and control participants.
| Variables | Control participants | Patients with UC in remission | Patients with UC in active phase | P-value | Vitamin RDA |
|---|---|---|---|---|---|
| Total energy (kcal/day) | 2,050±256 | 2,119±473 | 1,968±578 | 0.768 | - |
| Protein (% kcal/day) | 12.3±0.1 | 15.0±2.1 |
15.2±1.7 |
<0.001 | - |
| Fat (% kcal/day) | 19.8±0.2 | 26.2±6.0 |
21.3±7.0 | 0.001 | - |
| Carbohydrate (% kcal/day) | 66.1±1.2 | 56.5±7.9 |
61.3±6.0 | <0.001 | - |
| Vitamin B1 (mg/1,000 kcal/day) | 0.54±0.02 | 0.51±0.11 | 0.42±0.08 |
0.011 | 0.54 |
| Vitamin B2 (mg/1,000 kcal/day) | 0.85±0.01 | 0.65±0.10 |
0.53±0.19 |
<0.001 | 0.60 |
| Vitamin B6 (mg/g protein/day) | 0.031±0.003 | 0.022±0.043 |
0.019±0.035 |
<0.001 | 0.023 |
| Vitamin B12 (µg/1,000 kcal/day) | 2.4±0.6 | 4.1±1.6 | 6.7±6.2 |
0.002 | 1.2 |
| Vitamin C (mg/1,000 kcal/day) | 49.5±6.2 | 67.5±34.5 | 43.2±27.6 | 0.061 | 48.8 |
| Niacin (mgNE/1,000 kcal/day) | 5.6±0.1 | 10.5±3.4 |
10.7±3.5 |
<0.001 | 5.8 |
| Folate (µg/1,000 kcal/day) | 99.0±12.4 | 268.8±169.4 |
172.1±61.2 | <0.001 | 117 |
| NaCl (g/day) | 3.1±1.0 | 9.3±2.2 |
10.2±1.2 |
<0.001 | - |
Values are presented as the mean ± standard deviation, P-values and vitamin RDA. Vitamin RDA values for Japanese adults were obtained from (
bP<0.05 between participants with UC in remission and patients with active UC, compared by Tukey's post-hoc analysis. UC, ulcerative colitis; RDA, recommended dietary allowance; NE, niacin equivalent.
Urinary vitamin excretion in patients with UC and controls.
| Variables | Control participants | Patients with UC in remission | Patients with UC in active phase | P-value |
|---|---|---|---|---|
| Vitamin B1 (nmol/day) | 483.5±176.0 | 3,209±1,065 |
2,994±2,430 |
0.002 |
| Vitamin B2 (nmol/day) | 571±257 | 606±112 | 154±178 | 0.474 |
| 4-PIC |
3.0±0.6 | 4.2±3.0 | 3.2 | 0.175 |
| Vitamin B12 (pmol/day) | 119.0±47.8 | 42.9±19.2 |
27.3±14.1 |
<0.001 |
| Vitamin C (µmol/day) | 144.1±49.6 | 204.2±300.7 | 87.2±72.8 | 0.443 |
| Sum of niacin catabolites |
28.7±9.4 | 31.5±21.6 | 31.0±15.5 | 0.872 |
| Folate (nmol/day) | 21.1±3.1 | 21.2±30.8 | 19.7±17.7 | 0.988 |
Urinary vitamin excretion concentrations are presented as the mean ± standard deviation. Analysis of variance was used to compare the means of the three cohorts, followed by a post hoc application of the Tukey test when the F-value was significant at P<0.05. B1 to C denotes vitamin B1 to vitamin C. aCatabolite of vitamin B6.
bSum of
cP<0.05,
dP<0.01 compared with the control by Tukey's post-hoc analysis. UC, ulcerative colitis.
Blood vitamin concentrations in patients with UC and controls.
| Variables | Mean ± SD | Range | Difference | P-value | R2-value |
|---|---|---|---|---|---|
| Vitamin B1 (pmol/ml) | |||||
| UC | 87.2±21.7 | 42.6-136.6 | |||
| Control | 86.1±18.7 | 33.8-109.1 | |||
| Model 0 | 1.06 | <0.001 | 0.001 | ||
| Model 1 | 6.55 | <0.001 | 0.016 | ||
| Model 2 | 23.9 | 0.210 | 0.214 | ||
| Vitamin B2 (pmol/ml) | |||||
| UC | 141.1±24.7 | 86.1-186.5 | |||
| Control | 214.7±22.8 | 175-258 | |||
| Model 0 | -73.5 | <0.001 | 0.713 | ||
| Model 1 | -77.7 | <0.001 | 0.715 | ||
| Model 2 | -86.3 | 0.025 | 0.830 | ||
| Pyridoxal phosphate (vitamin B6 coenzyme; pmol/ml) | |||||
| UC | 63.0 ± 65.0 | 14.0-344.1 | |||
| Control | 78.7±15.2 | 52.7-113.3 | |||
| Model 0 | -15.7 | <0.001 | 0.026 | ||
| Model 1 | 6.0 | <0.001 | 0.066 | ||
| Model 2 | 9.8 | 0.59 | 0.242 | ||
| Vitamin B12 (pmol/ml)a | |||||
| UC | 1.12 (0.94,1.60) | 0.74-4.65 | |||
| Control | 0.42 (0.34, 0.70) | 0.26-0.92 | |||
| logB12 | |||||
| UC | 0.09±0.19 | -0.13-0.67 | |||
| Control | -0.33±0.18 | -0.59-(-0.04) | |||
| Model 0 | 0.43 | <0.001 | 0.586 | ||
| Model 1 | 0.38 | <0.001 | 0.590 | ||
| Model 2 | 0.20 | 0.244 | 0.829 | ||
| Vitamin C (nmol/ml) | |||||
| UC | 39.9±18.1 | 12.3-103.7 | |||
| Control | 64.5±12.5 | 47-100 | |||
| Model 0 | -24.5 | <0.001 | 0.387 | ||
| Model 1 | -25.3 | <0.001 | 0.388 | ||
| Model 2 | -42.2 | 0.002 | 0.554 | ||
| Niacin (nmol/ml) | |||||
| UC | 48.5±27.0 | 23.4-120.4 | |||
| Control | 60.5±5.6 | 52.8-75.4 | |||
| Model 0 | -12.0 | <0.001 | 0.086 | ||
| Model 1 | -19.1 | <0.001 | 0.111 | ||
| Model 2 | -42.8 | 0.003 | 0.270 | ||
| Folate (pmol/ml) | |||||
| UC | 9.8±7.3 | 1.2-34.7 | |||
| Control | 23.5±9.6 | 10.7-51.6 | |||
| Model 0 | -14.0 | <0.001 | 0.425 | ||
| Model 1 | -17.8 | <0.001 | 0.453 | ||
| Model 2 | -27.1 | 0.015 | 0.629 | ||
Coefficients for multiple linear regression models were used to examine differences in blood vitamin concentrations between the UC and control groups. As the distribution of blood vitamin B12 concentration was positively skewed, a logarithmic transformation was used to normalize the distribution. Model 0: Crude difference in patients and controls (patient-control). P-values by linear regression analyses. Model 1: Age-adjusted difference. Model 2: Model 1 variables + sex, body mass index, estimated glomerular filtration rate, urinary excretion, and dietary intake of each vitamin. R2 is a goodness-of-fit measure. aVitamin B12 concentrations are shown as median (25th, 75th percentile). UC, ulcerative colitis; SD, standard deviation.
Vitamin clearance rates (ml/min) in the UC and control groups.
| Variable | Control participants | Patients with UC in remission | Patients with UC in active phase | P-value |
|---|---|---|---|---|
| Vitamin B1 | 4.04±1.55 | 23.7±23.67 |
32.4±30.88 |
0.003 |
| Vitamin B2 | 1.87±0.86 | 2.55±4.38 | 0.734±0.713 | 0.431 |
| Vitamin B6 | 27.5±7.0 | 60.77±47.58 |
52.19±29.3 | 0.010 |
| Vitamin B12 | 0.179±0.065 | 0.263±0.123 |
0.152±0.11 |
<0.001 |
| Niacin | 0.33±0.11 | 0.45±0.31 | 0.60±0.40 | 0.080 |
| Folate | 0.70±0.23 | 1.90±2.09 |
1.45±0.90 | 0.032 |
| Vitamin C | 1.60±0.59 | 3.11±4.10 | 1.90±1.87 | 0.243 |
Vitamin clearance rates (ml/min) are presented as the mean ± standard deviation. Analysis of variance was used to compare the means of the three groups, followed by a followed by a post-hoc Tukey HSD test when the F-value was significant at P<0.05. aP<0.05
bP<0.01 compared with the control by Tukey's post-hoc analysis. UC, UC, ulcerative colitis.