Hostname: page-component-8448b6f56d-c4f8m Total loading time: 0 Render date: 2024-04-16T20:48:12.659Z Has data issue: false hasContentIssue false
  • English
  • Français

Evaluation of iodine nutritional status during pregnancy by estimated 24-h urinary iodine excretion: population variation range and individual accuracy

Published online by Cambridge University Press:  12 August 2021

Ye Bu ,
Yan Cai ,
Chunlei Ji Open the ORCID record for Chunlei Ji [Opens in a new window] ,
Chunyan Zhao ,
Chunyuan Tian ,
Bo Pang ,
Mengqi Shi ,
Xin Li ,
Ying Liu  and
Dianjun Sun Open the ORCID record for Dianjun Sun [Opens in a new window]
Ye Bu
Affiliation:
Key Laboratory of Etiology and Epidemiology, National Health and Family Planning Commission, Center for Endemic Disease Control, Chinese Center for Disease Control and Prevention, Harbin Medical University, No.196, Baojian road, Harbin, Heilongjiang 150086, People’s Republic of China The Fourth Affiliated Hospital of Harbin Medical University, Department of Obstetrics and Gynecology, Harbin, Heilongjiang, People’s Republic of China
Yan Cai
Affiliation:
The Fourth Affiliated Hospital of Harbin Medical University, Department of Obstetrics and Gynecology, Harbin, Heilongjiang, People’s Republic of China
Chunlei Ji
Affiliation:
The Fourth Affiliated Hospital of Harbin Medical University, Department of Obstetrics and Gynecology, Harbin, Heilongjiang, People’s Republic of China
Chunyan Zhao
Affiliation:
The Fourth Affiliated Hospital of Harbin Medical University, Department of Obstetrics and Gynecology, Harbin, Heilongjiang, People’s Republic of China
Chunyuan Tian
Affiliation:
Key Laboratory of Etiology and Epidemiology, National Health and Family Planning Commission, Center for Endemic Disease Control, Chinese Center for Disease Control and Prevention, Harbin Medical University, No.196, Baojian road, Harbin, Heilongjiang 150086, People’s Republic of China
Bo Pang
Affiliation:
The Fourth Affiliated Hospital of Harbin Medical University, Department of Obstetrics and Gynecology, Harbin, Heilongjiang, People’s Republic of China
Mengqi Shi
Affiliation:
Nantong Center for Disease Control and Prevention, Nantong, Jiangsu Province, People’s Republic of China
Xin Li
Affiliation:
Key Laboratory of Etiology and Epidemiology, National Health and Family Planning Commission, Center for Endemic Disease Control, Chinese Center for Disease Control and Prevention, Harbin Medical University, No.196, Baojian road, Harbin, Heilongjiang 150086, People’s Republic of China
Ying Liu*
Affiliation:
Key Laboratory of Etiology and Epidemiology, National Health and Family Planning Commission, Center for Endemic Disease Control, Chinese Center for Disease Control and Prevention, Harbin Medical University, No.196, Baojian road, Harbin, Heilongjiang 150086, People’s Republic of China
Dianjun Sun*
Affiliation:
Key Laboratory of Etiology and Epidemiology, National Health and Family Planning Commission, Center for Endemic Disease Control, Chinese Center for Disease Control and Prevention, Harbin Medical University, No.196, Baojian road, Harbin, Heilongjiang 150086, People’s Republic of China
*
*Corresponding authors: Email hrbmusdj@163.com; liuying@hrbmu.edu.cn
*Corresponding authors: Email hrbmusdj@163.com; liuying@hrbmu.edu.cn
Rights & Permissions [Opens in a new window]

Abstract

Objective:

To explore the accuracy of estimated 24-h urinary iodine excretion (24-h UIEest) in assessing iodine nutritional status.

Design:

Fasting venous blood, 24-h and spot urine samples were collected during the day. The urinary iodine concentration (UIC) and urinary creatinine concentration (UCrC) were measured, and the urinary iodine-to-creatinine ratio (UI/Cr), 24-h UIEest, and 24-h urinary iodine excretion (24-h UIE) were calculated. At the population level, correlation and consistency between UIC, UI/Cr, 24-h UIEest and 24-h UIE were assessed using correlation analysis and Bland–Altman plots. At the individual level, receiver operating characteristic (ROC) curves were used to analyse the accuracy of the above indicators for evaluating insufficient and excessive iodine intake. The reference interval of 24-h UIEest was established based on percentile values.

Setting:

Indicator can accurately evaluate individual iodine nutrition during pregnancy remains controversial.

Participants:

Pregnant women (n 788).

Results:

Using 24-h UIE as standard, the correlation coefficients of 24-h UIEest from different periods of the day ranged from 0·409 to 0·531, and the relative average differences ranged from 4·4 % to 10·9 %. For diagnosis of insufficient iodine intake, the area under the ROC curve of 24-h UIEest was 0·754, sensitivity and specificity were 79·6 % and 65·4 %, respectively. For diagnosis of excessive iodine intake, the area of 24-h UIEest was 0·771, sensitivity and specificity were 66·7 % and 82·0 %, respectively. The reference interval of 24-h UIEest was 58·43–597·65 μg.

Conclusions:

Twenty-four-hour UIEest can better indicate iodine nutritional status at a relatively large sample size in a given population of pregnant women. It can be used for early screening at the individual level to obtain more lead time for pregnant women.

Keywords

Pregnant womenIodine nutritionIndividual assessmentUrinary iodine excretionEstimated iodine excretionUrinary creatinineEpidemiology study
Type
Research paper
Information
Public Health Nutrition , Volume 25 , Issue 2 , February 2022 , pp. 237 - 247
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
Copyright
© The Author(s), 2021. Published by Cambridge University Press on behalf of The Nutrition Society

Iodine is an indispensable trace element, and the physiological demand for iodine increases during pregnancy(Reference Glinoer1). Iodine deficiency or excess has irreversible effects on fetal thyroid function, the nervous system, brain development, and the shape and function of the thyroid in pregnant women(Reference Pearce, Lazarus and Moreno-Reyes2,Reference Glinoer3) . As a result, an increasing number of pregnant women have a clear clinical need for diagnostic tests to assess iodine status.

The urinary iodine concentration (UIC) has been widely used to evaluate the iodine nutritional status in pregnant women in populations. The WHO/UNICEF/ICCIDD recommended that the median UIC can be used to assess the iodine status of populations(4). The Chinese guidelines on the diagnosis and management of thyroid disease during pregnancy and postpartum (2019)(5) recommended that the urinary iodine-to-creatinine ratio (UI/Cr) can be used to evaluate populations’ iodine nutritional status during pregnancy. Therefore, it is still an urgent need for establishing an index that can accurately evaluate individual iodine nutrition and establishing a range of reference values.

Under the current research conditions, 24-h urinary iodine excretion (24-h UIE) is recognised as the gold standard to evaluate individuals’ recent iodine nutrition status. However, 24-h urine is difficult to collect and achieve clinical implementation and promotion, so it is necessary to find a substitute indicator to accurately estimate 24-h UIE in the field of individual iodine nutrition evaluation. In recent years, some scholars have used 24-h creatinine scaling to estimate 24-h iodine excretion in adults(Reference Ma, Venn and Manning6,Reference Knudsen, Christiansen and Brandt-Christensen7) and children(Reference Chen, Li and Guo8,Reference Gabriela, Simone and Peter9) . However, it is currently uncertain whether this methodological approach also provides a more accurate assessment of iodine status in pregnant women. Therefore, the purpose of this methodological study was to determine the accuracy and variation range of estimated 24-h UIE (24-h UIEest) in evaluating iodine nutritional status during pregnancy at both the individual and population levels.

Materials and methods

Study participants

From June 2018 to October 2020, pregnant women were screened in hospitals in Harbin, Heilongjiang Province, an iodine adequate area in China. The exclusion criteria were (1) clinical/subclinical thyroid dysfunction; (2) family history of thyroid disease; (3) having taken iodine-containing drugs or supplements; (4) received treatment for thyroid disease; (5) visible or palpable goitre; (6) having consumed iodine-rich foods for 4 d before providing the urine sample; (7) multiple pregnancies; (8) Fe deficiency anaemia and (9) hyperemesis gravidarum.

Basic information collection

All participants completed questionnaires, which collected basic characteristic information, gestational history, history of taking nutritional drugs during pregnancy and disease history. In addition, we determined weight and body composition for all participants by direct segment multifrequency bioelectrical impedance analysis (DSM-BIA) with the Inbody 770 human component analyser.

Collection and detection of urine and blood samples

Professionals gave participants detailed instructions on the correct method of collecting 24-h and spot urine samples: at 6:00 am on the first day, and participants were instructed to empty their urine. Then, in the following 24 h, urine was collected each time until 6:00 am the next day (urine at 6:00 am the next day was included). Complete urine samples were collected and placed in 3000-ml clean polyethylene barrels provided by unification. Then, participants used cylinders to measure their 24-h urine volume. After the urine was thoroughly mixed, participants used cryogenic tubes to place a 5-ml 24-h urine sample(Reference Ye, Lin and Chunyuan10). For 24-h urine that did not meet the above requirements, new retention was required. Pregnant women who collected 24-h urine samples were also required to collect spot urine (fasting, 8:00–9:00, 11:00–12:00 and 16:00–17:00 in 24 h) at least twice a day. We used 1·8-ml cryogenic test tubes to place spot urine samples and directly transported the urine samples to the laboratory for analysis.

UIC was determined by arsenic and cerium catalytic spectrophotometry (WS/T107-2006), and urinary creatinine concentration (UCrC) was determined by spectrophotometry (JAFF method) (WS/T97–1996). External reference samples were provided by the National Laboratory for Prevention and Treatment of Iodine-Deficient Disorders in China. We used the certified reference material (GBW9110t, GBW9109l and GBW09108p) of the Center for Disease Control (CDC) of China as the control measurements. The standard values of the UIC reference materials were 239 ± 15 μg/l, 134 ± 10 μg/l and 69·5 ± 9·0 μg/l(Reference Ye, Lin and Chunyuan10), the interassay CV were 2·5 %, 2·2 %, and 1·7 %, and the intraassay CV were 3·1 %, 3·7 %, and 2·9 %, respectively. The target values of the urinary creatinine reference materials were 1·135 ± 0·11 g/l, the interassay CV was 3·2 % and the intraassay CV is 4·1 %.

Venous blood was collected from all pregnant women in the morning (8:00–11:00). After separating the serum, the levels of thyroid hormone (IT3000, Roche), ferritin (i2000SR, Abbott), and Hb (XN1000, Sysmex Corporation) were measured. A chemiluminescent immunoassay was used to determine the levels of thyroid hormones, including free triiodothyronine (FT3), free thyroxine (FT4), thyroid-stimulating hormone, thyroglobulin antibody and thyroid peroxidase antibody. Maternal serum ferritin levels were measured using an electrochemiluminescence immunoassay. Hb was measured using the electric resistance method.

Urine samples were preserved at 4°C, while serum samples were frozen at −20°C until analysis. All urine iodine and creatinine indicators were tested within 1 week and strictly controlled in the National Key Laboratory of Etiology and Epidemiology.

The equation of predicted 24-h urinary creatinine excretion

Twenty-four-hour UCrE is the 24-h urinary creatinine concentration (24-h UCrC) multiplied by 24-h urine volume. Twenty-four-hour UIEest is calculated by the UI/Cr multiplied by predicted 24-h UCrE. Some scholars have used UI/Cr multiplied by predicted 24-h UCrE(Reference Kesteloot and Joossens11,Reference Mage, Allen and Kodali12) to evaluate individual iodine nutritional status in healthy adults(Reference Perrine, Cogswell and Swanson13). However, the equation of predicted 24-h UCrE based on age, weight, height and other factors of pregnant women has not been officially established. Therefore, the predicted 24-h UCrE we used was the result of a preliminary study by our research group(Reference Ye, Lin and Chunyuan10). We used the multiple linear regression method to predict 24-h UCrE based on pregnancy weight, gestational weeks, age, pre-pregnancy BMI and body fat percentage from 743 healthy pregnant women and predicted the finally constructed multiple linear regression model 24-h UCrE = 0·423 + 0·016 × pregnancy weight(kg) (F = 45·029, P < 0·001; r 2 = 0·138).

Diagnostic criteria

Using the recommended nutrient intake and tolerable upper intake levels as the standard to reversely deduce the iodine intake from the iodine excreted in the urine, Bath SC(Reference Bath, Furmidge-Owen and Redman14) suggested that the median estimated 24-h UIE be >225 μg/d assuming the recommended 250 μg/d iodine intake(4,15) of which 90 % is excreted(Reference Vought and London16). In China, the recommended nutrient intake for iodine during pregnancy is 230 μg/d(17). Therefore, in this study, 24-h UIE < 207 μg/d was defined as ‘insufficient iodine intake’. Given that the upper intake levels of iodine during pregnancy is 600 μg/d(17), 24-h UIE > 540 μg/d is defined as ‘excessive iodine intake’.

The reference ranges of thyroid-stimulating hormone from different trimesters were 0·09–4·52 mU/l, 0·45–4·32 mU/l and 0·30–4·98 mU/l. The reference ranges for FT4 were 13·15–20·78 pmol/l, 9·77–18·89 pmol/l and 9·04–15·22 pmol/l, respectively. The above reference ranges were recommended by the guidelines for diagnosis and treatment of thyroid disorders in pregnancy and postpartum (2019)(5). The reference ranges of FT3, thyroglobulin antibody and thyroid peroxidase antibody (IT3000, Roche) were 3·1–6·8 pmol/l, 0-115 U/ml and 0–34 U/ml throughout pregnancy, respectively.

According to the recommendation of the 2014 guidelines for the diagnosis and treatment of Fe deficiency and Fe deficiency anaemia during pregnancy(18) in China, the diagnostic criteria for Fe deficiency anaemia are serum ferritin level < 20 g/l and Hb level < 110 g/l.

Statistical analysis

We used SPSS 25. 0 (IBM) for data processing and analysis and GraphPad 8.0 software to generate statistical charts. Normally distributed data are presented as the means and standard deviation, and one-way ANOVA was used to compare means between groups. The non-normally distributed data are represented using the median with the interquartile range. The Mann–Whitney U rank-sum test was used for the intergroup comparison of urinary iodine indicators, and the Spearman rank correlation test was used for correlation analysis. A receiver operating characteristic (ROC) curve was established, and the area comparison test evaluation index under the ROC curve was applied. The significance levels quoted are two-sided and P < 0·05 was used to show statistically significant differences.

Results

General characteristics of pregnant women

A total of 788 pregnant women (including 208 in the first trimester, 410 in the second trimester and 170 in the third trimester) were included in this study (see online Supplemental material Fig. 1).

The baseline characteristics of pregnant women in the different trimesters are shown in Table 1. Age, current weight (when collecting 24-h urine samples), body fat percentage, fat loss weight and muscle content varied by trimester (P < 0·001).

Table 1 General characteristics of pregnant women

Pre-pregnancy BMI was calculated by dividing pre-pregnancy weight by height squared.

First trimester: 0–13 weeks, second trimester: 14–27 weeks and third trimester: 28–40 weeks.

The value was presented as the means and standard deviation.

One-way ANOVA was used for the intergroup comparison, and P < 0 05 was considered statistically significant.

Twenty-four-hour urinary iodine parameters, spot urinary iodine concentration and urinary iodine-to-creatinine ratio measurements

The median 24-h UIE was 205·99 μg; 188·42 μg in the first trimester, 204·85 μg in the second trimester and 232·99 μg in the third trimester, with significant differences between the trimesters (P < 0·01). The median 24-h UIEest was 192·52 μg; 171·89 μg in the first trimester, 198·60 μg in the second trimester and 204·16 μg in the third trimester. The 24-h UIEest in the first trimester was significantly different from that in the second and third trimesters (both P < 0·01), while the difference between the second and third trimesters was not significant (P > 0·05).

Spot UIC within a day had median values of 151·89 μg/l (fasting), 136·67 μg/l (8:00–9:00), 125·81 μg/l (11:00–12:00) and 130·17 μg/l (16:00–17:00). The UIC at fasting was significantly different from the UIC at the other three time points (P < 0·01). Spot UI/Cr had median values of 122·86 μg/g, 128·20 μg/g, 129·37 μg/g and 139·69 μg/g, for the same four time periods. However, after adjusting for spot UCrC, the spot UI/Cr at different time points detected no significant differences (P = 0·99).

Increasing trends were found in 24-h UIEest and UI/Cr at fasting from the first to the third trimester, consistent with the changes in 24-h UIE values (P < 0·001). However, the median 24-h UIC between different trimesters showed no significant differences (P > 0·05). (see online Supplemental Material Table 1)

Correlation analysis of spot urinary iodine concentration, urinary iodine-to-creatinine ratio and estimated 24-h urinary iodine excretion with 24-h urinary iodine excretion

Compared with 24-h UIE measurements, the correlation coefficients for spot UIC ranged from 0·324 to 0·481 (P < 0·01), those for UI/Cr were 0·303–0·454 (P < 0·01), and those for 24-h UIEest were 0·409–0·531 (P < 0·01). The correlation coefficients of urinary indicators at fasting were higher than those at other time points of the day. Moreover, the correlation coefficients for 24-h UIEest at different time points within a day were higher than the other two indexes for the corresponding time points (Fig. 1).

Fig. 1 Correlation between spot UIC, UI/Cr, 24-h UIEest and 24-h UIE. UIC urinary iodine concentration, UI/Cr, urinary iodine-to-creatinine ratio; 24-h UIEest; estimated 24-h urinary iodine excretion; 24-h UIE, 24-h urinary iodine excretion. a, b and c represent the consistency of spot UIC, UI/Cr and 24-h UIEest compared with 24-h UIE, respectively. The urinary indicators at four time periods (at fasting, 8:00–9:00, 11:00–12:00 and 16:00–17:00) are expressed by tail 1, tail 2, tail 3 and tail 4

Consistency of urinary iodine concentration, urinary iodine-to-creatinine ratio and estimated 24-h urinary iodine excretion with 24-h urinary iodine excretion at each time point

Using 24-h UIE as the gold standard, we found that the relative average differences in 24-h UIEest between different periods during pregnancy clearly distinguished UIC and UI/Cr for the same periods. The relative average difference in 24-h UIEest ranged from 4·4 % to 10·9 % for the different time periods, while that for UIC and UI/Cr ranged from 34·1 % to 44·3 % and 25·3 % to 49·6 %, respectively (Fig. 2).

Fig. 2 Consistency of spot UIC, UI/Cr and 24-h UIEest compared with 24-h UIE at different urine collection times. UIC, urinary iodine concentration; UI/Cr, urinary iodine-to-creatinine ratio; 24-h UIEest, estimated 24-h urinary iodine excretion; 24-h UIE, 24-h urinary iodine excretion; n, number of participants. The Bland–Altman plot shows the consistency of spot UIC (a), UI/Cr (b) and 24-h UIEest (c) compared with 24-h UIE. The urinary indicators at four time periods (at fasting, 8:00–9:00, 11:00–12:00 and 16:00–17:00) are expressed by tail 1, tail 2, tail 3 and tail 4. The solid line represents the relative average difference, and the dotted line represents the 95 % reference interval for the relative average difference. On the X-axis, ‘Mean’ means the average of spot UIC, UI/Cr or 24-h UIEest with 24-h UIE

ROC curve

ROC curves of UIC, UI/Cr and 24-h UIEest at different times were established using these indicators as the gold standard (Fig. 3). Either UIC, UI/Cr or 24-h UIEest, when diagnosed with insufficient iodine intake or excessive iodine intake, had the AUC as the highest at fasting compared with the other three time points. For the diagnosis of insufficient or excessive iodine intake, the AUC of 24-h UIEest showed no difference from UIC at fasting; however, there were differences with UI/Cr at fasting with P-values of 0·007 and 0·033, respectively. In general, regardless of which urinary indicator was used for the diagnosis of insufficient iodine intake, the sensitivity ranged from 54·5 % to 79·6 %, and the specificity ranged from 42·6 % to 80·0 %. For the diagnosis of excessive iodine intake, the sensitivity ranged from 50 % to 87·5 %, and the specificity ranged from 54·5 % to 84·9 % (Table 2).

Fig. 3 ROC curves and tangent point values for UIC, UI/Cr and 24-h UIEest from different urine collection times. UIC, urinary iodine concentration; UI/Cr, urinary iodine-to-creatinine ratio; 24-h UIEest, estimated 24-h urinary iodine excretion; 24-h UIE, 24-h urinary iodine excretion; n, number of participants. a and b represent the ROC curves of UIC, UI/Cr and 24-h UIEest for diagnosing insufficient iodine intake and excessive iodine intake, respectively. The urinary indicators at four time periods (at fasting, 8:00–9:00, 11:00–12:00 and 16:00–17:00) are expressed by tail 1, tail 2, tail 3 and tail 4

Table 2 Receiver operating characteristic (ROC) curves of insufficient and excessive iodine intake

UIC, urinary iodine concentration; UI/Cr, urinary iodine-to-creatinine ratio; 24-h UIEest, estimated 24-hour urinary iodine excretion.

* Compared with UIC at the same time periods, P < 0 05.

Compared with UI/Cr at the same time periods, P < 0 05.

Reference values of 24-h urinary iodine excretion, estimated 24-h urinary iodine excretion (based on fasting urinary iodine-to-creatinine ratio), urinary iodine concentration and urinary iodine-to-creatinine ratio at fasting

We established the reference intervals of urinary iodine indicators for healthy pregnant women based on percentile values (Table 3). The reference interval of 24-h UIE was 78·95–553·29 µg. The reference intervals of 24-h UIEest, UIC and UI/Cr at fasting were 58·43–597·65 μg, 42·93–451·33 μg/l and 37·54–509·28 μg/g), respectively.

Table 3 Reference values of 24-h UIE, 24-h UIEest (based on fasting UI/Cr), UIC and UI/Cr at fasting during the entire pregnancy and for each trimester

24-h UIE, 24-hour urinary iodine excretion; 24-h UIEest, estimated 24-hour urinary iodine excretion; UIC, urinary iodine concentration; UI/Cr, urinary iodine-to-creatinine ratio.

First trimester: 0–13 weeks, second trimester: 14–27 weeks and third trimester: 28–40 weeks.

Described as the median, 2 5th and 97 5th centiles (P2 5–P97 5).

Discussion

Iodine is an essential trace element for synthesising thyroid hormone, which is essential for human growth and metabolism. Both the WHO/UNICEF/ICCIDD and Chinese Medical Association (CMA) recommend that pregnant women increase their nutritional iodine intake per day(4,17) . At present, urinary iodine indicators are generally used to evaluate iodine nutrition at the population level. However, at the individual level, it is still necessary to find a more accurate biomarker and confirm its reference interval. Therefore, we conducted a systematic and comprehensive methodological study on urinary iodine indicators.

Our study demonstrated that spot UIC at fasting of 788 pregnant women varied by the other three time points of the day (P < 0·001). This may be due to the hydration status and circadian rhythmicity during pregnancy. However, after adjusting for spot UCrC, the differences in UI/Cr were not significant. This further proved that the influence of urine volume on UIC could be excluded after creatinine correction. In different trimesters, the variation trend of 24-h UIC was different from that of 24-h UIE, which was consistent with 24-h UIEest. Spot UIC at the same time points also showed no obvious change rule (P > 0·05). The variation in spot UIC at fasting was different from the result of Pan(Reference Pan, Cui and Chen19); however, the variation in UI/Cr was consistent with Pan. Theoretically, with the increase in gestational weeks, morning sickness gradually subsides, and the total dietary energy intake and renal clearance of iodine increase, all of which caused 24-h UIE to show a gradually increasing trend(Reference François20). Although it has previously been shown that UIC is unstable in children and adults(Reference Ji, Liu and Sun21,Reference Rasmussen, Ovesen and Christiansen22) , our study further proves that UIC during pregnancy is unstable at different time periods of the day and in different trimesters.

In recent years, in the study of urine indicators, many investigators have used creatinine to correct UIC in a one-time random urine sample(Reference McMullan, Hamill and Doolan23,Reference Mulder, Korevaar and Peeters24) . However, few studies have focused on urinary creatinine metabolism during pregnancy(Reference Zhao, Li and Xia25). Our previous research demonstrated that spot UCrC varied irregularly during different trimesters and at different time periods of the day(Reference Ye, Lin and Chunyuan10). Although creatinine is known to be excreted at a relatively constant rate in 24 h(Reference Soldin26), spot UCrC are still affected by urine volume and circadian rhythmicity(Reference Chen, Li and Guo8). Furthermore, weight growth is evident during pregnancy, including not only the pregnant woman’s own increase in blood volume, breast, fat, uterus and fluid, but also the fetus, placenta, amniotic fluid and other weight. In addition to pregnancy-specific physiological changes (such as an increased glomerular filtration rate)(Reference Glinoer27) and increased dietary protein intake(28), the urine creatinine output during pregnancy is inevitably different from that during non-pregnancy. Our preliminary study results confirmed that pregnancy weight was an influencing factor on 24-h UCrE after adjusting for gestational weeks, age, pre-pregnancy BMI and percentage of body fat(Reference Ye, Lin and Chunyuan10). Thus, we established a multiple regression equation for 24-h UCrE in healthy pregnant women and made a comprehensive comparison of the relationship between UIC, UI/Cr, estimated 24-h UIE (24-h UIEest) and 24-h UIE.

Judging from our data, the correlation analysis found that in different periods of pregnancy, the UIC, UI/Cr and 24-h UIEest all showed moderate correlations with the 24-h UIE (Fig. 1), which was consistent with previous studies of Perrine CG(Reference Perrine, Cogswell and Swanson13). The consistency analysis showed that the relative average difference of 24-h UIEest ranged from 4·4 % to 10·9 %, which was better than those of UIC and UI/Cr as well as consistent with previous studies of Liu XB(Reference Liu, Wu and Zhang29). Furthermore, the relative average difference of 24-h UIEest (based on UI/Cr at fasting) was the lowest. Therefore, UIC, UI/Cr or 24-h UIEest could theoretically evaluate the iodine nutritional status within a given population of pregnant women. However, 24-h UIEest (based on UI/Cr at fasting) is the best estimate of 24-h UIE compared to the other two indicators.

Based on the above results at the population level, we drew the ROC curves of UIC, UI/Cr and 24-h UIEest. To diagnose insufficient iodine intake and excessive iodine intake, the AUC of UIC, UI/Cr and 24-h UIEest at fasting were highest compared with the other three time periods within groups. The AUC of UI/Cr at fasting had significant differences with 24-h UIEest at fasting, indicating that 24-h UIEest may be better than UI/Cr for the diagnosis of insufficient or excessive iodine intake in diagnostic efficiency. Although there was no difference between the AUC of UIC and 24-h UIEest at fasting, the correlation coefficient for spot UIC at fasting was lower than 24-h UIEest at the same time period. Furthermore, the relative average difference in spot UIC at fasting was higher than 24-h UIEest, thereby indicating that the strength of 24-h UIEest as a marker of individual iodine nutritional status was better than spot UIC and UI/Cr(Reference Patrick and Paul30). However, the gold standard we chose was 24-h UIE, for which diagnostic criteria were defined according to the iodine recommended nutrient intake and upper intake levels. Choosing different indicators as the gold standard may lead to different results, so the results of ROC curves might not be consistent with Li(Reference Li, Peng and Zhang31).

Sensitivity and specificity reflected the screening efficiency of urinary indicators in evaluating iodine nutrition(Reference Eastman, Ma and Li32,Reference Laurberg, Andersen and Bjarnodottir33) . The author considers that the main factor affecting the consistency is the biological variation of the subject. Due to the significant variation of spot urinary indicators of the individual(Reference Als, Helbling and Peter34), the same subject’s clinical measurement value at different times fluctuates. Pregnancy is a unique physiological period, when as the uterus gradually increases in size, the bladder pressure and hormone levels also increase, leading to an increased frequency of urination. As a result, the volume of every spot of urine in a day varies, affecting the spot UIC(Reference Andersen, Sorensen and Krejbjerg35) (see online Supplemental material Table 1).

Compared with urinary indicators, blood indicators such as serum iodine, thyroglobulin or thyroid-stimulating hormone do not change immediately with changes in dietary iodine intake(Reference Yu, Yin and Cheng36Reference Guo, Wang and Jin39). Because there are generally 9 months for pregnant women from the discovery of pregnancy to full-term delivery, missing iodine-deficient pregnant women might miss the best period of iodine supplementation(Reference Gabriella, María and Francisco40), leading to adverse pregnancy outcomes and consequences. It can be hypothesised that to evaluate the short-term iodine intake of pregnant women, the blood indicators may lag behind urinary iodine indicators in time. Therefore, it is undeniable that the urine index is still of significance in evaluating individual iodine nutrition in pregnant women. Finally, we established the reference values of 24-h UIE, 24-h UIEest (based on UI/Cr and 24-h UCrEest), UIC and UI/Cr at fasting throughout pregnancy and each trimester. The trend of the 95 % reference interval of the urinary indicators for healthy pregnant women was consistent with Liu(Reference Liu, Wang and Zhao41) and Wang(Reference Wang, Liu and Liu42).

The author believes that future research should focus on the following aspects: first, to the best of our knowledge, very few extensive sample studies have focused on the metabolic rule of urinary creatinine. Reference values or multiple linear regression equations for 24-h UCrE in healthy pregnant women in different regions should be established. Second, it is necessary to research the relationship between the duration of iodine deficiency or excess state and the changes in haematological indicators related to iodine nutrition. Further research could be associated with serum iodine, thyroglobulin, thyroid-stimulating hormone of maternal or newborn, FT4, ferritin, or selenium for the combined screening test to improve sensitivity and specificity. Last, in the field of iodine nutrition during pregnancy, research mainly focuses on maternal iodine nutrition status and intellectual and nervous system development, IQ and executive function, attention-deficit hyperactivity disorder or autistic traits, and language skills of the offspring(Reference Bath, Steer and Golding43,Reference Deborah, Bath and Guxens44) . However, it is not scientific to use only the WHO-endorsed cut-off of less than 150 µg/l from spot UIC or UI/Cr to evaluate maternal iodine nutritional status and then compare it with the neural and intellectual development of offspring, as the criteria for individual iodine deficiency are still controversial(Reference Eastman, Ma and Li32). Supposing individual criteria can be found, a reference range is proposed. In that case, the reference range may provide better criteria for determining individual iodine deficiency and iodine excess in the above studies, thus further promoting research progress in the field of iodine nutrition in pregnancy.

In conclusion, 24-h UCrE has an essential application in the assessment of individual iodine nutrition. We can use 24-h UIEest for early screening to obtain more lead time for pregnant women.

Strengths and limitations

Strengths

(1) To the best of our knowledge, this was a large-scale population cross-sectional study on the iodine nutrition evaluation method for pregnant women based on 24-h urine and (2) there have been few reports on the 24-h creatinine metabolism of healthy pregnant women in recent decades, which limited the use of 24-h UIEest in a summary of iodine nutrition evaluation during pregnancy. Therefore, we established a multiple linear regression equation of 24-h UCrE according to our previous research data to obtain 24-h UIEest; and (3) we also measured four spot UIC during the day to verify that UIC changed significantly in 1 d.

Limitations

(1) The sample size of pregnant women in each trimester was not uniformly distributed; (2) this was not a longitudinal cohort study; (3) not every pregnant woman collected urine at four different time points of the day; (4) we did not conduct a dietary survey to calculate dietary iodine intake accurately; and (5) we did not include blood indicators for analysis, and our follow-up studies are ongoing.

Acknowledgements

Acknowledgements: The authors are extremely grateful to all the pregnant women who participated in this study. The authors are grateful to Professor Peng Liu for help with suggestions for writing and revising the article. Financial support: This work was supported by the National Natural Science Foundation of China (DJ.S., grant number 81830098); and the Natural Science Foundation of Heilongjiang Province (DJ.S., grant number TD2019H001); and Health and Family Planning Commission of Heilongjiang Province (Y.B., grant number 2020-080). Conflict of interest: There are no conflicts of interest. Authorship: D.S., Y.L. and Y.C. formulated the research question and designed the study; Y.B., M.S. and C.Z. carried out the study and contributed to recruit pregnant women and data collection; C.T. and B.P. analyzed data and performed statistical analysis; C.J. and X.L. interpreted the findings; Y.B. wrote the article. All authors have read and approved the final manuscript. Ethics of human subject participation: All participants were informed of the participation process and details. Informed consent to participate in the study was obtained from all the enrolled subjects. This study was conducted according to the guidelines of the Declaration of Helsinki and its later amendments and has been approved by the Medical Ethics Committee of Harbin Medical University (20191101).

Supplementary material

For supplementary material accompanying this paper visit https://doi.org/10.1017/S1368980021003335

References

Glinoer, D (1997) The regulation of thyroid function in pregnancy: pathways of endocrine adaptation from physiology to pathology. Endocr Rev 18, 404433.CrossRefGoogle ScholarPubMed
Pearce, EN, Lazarus, JH, Moreno-Reyes, R et al. (2016) Consequences of iodine deficiency and excess in pregnant women: an overview of current knowns and unknowns. Am J Clin Nutr 104, 918s923s.CrossRefGoogle ScholarPubMed
Glinoer, D (2007) The importance of iodine nutrition during pregnancy. Public Health Nutr 10, 15421546.CrossRefGoogle ScholarPubMed
WHO, UNICEF & ICCIDD (2007) Assessment of Iodine Deficiency Disorders and Monitoring Their Elimination: A Guide for Programme Managers, 3rd ed. Geneva: WHO Press.Google Scholar
CSoPM & CSoE (2019) Guideline on diagnosis and management of thyroid diseases during pregnancy and postpartum (2nd edition). Chin J Perinat Med 22, 505506.Google Scholar
Ma, ZF, Venn, BJ, Manning, PJ et al. (2018) The sensitivity and specificity of thyroglobulin concentration using repeated measures of urinary iodine excretion. Eur J Nutr 57, 13131320.CrossRefGoogle ScholarPubMed
Knudsen, N, Christiansen, E, Brandt-Christensen, M et al. (2000) Age- and sex-adjusted iodine/creatinine ratio. A new standard in epidemiological surveys? Evaluation of three different estimates of iodine excretion based on casual urine samples and comparison to 24 h values. Eur J Clin Nutr 54, 361363.CrossRefGoogle ScholarPubMed
Chen, W, Li, X, Guo, X et al. (2017) Urinary iodine excretion (UIE) estimated by iodine/creatinine ratio from spot urine in Chinese school-age children. Clin Endocrinol 86, 628633.CrossRefGoogle ScholarPubMed
Gabriela, MB, Simone, AJ, Peter, S et al. (2015) Iodine status assessment in children: spot urine iodine concentration reasonably reflects true 24-h iodine excretion only when scaled to creatinine. Thyroid 25, 688697.Google Scholar
Ye, B, Lin, Y, Chunyuan, T et al. (2021) 24 h urinary creatinine excretion during pregnancy and its application in appropriate estimation of 24 h urinary iodine excretion. J Trace Elem Med Biol 66, 126751.Google Scholar
Kesteloot, H & Joossens, JV (1996) On the determinants of the creatinine clearance: a population study. J Hum Hypertens 10, 245249.Google ScholarPubMed
Mage, DT, Allen, RH & Kodali, A (2008) Creatinine corrections for estimating children’s and adults’ pesticide intake doses in equilibrium with urinary pesticide and creatinine concentrations. J Expo Sci Environ Epidemiol 18, 360368.CrossRefGoogle Scholar
Perrine, CG, Cogswell, ME, Swanson, CA et al. (2014) Comparison of population iodine estimates from 24-h urine and timed-spot urine samples. Thyroid 24, 748757.CrossRefGoogle Scholar
Bath, SC, Furmidge-Owen, VL, Redman, CWG et al. (2015) Gestational changes in iodine status in a cohort of pregnant women from the United Kingdom: season as an effect modifier. Am J Clin Nutr 101, 11801187.CrossRefGoogle Scholar
Institute of Medicine & Academy of Sciences (2001) Dietary Reference Intakes for Vitamin A, Vitamin K, Arsenic, Boron, Chromium, Copper, Iodine, Iron, Manganese, Molybdenum, Nickel, Silicon, Vanadium, and Zinc. Washington, DC: The National Academies Press.Google Scholar
Vought, RL & London, WT (1967) Iodine intake, excretion and thyroidal accumulation in healthy subjects. J Clin Endocrinol Metab 27, 913919.CrossRefGoogle ScholarPubMed
Local Branch of Chinese Medical Association, Chinese Society of Nutrition & Chinese Society of Endocrinology (2018) Guidelines for Iodine Supplementation for Chinese Residents. Beijing: People’s Medical Publishing House.Google Scholar
Chinese Society of Perinatal Medicine (2014) Guidelines for diagnosis and treatment of iron deficiency and iron deficiency anemia during pregnancy. Chin J Perinat Med 17, 451454.Google Scholar
Pan, ZY, Cui, TK, Chen, W et al. (2019) Serum iodine concentration in pregnant women and its association with urinary iodine concentration and thyroid function. Clin Endocrinol 90, 711718.CrossRefGoogle ScholarPubMed
François, D (2007) Iodine requirements during pregnancy, lactation and the neonatal period and indicators of optimal iodine nutrition. Public Health Nutr 10, 15711580.Google Scholar
Ji, X, Liu, P, Sun, Z et al. (2016) Intra-individual variation in urinary iodine concentration: effect of statistical correction on population distribution using seasonal three-consecutive-day spot urine in children. BMJ Open 6, e010217.CrossRefGoogle ScholarPubMed
Rasmussen, LB, Ovesen, L & Christiansen, E (1999) Day-to-day and within-day variation in urinary iodine excretion. Eur J Clin Nutr 53, 401407.CrossRefGoogle ScholarPubMed
McMullan, P, Hamill, L, Doolan, K et al. (2019) Iodine deficiency among pregnant women living in Northern Ireland. Clin Endocrinol 91, 639645.CrossRefGoogle ScholarPubMed
Mulder, TA, Korevaar, T, Peeters, RP et al. Urinary iodine concentrations in pregnant women and offspring brain morphology. Thyroid. Published online: 20 January 2021. doi: 10.1089/thy.2020.0582.Google Scholar
Zhao, W, Li, XY, Xia, XH et al. (2019) Iodine nutrition during pregnancy: past, present, and future. Biol Trace Elem Res 188, 196207.CrossRefGoogle ScholarPubMed
Soldin, OP (2002) Controversies in urinary iodine determinations. Clin Biochem 35, 575579.CrossRefGoogle ScholarPubMed
Glinoer, D (2004) The regulation of thyroid function during normal pregnancy: importance of the iodine nutrition status. Best Pract Res Clin Endocrinol Metab 18, 133152.CrossRefGoogle ScholarPubMed
Chinese Nutrition Society (CNS) (2016) Dietary Guidelines for Chinese Residents. Beijing: People’s Medical Publishing House.Google Scholar
Liu, XB, Wu, M, Zhang, Y et al. (2018) Assessment of iodine nutritional status for pregnant women using adjusted urine creatinine from spot and 24-h urine. Wei Sheng Yan Jiu 47, 548553.Google Scholar
Patrick, W & Paul, C (2019) The assessment of iodine status-populations, individuals and limitations. Ann Clin Biochem 56, 714.Google Scholar
Li, CY, Peng, SQ, Zhang, XM et al. (2016) The urine iodine to creatinine as an optimal index of iodine during pregnancy in an iodine adequate area in China. J Clin Endocrinol Metab 101, 12901298.CrossRefGoogle Scholar
Eastman, C J, Ma, G & Li, M (2019) Optimal assessment and quantification of iodine nutrition in pregnancy and lactation: laboratory and clinical methods, controversies and future directions. Nutrients 11, 2378.CrossRefGoogle ScholarPubMed
Laurberg, P, Andersen, S, Bjarnodottir, RI et al. (2007) Evaluating iodine deficiency in pregnant women and young infants – complex physiology with a risk of misinterpretation. Public Health Nutr 10, 15471552.CrossRefGoogle Scholar
Als, C, Helbling, A, Peter, K et al. (2000) Urinary iodine concentration follows a circadian rhythm: a study with 3023 spot urine samples in adults and children. J Clin Endocrinol Metab 85, 13671369.Google Scholar
Andersen, SL, Sorensen, LK, Krejbjerg, A et al. (2014) Challenges in the evaluation of urinary iodine status in pregnancy: the importance of iodine supplement intake and time of sampling. Eur Thyroid J3, 179188.CrossRefGoogle Scholar
Yu, S, Yin, Y, Cheng, Q et al. (2018) Validation of a simple inductively coupled plasma mass spectrometry method for detecting urine and serum iodine and evaluation of iodine status of pregnant women in Beijing. Scand J Clin Lab Invest 78, 501507.CrossRefGoogle ScholarPubMed
Alexandra, CP, Tuija, M, Griffith, AB et al. (2019) The joint role of thyroid function and iodine status on risk of preterm birth and small for gestational age: a population-based nested case-control study of Finnish women. Nutrients 11, 2573.Google Scholar
Nishiyama, S, Mikeda, T, Okada, T et al. (2004) Transient hypothyroidism or persistent hyperthyrotropinemia in neonates born to mothers with excessive iodine intake. Thyroid 14, 10771083.CrossRefGoogle ScholarPubMed
Guo, WX, Wang, W, Jin, J et al. (2020) Trimester-specific thyroid function in pregnant women with different iodine statuses. Ann Nutr Metab 76, 165174.CrossRefGoogle ScholarPubMed
Gabriella, ME, María, JO & Francisco, ER (2007) Iodine deficiency and brain development in the first half of pregnancy. Public Health Nutr 10, 15541570.Google Scholar
Liu, P, Wang, Y, Zhao, J et al. (2015) Investigation of thyroid function change and urinary iodine standard of pregnant women. Chin J Endemiol 34, 357360.Google Scholar
Wang, L, Liu, P & Liu, L (2011) The proper urinary iodine reference values of pregnancy and lactating women in parts of China. J Pract Obstet Gynecol 27, 269271.Google Scholar
Bath, SC, Steer, CD, Golding, J et al. (2013) Effect of inadequate iodine status in UK pregnant women on cognitive outcomes in their children: results from the Avon Longitudinal Study of Parents and Children (ALSPAC). Lancet 382, 331337.CrossRefGoogle Scholar
Deborah, L, Bath, SC, Guxens, M et al. (2020) Maternal iodine status during pregnancy is not consistently associated with attention-deficit hyperactivity disorder or autistic traits in children. J Nutr 150, 15161528.Google Scholar
Figure 0

Table 1 General characteristics of pregnant women

Figure 1

Fig. 1 Correlation between spot UIC, UI/Cr, 24-h UIEest and 24-h UIE. UIC urinary iodine concentration, UI/Cr, urinary iodine-to-creatinine ratio; 24-h UIEest; estimated 24-h urinary iodine excretion; 24-h UIE, 24-h urinary iodine excretion. a, b and c represent the consistency of spot UIC, UI/Cr and 24-h UIEest compared with 24-h UIE, respectively. The urinary indicators at four time periods (at fasting, 8:00–9:00, 11:00–12:00 and 16:00–17:00) are expressed by tail 1, tail 2, tail 3 and tail 4

Figure 2

Fig. 2 Consistency of spot UIC, UI/Cr and 24-h UIEest compared with 24-h UIE at different urine collection times. UIC, urinary iodine concentration; UI/Cr, urinary iodine-to-creatinine ratio; 24-h UIEest, estimated 24-h urinary iodine excretion; 24-h UIE, 24-h urinary iodine excretion; n, number of participants. The Bland–Altman plot shows the consistency of spot UIC (a), UI/Cr (b) and 24-h UIEest (c) compared with 24-h UIE. The urinary indicators at four time periods (at fasting, 8:00–9:00, 11:00–12:00 and 16:00–17:00) are expressed by tail 1, tail 2, tail 3 and tail 4. The solid line represents the relative average difference, and the dotted line represents the 95 % reference interval for the relative average difference. On the X-axis, ‘Mean’ means the average of spot UIC, UI/Cr or 24-h UIEest with 24-h UIE

Figure 3

Fig. 3 ROC curves and tangent point values for UIC, UI/Cr and 24-h UIEest from different urine collection times. UIC, urinary iodine concentration; UI/Cr, urinary iodine-to-creatinine ratio; 24-h UIEest, estimated 24-h urinary iodine excretion; 24-h UIE, 24-h urinary iodine excretion; n, number of participants. a and b represent the ROC curves of UIC, UI/Cr and 24-h UIEest for diagnosing insufficient iodine intake and excessive iodine intake, respectively. The urinary indicators at four time periods (at fasting, 8:00–9:00, 11:00–12:00 and 16:00–17:00) are expressed by tail 1, tail 2, tail 3 and tail 4

Figure 4

Table 2 Receiver operating characteristic (ROC) curves of insufficient and excessive iodine intake

Figure 5

Table 3 Reference values of 24-h UIE, 24-h UIEest (based on fasting UI/Cr), UIC and UI/Cr at fasting during the entire pregnancy and for each trimester

Supplementary material: File

Bu et al. supplementary material

Table S1

Download Bu et al. supplementary material(File)
File 30 KB
Supplementary material: PDF

Bu et al. supplementary material

Figure S1

Download Bu et al. supplementary material(PDF)
PDF 1.9 MB