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Article

Selenium Intake and its Interaction with Iron Intake Are Associated with Cognitive Functions in Chinese Adults: A Longitudinal Study

1
School of Public Health, Chongqing Medical University, Chongqing 400016, China
2
Research Center for Medicine and Social Development, Chongqing Medical University, Chongqing 400016, China
3
Research Center for Public Health Security, Chongqing Medical University, Chongqing 400016, China
4
Chongqing Key Laboratory of Child Nutrition and Health, Children’s Hospital of Chongqing Medical University, Chongqing 400014, China
5
Human Nutrition Department, College of Health Sciences, QU Health, Qatar University, Doha 2713, Qatar
*
Author to whom correspondence should be addressed.
Nutrients 2022, 14(15), 3005; https://doi.org/10.3390/nu14153005
Submission received: 14 June 2022 / Revised: 12 July 2022 / Accepted: 20 July 2022 / Published: 22 July 2022

Abstract

:
Studies on the relation between selenium intake and cognitive function are inconclusive. This study aimed to examine the associations between dietary selenium intake and cognitive function among Chinese adults and tested the interaction effect of selenium intake and iron intake on cognition. Data from 4852 adults aged 55 years and above who attended the 1991–2006 China Health and Nutrition Survey (CHNS) were used. Cognitive function was assessed through face-to-face interviews in 1997, 2000, 2004, and 2006. A 3-day, 24-hour recall was used to collect dietary selenium intake. Multivariable mixed linear regression and logistic regression were used in the analyses. In fully adjusted regression models, the regression coefficients (95% confidence interval) were 0.00, 0.29 (−0.12–0.70), 0.26 (−0.18–0.70), and 0.50 (0.02–0.97) across the quartiles of selenium intake. In the subgroup analysis, the positive association between selenium intake and cognitive function was only observed in the participants who live in the southern region but not those in the northern region. The selenium-intake-to-iron-intake ratio was inversely associated with low global cognition scores. Furthermore, only those with a normal BMI had a positive association between selenium and cognition. In conclusion, high selenium intake was linked to better cognitive function and a lower risk of cognition decline in Chinese adults among those with low iron intake. A substantial interaction was found between selenium intake and BMI or region.

1. Introduction

Dementia imposes a considerable burden on human health. This disease was reported in 2020 to occur in over 55 million people worldwide and the occurrence was reported to likely double every 20 years [1,2]. The total estimated worldwide cost of dementia was USD 1.3 trillion in 2019, which represented 1.4% of the global gross domestic product (GDP). If global dementia care was a country, it would have the 15th largest economy in the world [1,2].
Selenium is an essential trace element that protects tissues from oxidative damage [3]. It also plays a critical role in anti-inflammatory effects, thyroid hormone metabolism, DNA synthesis, antiapoptotic function, and reproduction [4]. Furthermore, selenium is vital for the central nervous system and participates in the pathology of disorders, such as Alzheimer’s disease (AD) and Parkinson’s disease (PD) [5]. The first direct evidence that selenium has a particular role in the central nervous system came from a study of children with intractable seizures who were found to have reduced glutathione peroxidase activity and showed clinical improvement after taking selenium supplements. [6]. Furthermore, selenium levels in the body decrease progressively with age and have a positive correlation with cognitive performance in older adults [7,8]. These pieces of evidence suggest that maintaining normal selenium levels in humans may reduce the risk of cognitive disorders.
However, some studies suggest that environmental exposure to excess selenium levels may cause the onset and/or development of neurobehavioral abnormalities in humans and animals [9,10]. In addition, excessive selenium exposure may impair the functions of several important proteins, neurotransmitter systems (including the dopaminergic, glutamatergic, cholinergic, and serotonergic systems), and signaling molecules involved in the management and regulation of cognitive function [9,11,12]. Population studies found that high selenium exposure is associated with the development of several neurodegenerative and neuropsychiatric diseases [13,14,15,16].
In fact, selenium deficiency and selenium overload are common. In China, 39–61% of the population have a selenium intake level below the WHO/FAO (2004) recommendation (<55 μg/day), and 10% of the population have a selenium intake level above the recommendation (>400 μg/day) [17]. Some populations may tolerate low or high selenium intake better than others (such as the Inuit in Greenland and some populations in China) [18]. In addition, previous studies focused more on Keshan disease, which is endemic to soil and grain selenium deficient areas in China [19,20]. Therefore, the relationship between selenium and cognition needs to be further explored in different populations.
Overall, studies on the association between cognitive function and selenium intake are limited. No study has examined the association between selenium intake status and cognitive function in China. This study analyzed the data from the China Health and Nutrition Survey (CHNS) to examine the associations between dietary selenium intake and cognitive function among Chinese adults aged 55 years and above to close this research gap.

2. Methods

2.1. Study Design and Study Sample

The CHNS, which is an ongoing cohort survey, is a joint project between the National Institute for Nutrition and Health at the Chinese Center for Disease Control and Prevention and the Carolina Population Center at the University of North Carolina at Chapel Hill. This nationwide survey uses a multistage cluster sampling technique to select participants in urban and rural areas. A variety of methods were used for data collection, including interviews, questionnaires, physical examinations, and anthropometric measurements. Eleven waves of surveys were conducted (1989, 1991, 1993, 1997, 2000, 2004, 2006, 2009, 2011, 2015, and 2018). Cognitive function screening tests were administered to participants over the age of 55 in the surveys conducted in 1997, 2000, 2004, and 2006. A total of 4852 participants who took the cognitive screening test between 1997 and 2006 had dietary intake data (Figure 1). Among these participants, 3302 participated in ≥2 survey screening tests. Participants who completed at least one cognitive screening test were included in the analysis. The Chinese National Institute of Nutrition and Food Safety and the University of North Carolina’s Institutional Review Board both gave their approval for this study. All participants gave informed consent. The response rate of those who participated in the survey in 1989 and 2006 was more than 60%. The data used in the present study were downloaded from the CHNS website (https://www.cpc.unc.edu/projects/china. Accessed on 21 January 2022).

2.2. Outcome Variable: Cognitive Function

Global cognitive function: The cognitive function test items used in the CHNS included a subset of items from the widely used Telephone Interview for Cognitive Status-Modified (TICS-M) [21,22,23]. The test was administered through a face-to-face cognitive function screening test. The cognitive screening consisted of three tasks: (1) immediate and delayed recall of a list of 10 words (10 points each), (2) counting down from 20 to 1 (2 points), and (3) serial 7 subtraction (5 points). In the current study, the first quartile of the cognitive function test score, which is equivalent to the cutoff value < 7 for the global cognitive function score, was chosen to represent poor cognitive function. The cutoff was chosen in light of a study in Shanghai, which revealed a 20% prevalence of mild cognitive impairment in persons 60 years and older. [24].
Self-reported memory: Self-reported memory was assessed by the question “How is your memory? (1) Very good, (2) good, (3) OK, (4) bad, (5) very bad, (9) unknown.” Participants were defined as having a poor memory if they answered “bad” or “‘very bad”. Participants were asked about their change in memory by the question “In the past 12 months, how has your memory changed? (1) Improved, (2) stayed the same, (3) declined, (9) unknown.” Participants were defined as having self-reported memory decline if they reported “declined”.

2.3. Exposure Variable: Dietary Intake of Selenium

A 3-day, 24-hour recall was used to collect dietary intake data in each survey wave. During the 3-day diet survey, food and condiments from household stock, market, garden, and leftover food scraps were weighed and recorded by well-trained investigators. The intake of nutrients, including selenium, was calculated using the average of 3 days’ food consumption data in combination with the Chinese Food Composition Table [25]. Regional differences in the nutrient composition of foods (such as rice) grown in different regions were reflected in the China Food Composition Table by specific food codes. The cumulative selenium consumption was calculated and used as an exposure variable. This approach was used to reduce individual variation and reflect long-term eating patterns [26]. For instance, if a person consumed x in 2000, y in 2004, and z in 2006, the cumulative mean in 2004 was (x + y)/2, whereas that in 2006 was (x + y + z)/3.

2.4. Covariates

In each survey, sociodemographic and lifestyle factors were collected using a structured questionnaire. The following constructed variables were considered covariates: age, sex, per capita annual family income (recoded as low, medium, and high), education (low, illiterate/primary school; medium, middle school; and high, senior high school and higher), urbanization levels (low, medium, and high), smoking status (non-smoker, ex-smoker, and current smoker), and leisure time physical activity (metabolic equivalent of task (MET), min/week). Hypertension was defined as systolic blood pressure over 140 mmHg, diastolic blood pressure over 90 mmHg, or known hypertension. Physical activity level (MET) was computed based on self-reported activities (including occupational, domestic, transportation, and leisure time physical activity) and duration was calculated using the Adult Compendium of Physical Activities [27]. Body mass index (BMI) was used to assess adiposity levels, and overweight was defined as BMI ≥ 24 kg/m2 [28]. Diabetes and stroke were self-reported and recorded as “yes” or “no”.

2.5. Statistical Analyses

Intake of selenium was categorized into quartiles. Frequency and proportion (%) were used to describe categorical variables, and mean ± standard deviation (SD) was used to describe continuous variables. Baseline sample characteristics were presented according to the quartiles of selenium intake and compared using a chi-square test for categorical variables or ANOVA for continuous variables. The association between cumulative mean dietary selenium intake and cognitive function was investigated using mixed-effect logistic regression analysis in Stata with the mixed command. A negative regression coefficient indicates a decline in cognitive function. To examine the association, six multivariable models were used. Model 1 was adjusted for age, gender, and energy intake. Model 2 was further adjusted for fat intake, smoking, alcohol drinking, income, urbanicity, education, and physical activity. Model 3 was further adjusted for fruit and vegetable intake. Model 4 was further adjusted for BMI and hypertension. Model 5 excluded those who only participated in one wave of the cognitive function tests. Model 6 was further adjusted for self-reported diabetes and stroke. In the subgroup analyses, the multiplicative interaction between selenium intake and covariates (income, sex, urbanization, region, overweight, and hypertension) was added by adding a product term in the regression model. The marginsplot function in Stata was utilized to visualize the interaction. Stata 17.1 (Stata Corporation, College Station, TX, USA) was used in all analyses. There was consideration of statistical significance when p < 0.05 (two-sided).

3. Results

Table 1 shows the sample characteristics of the participants who attended the first cognitive function test based on the quartiles of selenium intake. Across the quartiles of selenium intake, the mean (±SD) cumulative selenium intake was 22.3 ± 4.9, 32.5 ± 2.2, 40.3 ± 2.6, and 60.7 ± 22.9. Energy, fat, protein, carbohydrate, iron, meat, fresh vegetable, and fruit intake increased across the quartiles of selenium intake. Participants with high selenium intake had a higher BMI and were more likely to drink alcohol. Urbanization, education, and family income were positively associated with selenium intake.

3.1. Association between Selenium Intake and Global Cognitive Function

Selenium intake was positively associated with cognitive function (Table 2). In the model adjusted for sociodemographic factors and lifestyle factors (model 3), the regression coefficients (95% confidence interval (CI)) were 0.00, 0.32 (−0.05–0.69), 0.44 (0.05–0.83), and 0.45 (0.02–0.87) across the quartiles of selenium intake. However, the association was attenuated and became marginally significant after further adjusting for BMI and hypertension (model 4). After the participants who only participated in one wave of the cognitive function test were excluded, high selenium intake was positively associated with global cognition score. Further adjusting for self-reported diabetes or stroke did not change the above association.

3.2. Association between Selenium Intake and Self-Reported Memory

Selenium intake was inversely associated with self-reported poor memory in a dose–response manner (Table 3). In the fully adjusted model, the odds ratios (ORs, 95% CI) across the quartiles of selenium intake were 1.00, 0.80 (0.67–0.96), 0.75 (0.61–0.91), and 0.68 (0.54–0.84), for self-reported poor memory and 1.00, 0.85 (0.73–1.01), 0.71 (0.60–0.85), and 0.65 (0.54–0.78), for self-reported memory decline.

3.3. Weight Status Modifies the Association between Selenium Intake and Global Cognitive Function

There was a significant interaction (p = 0.002) between selenium intake and BMI on the global cognitive function score (Figure 2). A strong positive association between selenium intake and good cognitive function was found among participants with low BMI. By contrast, there was an inverse association between selenium intake and cognitive function among participants with high BMI. In the subgroup analyses, a significant inverse association between selenium intake and a global cognition score < 7 was found only among participants with normal BMI (p for interaction = 0.012).

3.4. Subgroup Analyses

Selenium intake had no interactions with income, hypertension, gender, and urbanization in relation to the association with a global cognition score < 7. However, a regional difference in the association was observed. The association was only observed in the participants from the southern region but not those from the northern region (p for interaction = 0.005) (Table 4).
The selenium-intake-to-iron-intake ratio was inversely associated with a global cognition score < 7. In the fully adjusted model, the ORs (95% CI) across the quartiles of the selenium-intake-to-iron-intake ratio for a global cognition score < 7 were 1.00, 0.88 (0.74–1.06), 0.62 (0.51–0.77), and 0.60 (0.47–0.77, p < 0.001). However, the association between selenium intake and cognitive function was independent of iron intake (data not shown).

4. Discussion

This study investigated the association of selenium intake with cognitive function in a large cohort of Chinese adults aged 55 years and above. Those with high selenium intake were associated with a high global cognition score and less likely to report poor memory and memory decline. Selenium intake had remarkable interactions with BMI and region. The positive association between selenium intake and cognition was only observed among those with a normal BMI and those who lived in the southern region.
Studies on the association between selenium status and cognitive function are inconsistent. In adults, selenium levels decrease with age and may contribute to age-related decline in cognitive function [29]. Using the National Health and Nutrition Examination Survey database, which focuses on adult participants aged 60 years or older, Li et al. found that high selenium intake is inversely associated with the prevalence of low cognitive performance [30]. A cohort study of 1666 French adults aged 60–70 years old indicated that those with low blood selenium levels have an elevated risk of cognitive decline [31]. A cross-sectional survey of 2000 Chinese rural residents aged 65 years or older in two provinces in China showed that lower nail selenium levels are substantially associated with lower cognitive scores [32]. A study conducted in old Sicilian individuals aged 60 years and above demonstrated that patients with AD have reduced blood selenium concentrations [33]. However, some studies found that plasma selenium is not associated with cognitive performance [34] and observed no changes in total selenium concentration in the serum or cerebrospinal fluid of participants with AD compared with patients with mild cognitive impairment and healthy controls [35]. Certain selenium species were even deemed risk factors for neurodegeneration in several observational studies. Vinceti et al. reported that higher levels of selenoprotein P in the cerebrospinal fluid are linked to a lower risk of sporadic amyotrophic lateral sclerosis (ALS), whereas elevated selenite in the cerebrospinal fluid is linked to a higher risk of neurodegeneration [36]. Recently, Vinceti et al. also observed an increased risk of developing AD later in life among patients with mild cognitive impairment who have increased concentration of the potentially toxic inorganic selenium species, selenate or Se(VI), in the cerebrospinal fluid [37].
The mechanisms linking selenium intake and cognitive function are yet to be fully elucidated. Oxidative stress is thought to be a major cause of cognitive impairment involved in the development of multiple neurodegenerative diseases [38]. Selenium is an important antioxidant; therefore, it may be especially helpful for combating oxidative stress. Free radicals are related with problems in mitochondrial function, neuroinflammation, synaptic transmission, and axonal transport; a shortage in this mineral may increase oxidative stress, which can lead to neuronal death [39,40]. The brain’s principal selenoproteins are selenoprotein P and glutathione peroxidase. Selenoprotein P is the major selenium transporter. This protein was found in the characteristic senile plaques and neurofibrillary tangles in the brains of patients with AD, which implies that it plays a key function in oxidative damage protection [41]. Glutathione peroxidase enzymes are expressed by neurons and glial cells [42]. They have a crucial antioxidant role; they accelerate the elimination of hydrogen peroxides, organic hydroperoxides, and lipid peroxides and protect cells from oxidative damage by lowering glutathione [43]. In summary, a selenium deficiency reduces the protective effects of antioxidant enzymes in the brain and causes oxidative stress, which can lead to brain tissue damage and cognitive decline.
A positive association between the ratio of selenium intake to iron intake and cognitive function means that higher selenium intake and lower iron intake lead to better cognitive function. Previous studies in China reported the negative effects of excessive iron intake on cognitive function in the elderly [44,45]. Furthermore, some population studies found that iron intake is positively associated with disorders that cause cognitive deterioration, such as PD [46,47]. Several human laboratory reviews also indicated a consistent correlation between iron deposition and cognitive impairment in humans with the usage of imaging techniques and found that iron chelation could be used as a potential therapy for memory deficits [48,49,50]. As a redox-active ion, iron impairs neurocognitive function by causing oxidative stress, damaging the mitochondria, and resulting in neurons’ energy production being hindered. Oxidative stress may also induce apoptosis, which contributes to neuronal loss and finally leads to cognitive decline [48].
In our study, the positive association between selenium intake and a low cognitive function score was only observed in the participants from the southern region, but not in those from the northern region. This finding could be attributed to the higher prevalence of dementia in North China compared with that in South China. The prevalence of dementia is 5.5% in North China and 4.8% in South China according to a meta-analysis published in 2018 [51]. The northern region may have more important factors influencing the prevalence of dementia other than selenium, such as obesity and smoking [2]. Additionally, the northern and southern regions of China have different dietary habits. For example, rice is the staple food in the south, whereas selenium-rich wheat is the staple food in the north, which means that the people from the north have a higher selenium intake than those from the south [52]. Some studies found that the dietary selenium intake of over 55 μg/day cannot improve selenoprotein synthesis or activity in selenium-deficient patients [53,54]. Therefore, no association in the north may also be due to excessive selenium intake in some participants from the north. However, we have some conflicting results here. For self-reported poor memory/memory decline, the inverse association with selenium intake was significant in the north (data not shown). Further studies are needed to elucidate the mechanisms of the regional difference in the association between selenium intake and cognition.
The interaction between BMI and selenium intake with regard to cognitive function is interesting. The positive correlation between the cognitive function score and selenium intake diminishes as BMI increases. The relationship even becomes negative in obese participants. A study by Benjamin et al. indicated that cognitive decline slows down among patients with amnestic mild cognitive impairment (aMCI) and a higher BMI [55]. Another study found high BMI is associated with higher baseline impairment in aMCI and AD and slower clinical progression in aMCI [56]. Additionally, according to a cohort study of nearly 2 million people tracked retrospectively over 20 years, those who are underweight had a significantly increased risk of dementia [57]. These pieces of evidence imply that obesity may be an independent protective factor for cognitive impairment. The mechanisms of the interaction need to be further explored.
Several strengths in our study should be highlighted. First of all, this is a longitudinal study with multiple waves of dietary assessments based on three-day meal recalls and household food inventory records which provide a robust estimate of long-term selenium intake. Second, the large sample from different provinces allowed our findings to be generalized in a broader population. Third, we were able to control for a variety of potential confounders. Lastly, analyzing the link between high selenium intake and cognitive function was possible because of the large variation in selenium intake.
This study also has limitations. First, using a 3-day dietary intake survey to quantify long-term dietary selenium consumption may be insufficient. Second, respondents may have recall bias for the information collected on self-reported poor memory, memory decline, and other self-reported variables. Third, although we adjusted various sociodemographic and lifestyle factors in the multivariate analysis such as income, BMI, and diet, other residual confounding factors may also be present. Last, no data on selenium biomarkers (e.g., hair and serum selenium) were available.

5. Conclusions

In summary, high selenium intake was associated with a better cognitive function and lower risk of cognition decline in Chinese individuals aged 55 years and above regardless of gender, lifestyle, and sociodemographic factors. There was a significant interaction between selenium intake and iron intake, showing improved cognitive function in those with higher selenium intake and low iron intake. We also found selenium intake had remarkable interactions with BMI and region. Further studies with repeated measures of selenium intake and serum selenium in different populations are needed to confirm our finding.

Author Contributions

K.J. and Z.S. contributed to the conception, analysis, and interpretation of data, drafted the report and received the final version for publication. C.X., Z.L., H.Z. contributed to analyzing and interpreting the data, commented on the report and revised the manuscript. Project administration, Y.Z.; Supervision, Y.Z.; Writing—review & editing, C.X., Z.L., H.Z. and Y.Z. All authors have read and agreed to the published version of the manuscript.

Funding

This project was funded by the project of Chongqing Nutrition Society (2019001)— Research on dietary selenium intake and its relationship with hypertension and diabetes in middle-aged and older adults in Jiangjin Chongqing. The funders had no role in the design, analysis, data interpretation, and publication of the findings.

Institutional Review Board Statement

Written informed consent for CHNS was reviewed by the University of North Carolina (USA) and the National Institute of Nutrition and Food Safety (China). We used publicly-available datasets from the official CHNS website (https://www.cpc.unc.edu/projects/china accessed on 21 January 2022). Therefore, the need for ethics approval was not applicable.

Informed Consent Statement

Written informed consent for CHNS was reviewed by the University of North Carolina (USA) and the National Institute of Nutrition and Food Safety (China). We used publicly-available datasets from the official CHNS website (https://www.cpc.unc.edu/projects/china accessed on 21 January 2022). Therefore, the need for ethics approval was not applicable.

Data Availability Statement

The datasets generated during and analyzed during the current study are available in the CHNS repository, https://www.cpc.unc.edu/projects/china accessed on 21 January 2022.

Conflicts of Interest

The authors have no relevant financial or non-financial interests to disclose.

References

  1. Fleming, R.; Zeisel, J.; Arch, K.B.B. World Alzheimer Report 2020; Alzheimer’s Disease International (ADI): London, UK, 2020. [Google Scholar]
  2. WHO. Dementia. 2022. Available online: https://www.who.int/en/news-room/fact-sheets/detail/dementia (accessed on 15 December 2021).
  3. Shreenath, A.P.; Ameer, M.A.; Dooley, J. Selenium Deficiency. In StatPearls; StatPearls Publishing: Treasure Island, FL, USA, 2021. [Google Scholar]
  4. Liu, B.; Xu, G.; Yang, W.; Strathearn, L.; Snetselaar, L.G.; Bao, W. Association between serum selenium concentrations and learning disability in a nationally representative sample of U.S. children. Nutr. Neurosci. 2021, 25, 1558–1564. [Google Scholar] [CrossRef] [PubMed]
  5. Solovyev, N.D. Importance of selenium and selenoprotein for brain function: From antioxidant protection to neuronal signalling. J. Inorg. Biochem. 2015, 153, 1–12. [Google Scholar] [CrossRef] [PubMed]
  6. Weber, G.F.; Maertens, P.; Meng, X.Z.; Pippenger, C.E. Glutathione peroxidase deficiency and childhood seizures. Lancet 1991, 337, 1443–1444. [Google Scholar] [CrossRef]
  7. Robberecht, H.; De Bruyne, T.; Davioud-Charvet, E.; Mackrill, J.; Hermans, N. Selenium Status in Elderly People: Longevity and Age-Related Diseases. Curr. Pharm. Des. 2019, 25, 1694–1706. [Google Scholar] [CrossRef] [PubMed]
  8. Fukui, K.; Omoi, N.O.; Hayasaka, T.; Shinnkai, T.; Suzuki, S.; Abe, K.; Urano, S. Cognitive impairment of rats caused by oxidative stress and aging, and its prevention by vitamin E. Ann. N. Y. Acad. Sci. 2002, 959, 275–284. [Google Scholar] [CrossRef]
  9. Nogueira, C.W.; Rocha, J.B. Toxicology and pharmacology of selenium: Emphasis on synthetic organoselenium compounds. Arch. Toxicol. 2011, 85, 1313–1359. [Google Scholar] [CrossRef]
  10. Oliveira, C.S.; Piccoli, B.C.; Aschner, M.; Rocha, J. Chemical Speciation of Selenium and Mercury as Determinant of Their Neurotoxicity. Adv. Neurobiol. 2017, 18, 53–83. [Google Scholar]
  11. Lemly, A.D. Aquatic selenium pollution is a global environmental safety issue. Ecotoxicol. Environ. Saf. 2004, 59, 44–56. [Google Scholar] [CrossRef] [Green Version]
  12. Dolgova, N.V.; Hackett, M.J.; MacDonald, T.C.; Nehzati, S.; James, A.K.; Krone, P.H.; George, G.N.; Pickering, I.J. Distribution of selenium in zebrafish larvae after exposure to organic and inorganic selenium forms. Metallomics 2016, 8, 305–312. [Google Scholar] [CrossRef] [Green Version]
  13. Naderi, M.; Puar, P.; Zonouzi-Marand, M.; Chivers, D.P.; Niyogi, S.; Kwong, R.W.M. A comprehensive review on the neuropathophysiology of selenium. Sci. Total Environ. 2021, 767, 144329. [Google Scholar] [CrossRef]
  14. Vinceti, M.; Guidetti, D.; Pinotti, M.; Rovesti, S.; Merlin, M.; Vescovi, L.; Bergomi, M.; Vivoli, G. Amyotrophic lateral sclerosis after long-term exposure to drinking water with high selenium content. Epidemiology 1996, 7, 529–532. [Google Scholar] [CrossRef] [PubMed]
  15. Callaghan, B.; Feldman, D.; Gruis, K.; Feldman, E. The association of exposure to lead, mercury, and selenium and the development of amyotrophic lateral sclerosis and the epigenetic implications. Neurodegener. Dis. 2011, 8, 1–8. [Google Scholar] [CrossRef] [PubMed]
  16. Bergomi, M.; Vinceti, M.; Nacci, G.; Pietrini, V.; Brätter, P.; Alber, D.; Ferrari, A.; Vescovi, L.; Guidetti, D.; Sola, P.; et al. Environmental exposure to trace elements and risk of amyotrophic lateral sclerosis: A population-based case-control study. Environ. Res. 2002, 89, 116–123. [Google Scholar] [CrossRef] [PubMed]
  17. Dinh, Q.T.; Cui, Z.; Huang, J.; Tran, T.A.T.; Wang, D.; Yang, W.; Zhou, F.; Wang, M.; Yu, D.; Liang, D. Selenium distribution in the Chinese environment and its relationship with human health: A review. Environ. Int. 2018, 112, 294–309. [Google Scholar] [CrossRef] [PubMed]
  18. Rayman, M.P. Selenium intake, status, and health: A complex relationship. Hormones 2020, 19, 9–14. [Google Scholar] [CrossRef] [Green Version]
  19. Zhou, H.; Wang, T.; Li, Q.; Li, D. Prevention of Keshan Disease by Selenium Supplementation: A Systematic Review and Meta-analysis. Biol. Trace Elem. Res. 2018, 186, 98–105. [Google Scholar] [CrossRef]
  20. Chen, J. An original discovery: Selenium deficiency and Keshan disease (an endemic heart disease). Asia Pac. J. Clin. Nutr. 2012, 21, 320–326. [Google Scholar]
  21. Lei, X.; Hu, Y.; McArdle, J.J.; Smith, J.P.; Zhao, Y. Gender Differences in Cognition among Older Adults in China. J. Hum. Resour. 2012, 47, 951–971. [Google Scholar]
  22. Duff, K.; Tometich, D.; Dennett, K. The Modified Telephone Interview for Cognitive Status is More Predictive of Memory Abilities Than the Mini-Mental State Examination. J. Geriatr. Psychiatry Neurol. 2015, 28, 193–197. [Google Scholar] [CrossRef] [Green Version]
  23. Plassman, B.L.; Welsh, K.A.; Helms, M.; Brandt, J.; Page, W.F.; Breitner, J.C. Intelligence and education as predictors of cognitive state in late life: A 50-year follow-up. Neurology 1995, 45, 1446–1450. [Google Scholar] [CrossRef]
  24. Ding, D.; Zhao, Q.; Guo, Q.; Meng, H.; Wang, B.; Luo, J.; Mortimer, J.A.; Borenstein, A.R.; Hong, Z. Prevalence of mild cognitive impairment in an urban community in China: A cross-sectional analysis of the Shanghai Aging Study. Alzheimer’s Dement. 2015, 11, 300–309. [Google Scholar] [CrossRef] [PubMed]
  25. Yang, Y. Chinese Food Composition Table 2004; Peking University Medical Press: Beijing, China, 2005. [Google Scholar]
  26. Hu, F.B.; Stampfer, M.J.; Rimm, E.; Ascherio, A.; Rosner, B.A.; Spiegelman, D.; Willett, W.C. Dietary fat and coronary heart disease: A comparison of approaches for adjusting for total energy intake and modeling repeated dietary measurements. Am. J. Epidemiol. 1999, 149, 531–540. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  27. Ainsworth, B.E.; Haskell, W.L.; Whitt, M.C.; Irwin, M.L.; Swartz, A.M.; Strath, S.J.; O’Brien, W.L.; Bassett, D.J.; Schmitz, K.H.; Emplaincourt, P.O.; et al. Compendium of physical activities: An update of activity codes and MET intensities. Med. Sci. Sports Exerc. 2000, 32, S498–S504. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  28. Zhou, B.F. Predictive values of body mass index and waist circumference for risk factors of certain related diseases in Chinese adults—Study on optimal cut-off points of body mass index and waist circumference in Chinese adults. Biomed. Environ. Sci. 2002, 15, 83–96. [Google Scholar]
  29. Mecocci, P.; Polidori, M.C. Antioxidant clinical trials in mild cognitive impairment and Alzheimer’s disease. Biochim. Biophys. Acta (BBA)-Mol. Basis Dis. 2012, 1822, 631–638. [Google Scholar] [CrossRef]
  30. Li, S.; Sun, W.; Zhang, D. Association of Zinc, Iron, Copper, and Selenium Intakes with Low Cognitive Performance in Older Adults: A Cross-Sectional Study from National Health and Nutrition Examination Survey (NHANES). J. Alzheimer’s Dis. 2019, 72, 1145–1157. [Google Scholar] [CrossRef]
  31. Berr, C.; Balansard, B.; Arnaud, J.; Roussel, A.M.; Alpérovitch, A. Cognitive decline is associated with systemic oxidative stress: The EVA study. Etude Du Vieil. Artériel. J. Am. Geriatr. Soc. 2000, 48, 1285–1291. [Google Scholar] [CrossRef]
  32. Gao, S.; Jin, Y.; Hall, K.S.; Liang, C.; Unverzagt, F.W.; Ji, R.; Murrell, J.R.; Cao, J.; Shen, J.; Ma, F.; et al. Selenium Level and Cognitive Function in Rural Elderly Chinese. Am. J. Epidemiol. 2007, 165, 955–965. [Google Scholar] [CrossRef] [Green Version]
  33. Giacoppo, S.; Galuppo, M.; Calabrò, R.S.; Aleo, G.; Marra, A.; Sessa, E.; Bua, D.G.; Potortì, A.G.; Dugo, G.; Bramanti, P.; et al. Heavy Metals and Neurodegenerative Diseases: An Observational Study. Biol. Trace Elem. Res. 2014, 161, 151–160. [Google Scholar] [CrossRef]
  34. Cardoso, B.; Szymlek-Gay, E.; Roberts, B.; Formica, M.; Gianoudis, J.; Connell, S.; Nowson, C.; Daly, R. Selenium Status Is Not Associated with Cognitive Performance: A Cross-Sectional Study in 154 Older Australian Adults. Nutrients 2018, 10, 1847. [Google Scholar] [CrossRef] [Green Version]
  35. Cardoso, B.R.; Hare, D.J.; Bush, A.I.; Li, Q.; Fowler, C.J.; Masters, C.L.; Martins, R.N.; Ganio, K.; Lothian, A.; Mukherjee, S.; et al. Selenium Levels in Serum, Red Blood Cells, and Cerebrospinal Fluid of Alzheimer’s Disease Patients: A Report from the Australian Imaging, Biomarker & Lifestyle Flagship Study of Ageing (AIBL). J. Alzheimer’s Dis. 2017, 57, 183–193. [Google Scholar]
  36. Vinceti, M.; Solovyev, N.; Mandrioli, J.; Crespi, C.M.; Bonvicini, F.; Arcolin, E.; Georgoulopoulou, E.; Michalke, B. Cerebrospinal fluid of newly diagnosed amyotrophic lateral sclerosis patients exhibits abnormal levels of selenium species including elevated selenite. Neurotoxicology 2013, 38, 25–32. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  37. Vinceti, M.; Chiari, A.; Eichmüller, M.; Rothman, K.J.; Filippini, T.; Malagoli, C.; Weuve, J.; Tondelli, M.; Zamboni, G.; Nichelli, P.F. A selenium species in cerebrospinal fluid predicts conversion to Alzheimer’s dementia in persons with mild cognitive impairment. Alzheimer’s Res. Ther. 2017, 9, 100. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  38. Cui, K.; Luo, X.; Xu, K.; Murthy, M.V. Role of oxidative stress in neurodegeneration: Recent developments in assay methods for oxidative stress and nutraceutical antioxidants. Prog. Neuro-Psychopharmacol. Biol. Psychiatry 2004, 28, 771–799. [Google Scholar] [CrossRef]
  39. de la Monte, S.M.; Tong, M.; Lester-Coll, N.; Plater, M., Jr.; Wands, J.R. Therapeutic rescue of neurodegeneration in experimental type 3 diabetes: Relevance to Alzheimer’s disease. J. Alzheimer’s Dis. 2006, 10, 89–109. [Google Scholar] [CrossRef]
  40. Swerdlow, R.H.; Burns, J.M.; Khan, S.M. The Alzheimer’s disease mitochondrial cascade hypothesis: Progress and perspectives. Biochim. Et Biophys. Acta (BBA)-Mol. Basis Dis. 2014, 1842, 1219–1231. [Google Scholar] [CrossRef] [Green Version]
  41. Solovyev, N. Selenoprotein P and its potential role in Alzheimer’s disease. Hormones 2020, 19, 73–79. [Google Scholar] [CrossRef]
  42. Zhang, S.; Rocourt, C.; Cheng, W. Selenoproteins and the aging brain. Mech. Ageing Dev. 2010, 131, 253–260. [Google Scholar] [CrossRef]
  43. Adwas, A.A.; Elsayed, A.; Azab, A.E.; Quwaydir, F.A. Oxidative stress and antioxidant mechanisms in human body. J. Appl. Biotechnol. Bioeng. 2019, 6, 43–47. [Google Scholar]
  44. Shi, Z.; Li, M.; Wang, Y.; Liu, J.; El-Obeid, T. High iron intake is associated with poor cognition among Chinese old adults and varied by weight status—A 15-y longitudinal study in 4852 adults. Am. J. Clin. Nutr. 2019, 109, 109–116. [Google Scholar] [CrossRef]
  45. Shi, Z.; El-Obeid, T.; Li, M.; Xu, X.; Liu, J. Iron-related dietary pattern increases the risk of poor cognition. Nutr. J. 2019, 18, 48. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  46. Logroscino, G.; Gao, X.; Chen, H.; Wing, A.; Ascherio, A. Dietary iron intake and risk of Parkinson’s disease. Am. J. Epidemiol. 2008, 168, 1381–1388. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  47. Powers, K.M.; Smith-Weller, T.; Franklin, G.M.; Longstreth, W.J.; Swanson, P.D.; Checkoway, H. Parkinson’s disease risks associated with dietary iron, manganese, and other nutrient intakes. Neurology 2003, 60, 1761–1766. [Google Scholar] [CrossRef] [PubMed]
  48. Schröder, N.; Figueiredo, L.S.; de Lima, M.N. Role of brain iron accumulation in cognitive dysfunction: Evidence from animal models and human studies. J. Alzheimers Dis. 2013, 34, 797–812. [Google Scholar] [CrossRef]
  49. Ward, R.J.; Zucca, F.A.; Duyn, J.H.; Crichton, R.R.; Zecca, L. The role of iron in brain ageing and neurodegenerative disorders. Lancet Neurol. 2014, 13, 1045–1060. [Google Scholar] [CrossRef] [Green Version]
  50. Lavado, L.K.; Zhang, M.H.; Patel, K.; Khan, S.; Patel, U.K. Biometals as Potential Predictors of the Neurodegenerative Decline in Alzheimer’s Disease. Cureus 2019, 11, e5573. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  51. Wu, Y.T.; Ali, G.C.; Guerchet, M.; Prina, A.M.; Chan, K.Y.; Prince, M.; Brayne, C. Prevalence of dementia in mainland China, Hong Kong and Taiwan: An updated systematic review and meta-analysis. Int. J. Epidemiol. 2018, 47, 709–719. [Google Scholar] [CrossRef] [Green Version]
  52. Song, F.; Cho, M.S. Geography of Food Consumption Patterns between South and North China. Foods 2017, 6, 34. [Google Scholar] [CrossRef] [Green Version]
  53. Burk, R.F. Selenium, an antioxidant nutrient. Nutr. Clin. Care 2002, 5, 75–79. [Google Scholar] [CrossRef]
  54. Mayne, S.T. Dietary Reference Intakes for Vitamin C, Vitamin E, Selenium, and Carotenoids; National Academies Press (US): Washington, DC, USA, 2000. [Google Scholar]
  55. Cronk, B.B.; Johnson, D.K.; Burns, J.M.; Initiative, A.S.D.N. Body mass index and cognitive decline in mild cognitive impairment. Alzheimer Dis. Assoc. Disord. 2010, 24, 126. [Google Scholar] [CrossRef] [Green Version]
  56. Besser, L.M.; Gill, D.P.; Monsell, S.E.; Brenowitz, W.; Meranus, D.; Kukull, W.; Gustafson, D.R. Body mass index, weight change, and clinical progression in mild cognitive impairment and Alzheimer’s disease. Alzheimer Dis. Assoc. Disord. 2014, 28, 36. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  57. Qizilbash, N.; Gregson, J.; Johnson, M.E.; Pearce, N.; Douglas, I.; Wing, K.; Evans, S.J.; Pocock, S.J. BMI and risk of dementia in two million people over two decades: A retrospective cohort study. Lancet Diabetes Endocrinol. 2015, 3, 431–436. [Google Scholar] [PubMed]
Figure 1. Sample flowchart of participants attending the China Health and Nutrition Survey.
Figure 1. Sample flowchart of participants attending the China Health and Nutrition Survey.
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Figure 2. Interaction between selenium intake and BMI in relation to cognitive function score. Values are means (95% CI) derived by using the margins command in Stata after running a mixed linear model adjusted for age, gender, intake of energy and fat, education, urbanicity, smoking, alcohol drinking, physical activity, and fruit and vegetable intake. p for interaction between selenium intake and BMI was 0.002. An ordinal value (1, 2, 3, 4) was assigned to reflect the quartiles of selenium intake level. Q, quartile.
Figure 2. Interaction between selenium intake and BMI in relation to cognitive function score. Values are means (95% CI) derived by using the margins command in Stata after running a mixed linear model adjusted for age, gender, intake of energy and fat, education, urbanicity, smoking, alcohol drinking, physical activity, and fruit and vegetable intake. p for interaction between selenium intake and BMI was 0.002. An ordinal value (1, 2, 3, 4) was assigned to reflect the quartiles of selenium intake level. Q, quartile.
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Table 1. Sample characteristics of Chinese adults aged ≥55 years old attending the first cognitive function test by quartiles of cumulative selenium intake (n = 4661).
Table 1. Sample characteristics of Chinese adults aged ≥55 years old attending the first cognitive function test by quartiles of cumulative selenium intake (n = 4661).
Q1Q2Q3Q4p-Value
n = 1189n = 1095n = 1145n = 1232
Age (years)65.9 (8.6)63.7 (8.0)62.1 (7.0)62.0 (6.7)<0.001
Sex <0.001
  Men424 (35.7%)456 (41.6%)594 (51.9%)763 (61.9%)
  Women765 (64.3%)639 (58.4%)551 (48.1%)469 (38.1%)
Income <0.001
  Low509 (43.3%)355 (32.7%)323 (28.3%)276 (22.8%)
  Medium362 (30.8%)363 (33.4%)391 (34.3%)280 (23.2%)
  High304 (25.9%)369 (33.9%)427 (37.4%)652 (54.0%)
Education <0.001
  Low870 (85.9%)811 (80.9%)722 (67.9%)645 (57.1%)
  Medium80 (7.9%)112 (11.2%)206 (19.4%)225 (19.9%)
  High63 (6.2%)79 (7.9%)135 (12.7%)260 (23.0%)
Urbanization <0.001
  Low425 (35.7%)313 (28.6%)264 (23.1%)181 (14.7%)
  Medium355 (29.9%)326 (29.8%)320 (27.9%)297 (24.1%)
  High409 (34.4%)456 (41.6%)561 (49.0%)754 (61.2%)
Region <0.001
  North430 (39.9%)367 (36.4%)461 (45.6%)658 (59.3%)
  South647 (60.1%)640 (63.6%)551 (54.4%)451 (40.7%)
Smoking <0.001
  Non-smoker845 (71.5%)788 (72.2%)749 (65.5%)750 (60.9%)
  Ex-smoker45 (3.8%)38 (3.5%)38 (3.3%)49 (4.0%)
  Current smoker292 (24.7%)266 (24.4%)357 (31.2%)433 (35.1%)
Survey year <0.001
  1997611 (51.4%)527 (48.1%)486 (42.4%)428 (34.7%)
  2000189 (15.9%)183 (16.7%)180 (15.7%)245 (19.9%)
  2004271 (22.8%)239 (21.8%)282 (24.6%)314 (25.5%)
  2006118 (9.9%)146 (13.3%)197 (17.2%)245 (19.9%)
Alcohol drinking272 (23.4%)300 (27.8%)388 (34.7%)472 (38.8%)<0.001
Physical activity (MET)84.8 (100.4)96.3 (105.5)92.3 (101.2)78.9 (89.4)<0.001
BMI (kg/m2)22.2 (3.7)22.7 (3.6)23.3 (3.5)23.9 (3.4)<0.001
BMI ≥24 (kg/m2)293 (27.4%)339 (33.0%)426 (39.4%)543 (47.2%)<0.001
Energy intake (kcal/day)1771.0 (520.8)2025.6 (549.9)2169.3 (587.5)2393.8 (667.0)<0.001
Fat intake (g/day)51.2 (28.5)62.5 (35.7)69.0 (35.2)83.2 (38.9)<0.001
Protein intake (g/day)47.5 (14.8)59.2 (16.1)66.7 (18.7)80.2 (26.3)<0.001
Carbohydrate intake (g/day)277.2 (93.0)301.6 (98.2)313.3 (107.6)321.4 (118.0)<0.001
Iron intake (g/day)15.5 (7.0)19.0 (8.0)20.9 (9.5)25.1 (17.0)<0.001
Intake of fruit (g/day)13.1 (52.2)18.3 (83.8)21.6 (70.4)38.9 (100.9)<0.001
Intake of fresh vegetables (g/day)249.2 (179.9)270.3 (162.4)281.3 (186.7)298.2 (173.4)<0.001
Intake of meat (g/day)37.9 (49.5)65.0 (67.2)81.2 (77.6)111.1 (104.5)<0.001
Most recent selenium intake (mg/day)21.6 (8.1)31.8 (9.4)39.6 (12.6)62.5 (62.4)<0.001
Cumulative selenium intake (mg/day)22.3 (4.9)32.5 (2.2)40.3 (2.6)60.7 (22.9)<0.001
Hypertension406 (37.0%)332 (31.7%)389 (35.6%)439 (37.4%)0.023
Diabetes31 (2.7%)29 (2.7%)32 (2.9%)57 (4.7%)0.011
Stroke28 (2.4%)20 (0.9%)19 (1.7%)33 (2.7%)0.29
Poor memory350 (29.7%)223 (20.7%)210 (18.4%)181 (14.8%)<0.001
Memory decline574 (49.3%)446 (42.4%)397 (35.7%)362 (30.2%)<0.001
Global cognitive function score <7320 (26.9%)215 (19.6%)152 (13.3%)150 (12.2%)<0.001
Data are presented as mean (SD) for continuous measures, and n (%) for categorical measures.
Table 2. Association between quartiles of selenium intake and cognitive function among Chinese adults aged 55 years and above attending the China Health and Nutrition Survey (n = 4852).
Table 2. Association between quartiles of selenium intake and cognitive function among Chinese adults aged 55 years and above attending the China Health and Nutrition Survey (n = 4852).
Quartiles of Selenium Intakep-Value
Q1Q2Q3Q4
Global cognitive function
Model 10.000.80(0.45–1.15)1.35(0.98–1.73)1.80(1.41–2.20)0.000
Model 20.000.32(−0.06–0.69)0.44(0.05–0.84)0.46(0.03–0.88)0.037
Model 30.000.32(−0.05–0.69)0.44(0.05–0.83)0.45(0.02–0.87)0.044
Model 40.000.28(−0.10–0.67)0.37(−0.03–0.78)0.42(−0.02–0.85)0.075
Model 50.000.27(−0.14–0.68)0.29(−0.15–0.72)0.48(0.01–0.95)0.074
Model 60.000.29(−0.12–0.70)0.26(−0.18–0.70)0.50(0.02–0.97)0.071
Values are regression coefficients (95% CI) from mixed-effect linear regression. Model 1 adjusted for age, gender, and energy intake. Model 2 further adjusted for intake of fat, smoking, alcohol drinking, income (low, medium, and high), urbanicity (low, medium, and high), education (low, medium, and high), and physical activity level (continuous). Model 3 further adjusted for fruit and vegetable intake (continuous). Model 4 further adjusted for BMI and hypertension. Model 5 further excluded those who only participated in one wave of the cognitive function tests. Model 6 further adjusted for self-reported diabetes and stroke. All the adjusted variables are treated as time-varying covariates (except gender).
Table 3. Odds ratios (95% CI) for self-reported poor memory and self-reported memory decline by quartiles of selenium intake among Chinese adults aged ≥55 years in the China Health and Nutrition Survey (n = 4852).
Table 3. Odds ratios (95% CI) for self-reported poor memory and self-reported memory decline by quartiles of selenium intake among Chinese adults aged ≥55 years in the China Health and Nutrition Survey (n = 4852).
Quartiles of Selenium Intake
Q1Q2Q3Q4p for Trend
Self-reported poor memory
Model 11.000.73(0.63–0.85)0.65(0.55–0.76)0.53(0.45–0.62)<0.001
Model 21.000.80(0.68–0.94)0.75(0.63–0.90)0.68(0.56–0.83)<0.001
Model 31.000.80(0.68–0.94)0.75(0.63–0.89)0.67(0.55–0.81)<0.001
Model 41.000.80(0.68–0.95)0.78(0.65–0.94)0.67(0.55–0.83)0.001
Model 51.000.81(0.68–0.98)0.76(0.62–0.92)0.68(0.55–0.85)0.001
Model 61.000.80(0.67–0.96)0.75(0.61–0.91)0.68(0.54–0.84)0.001
Self-reported memory decline
Model 11.000.80(0.67–0.96)0.75(0.61–0.91)0.68(0.54–0.84)<0.001
Model 21.000.82(0.72–0.93)0.65(0.57–0.74)0.51(0.45–0.59)<0.001
Model 31.000.88(0.76–1.02)0.74(0.64–0.87)0.66(0.56–0.78)<0.001
Model 41.000.88(0.76–1.02)0.74(0.64–0.87)0.66(0.56–0.78)<0.001
Model 51.000.88(0.75–1.02)0.74(0.63–0.87)0.65(0.54–0.77)<0.001
Model 61.000.85(0.73–1.01)0.71(0.60–0.85)0.65(0.54–0.78)<0.001
Model 1 adjusted for age, gender, and energy intake. Model 2 further adjusted for intake of fat, smoking, alcohol drinking, income, urbanicity, education, and physical activity. Model 3 further adjusted for overall dietary patterns. Model 4 further adjusted for BMI and hypertension. Model 5 further excluded those who only participated in one wave of the cognitive function tests. Model 6 further adjusted for self-reported diabetes and stroke. All the adjusted variables are treated as time-varying covariates (except gender).
Table 4. ORs (95% CIs) for global cognitive scores < 7 across quartiles of selenium intake among Chinese adults aged ≥55 y by sample characteristics: China Health and Nutrition Survey (n = 4852).
Table 4. ORs (95% CIs) for global cognitive scores < 7 across quartiles of selenium intake among Chinese adults aged ≥55 y by sample characteristics: China Health and Nutrition Survey (n = 4852).
Quartiles of Selenium Intake
Q1Q2Q3Q4p Trendp for Interaction
All1.000.76(0.63–0.92)0.70(0.57–0.87)0.69(0.54–0.87)0.001
Income 0.469
  Low1.000.66(0.50–0.89)0.64(0.46–0.90)0.48(0.32–0.71)0.000
  Medium1.000.87(0.63–1.20)0.69(0.49–0.99)0.77(0.51–1.17)0.087
  High1.000.85(0.56–1.30)0.82(0.52–1.29)0.96(0.61–1.52)0.930
Overweight 0.012
  No1.000.69(0.55–0.86)0.60(0.47–0.78)0.52(0.39–0.71)0.000
  Yes1.001.03(0.72–1.47)1.02(0.71–1.46)1.16(0.79–1.71)0.481
Hypertension 0.680
  No1.000.80(0.64–1.00)0.67(0.52–0.87)0.70(0.52–0.93)0.003
  Yes1.000.68(0.49–0.94)0.76(0.54–1.07)0.65(0.44–0.96)0.049
sex 0.513
  Men1.000.90(0.63–1.28)0.69(0.48–1.00)0.67(0.45–0.98)0.019
  Women1.000.70(0.56–0.88)0.71(0.54–0.92)0.72(0.53–0.98)0.016
Urbanization 0.439
  Low1.000.66(0.47–0.93)0.66(0.44–0.99)0.62(0.38–1.03)0.022
  Medium1.000.91(0.64–1.29)0.93(0.63–1.38)0.65(0.41–1.02)0.108
  High1.000.75(0.55–1.02)0.60(0.43–0.85)0.74(0.52–1.06)0.064
Region 0.005
  North1.000.90(0.61–1.33)0.79(0.53–1.17)1.26(0.84–1.90)0.385
  South1.000.70(0.55–0.89)0.66(0.50–0.88)0.50(0.35–0.72)0.000
Values are odds ratios (95% CI) from mixed-effect logistic regression. Mixed-effect logistic modes adjusted for age, gender, intake of energy and fat, smoking, alcohol drinking, income, urbanicity, education, physical activity, intake of fruits and vegetables, BMI, and hypertension. Stratification variables were not adjusted in the corresponding models. Income was categorized into low, medium, and high on the basis of tertiles of year-specific income.
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Jiang, K.; Xie, C.; Li, Z.; Zeng, H.; Zhao, Y.; Shi, Z. Selenium Intake and its Interaction with Iron Intake Are Associated with Cognitive Functions in Chinese Adults: A Longitudinal Study. Nutrients 2022, 14, 3005. https://doi.org/10.3390/nu14153005

AMA Style

Jiang K, Xie C, Li Z, Zeng H, Zhao Y, Shi Z. Selenium Intake and its Interaction with Iron Intake Are Associated with Cognitive Functions in Chinese Adults: A Longitudinal Study. Nutrients. 2022; 14(15):3005. https://doi.org/10.3390/nu14153005

Chicago/Turabian Style

Jiang, Ke, Changxiao Xie, Zhourong Li, Huan Zeng, Yong Zhao, and Zumin Shi. 2022. "Selenium Intake and its Interaction with Iron Intake Are Associated with Cognitive Functions in Chinese Adults: A Longitudinal Study" Nutrients 14, no. 15: 3005. https://doi.org/10.3390/nu14153005

APA Style

Jiang, K., Xie, C., Li, Z., Zeng, H., Zhao, Y., & Shi, Z. (2022). Selenium Intake and its Interaction with Iron Intake Are Associated with Cognitive Functions in Chinese Adults: A Longitudinal Study. Nutrients, 14(15), 3005. https://doi.org/10.3390/nu14153005

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