Study protocol: associations between dietary patterns, cognitive function and metabolic syndrome in older adults – a cross-sectional study

The participants in this cross-sectional study will be men and women aged 65–74 years, living independently in Auckland, New Zealand and proficient in English. Participants will be excluded if they are colour blind (due to the computerised cognitive testing requiring colour recognition); have a diagnosis of dementia or any of the following conditions which may impair cognitive function: stroke, traumatic head or brain injury, a neurological or psychiatric condition; or if they are taking medication which may influence their cognitive function. Another exclusion criterion is any event in the last 2 years which had a substantial impact on dietary intake and cognitive function, for example, death or illness of a family member.

A sample size of 350 participants is required to see a medium size effect (Pearson correlation 0.3) with 80% power for the main outcome of a linear association between the cognitive scales and dietary patterns. This sample size is similar to other studies investigating cognitive function and dietary patterns [36]. Data will be collected from 360 participants to allow for missing or incomplete data.

Recruitment and data collection will commence in 2018 and is expected to take 12 months. Participants will be required to attend the Human Nutrition Research Unit, Massey University, Auckland, New Zealand on one occasion. Informed consent forms will be completed at the research facility prior to data collection. The research day involves collecting health and demographic data, blood pressure, anthropometric and physical activity data as per Table 1. A fasted blood sample will be taken prior to a standardised breakfast. Two cognitive assessments will be completed after breakfast. An online food frequency questionnaire (FFQ) and a food diary information video complete the session.

Funding is provided by the Health Research Council of New Zealand, Grant 17/566. Ethical approval has been granted by Massey University Human Ethics Committee: Southern A, Application 17/69.

Participants will be recruited throughout the wider Auckland region via several channels including: the Human Nutrition Research Unit, Massey University participant database; media, including radio interviews and press releases from Massey University; posters and flyers at local libraries, community centres, recreation centres, sports and hobby clubs, Citizens Advice Bureaus, retirement villages and second hand shops; inclusion in relevant newsletters, e.g. Age Concern New Zealand; and online promotion on appropriate social media pages e.g. GrownUps, Office for Seniors Facebook page. The REACH study will have a website where potential participants will be directed for further information and to register interest [48]. Only one person per household will be eligible to participate in the study. Participants expressing an interest in the study will be provided with an information sheet and undergo a screening interview [48], via telephone, to ensure inclusion criteria are met.

Health, demographics, lifestyle and physical activity information will be collected through written questionnaires in person (Table 1). Data quality will be ensured by checking questionnaires for completeness and sensibility. If further clarification is required, it will be done immediately or within a few days by phone or email. Socio-demographic information includes age, gender, ethnicity, marital status, education, household income, work history, living situation and food security. Health information will include past and current disease (acute and chronic), medication, family history of dementia or cognitive impairment, vision, hearing, dental health and mobility issues. Lifestyle information will include smoking history, alcohol intake, substance abuse, supplement use and changes in physical activity. Dietary information will include changes in diet over past 10 years and possible factors behind these changes e.g., dentition, health concerns, disposable income, appetite. An Index of Multiple Deprivation will be calculated from the residential address of participants [49].

Anthropometry, including body fat percentage, BMI, hip and waist circumference, and blood pressure will be measured as in Table 1.

Blood pressure will be measured twice. Participants will rest quietly (seated) for 5 min before the first measurement is taken. There will be a 1-min rest period between measurements. If either systolic or diastolic measurements differ by more than 5 mmHg between measurements, a third measurement will be taken.

For consistency, all participants will be fasted (except water) from 2200 h the night prior to their visit. Between 0700 and 0900 at the research facility, a qualified phlebotomist will draw fasted blood samples in the following order: 10 ml BD Vacutainer® Plus (cat 367895), 10 ml BD Vacutainer® K2EDTA (cat 367525) and 6 ml BD Vacutainer® K2EDTA (cat 367873). The 10 ml BD Vacutainer® Plus will be maintained at an ambient temperature for 30 min to allow clotting, then will be centrifuged with the 10 ml BD Vacutainer® K2EDTA (Heraeus Labofuge 400R) for 15 min at 1547 g-force (3500 rpm) at 4 °C. The resulting serum, from the 10 ml BD Vacutainer® Plus, will be aliquoted into four Eppendorf tubes which will be stored for further measures. The resulting plasma, from the 10 ml BD Vacutainer K2EDTA, will be aliquoted into six Eppendorf tubes and stored for further research. The 6 ml EDTA vacutainer will be placed on ice and tested for blood glucose, HbA1c and a lipid profile using point-of-care equipment (Table 1). The remaining blood (~ 5 ml) will be stored for ApoE ε4 analysis (Table 1) by an accredited laboratory, and two Eppendorf tubes (500 μl) will be kept for backup. All samples will be stored at -80 °C.

The study spans a 10-month period from autumn to summer. Dietary data will be collected using two methods. First, a self-administered 109-item FFQ will collect data, covering the previous month, via an online survey on two occasions: at the research facility (FFQ1) and 1 month later (at home) (FFQ2) to assess reproducibility. The FFQ is adapted from a validated New Zealand FFQ aimed at assessing iron related dietary patterns in young women [46]. Changes included the addition of serving sizes; combining some food groups to shorten the questionnaire; the addition of foods not included in the initial nutrient specific FFQ e.g. confectionary; as well as extra questions for added clarification e.g. type of milk or oils used. The FFQ was further cross-checked with the New Zealand Women’s Food Frequency Questionnaire [50, 51] to ensure all relevant food groups were included. Ten individuals in the study age range pre-tested the FFQ for understanding and readability. The completed FFQ will be entered into Foodworks 9 (Xyris Software, 2017), which uses the New Zealand FOODfiles⁽™⁾ 2016 [52] food composition database. After data entry and inspection, any necessary adjustments will be made e.g. Goldberg Cut-off for energy intake [53].

Second, an estimated 4-day food diary will be collected from a subset of participants to validate the modified FFQ for food and dietary patterns. Participants will complete the 4-day food diary within 1 month of the study visit. The 4-day food diary covers four consecutive days including at least one weekend day. Prior to completing the 4-day food diary, participants will view an instructional video which explains the need to record all foods and beverages consumed including type, brands, and cooking methods. Participants will be taught how to estimate quantities using pictures [54], household measures, and measuring scales. The 4-day food diary will be processed by four trained nutritionists using Foodworks 9 (Xyris Software, 2017). A register of common food items will be kept ensuring consistency in data entry among the four nutritionists. Additionally, every tenth food record entered will be audited for accuracy and consistency.

Cognitive testing will be carried out after a standardised breakfast to minimise any effects food may have on cognition. The cognitive testing will be undertaken in two parts. First, a trained examiner will administer the Montreal Cognitive Assessment (MoCA) on a one to one basis. MoCA is a clinically available and validated [47] tool. It takes 10 min, assesses global cognitive function, short-term memory, visuospatial and executive function, attention, language and orientation, concentration and working memory [47]. MoCA will be used to provide comparisons with other studies, and as a descriptor.

The second part will be the Computerised Mental Performance Assessment System (COMPASS-Northumbria University, Newcastle upon Tyne, UK). This software platform presents tasks on desktop computers using a variety of methods to collect responses: mouse and cursor, a four-button coloured response pad, and pen and paper for word recall. This broad battery of tests assesses all cognitive domains (Table 2) and is sensitive to normal age-related effects and dietary factors [55, 56].

The reaction time for correct responses will be assessed and participants will be assigned a composite score for global cognitive function and for each cognitive domain.

Cognitive testing will be undertaken in a cognitive suite controlled for environmental factors e.g. noise and temperature. The tests will be taken at a similar time of day and participants will be instructed to avoid undue stress, alcohol, recreational drugs and physical activity that is not routine prior to their appointment. Testing will take approximately 1 h. The first 15 min will be training. The investigator will verbally describe the tasks, the format of the testing, and use of the response pad, and will answer any questions. The practice tests will be shorter and easier versions of the actual test. Participants will have a 5-min break before actual assessment is undertaken. The investigator will ensure any new computer users are comfortable with using a mouse before testing starts.

To determine the incidence of metabolic syndrome the criteria recommended by the American Heart Association/National Health, Lung and Blood Institute Scientific Statement will be followed [57]. Metabolic syndrome will be considered to exist where three of the following five criteria are met or medication is used to treat: waist circumference ≥ 88 cm for women and ≥ 102 cm for men; a triglyceride level of ≥1.7 mmol/L; HDL cholesterol level of < 1.03 mmol/L in men or < 1.3 mmol/L in women; blood pressure ≥ 130/85 mmHg; fasting blood glucose ≥5.6 mmol/L.

Feedback to participants after assessment will include anthropometric measurements (height, weight, BMI, waist and hip circumference, body fat %), blood pressure and blood results (HbA1c, fasting blood glucose, lipid profile). A registered (NZ Medical Council) general practitioner will review all biochemical results prior to communicating them to participants. On completion of the study, participants will receive a report summarising the main findings of the REACH study.

Statistical analysis will be performed using R [58]. Participant data will be described using mean (95% confidence intervals) for normally distributed data, median (25, 75 percentile) for non-normally distributed data, or frequency summary statistics for categorical data. The Shapiro-Wilk test and normality plot will evaluate the normality of distributions.

Dietary patterns will be identified using rotated principal component analysis, a statistical technique to reduce data and produce patterns based on the correlations between food groups [23]. The FFQ food group items will be further collapsed based on other studies investigating dietary patterns [40, 41]. Three separate analyses will be performed: FFQ1 to determine dietary patterns, the 4-day food diary to assess validity of the dietary patterns identified in FFQ1, and FFQ2 vs FFQ1 to assess reproducibility. Orthogonal varimax rotation will be used to facilitate interpretability of components. The number of components retained will be based on the scree plot, eigenvalue (> 1), and interpretability of the dietary pattern. The Kaiser-Meyer-Olkin measure of sampling adequacy and Bartlett’s Test P values (to determine the presence of relationships between variables in the factor analysis) will be examined [59]. Labelling of dietary patterns will be based on the interpretation of foods with high factor loadings for each dietary pattern [60].

Multivariate multiple regression analysis [61] will be used to determine the association between dietary patterns and various domains of cognitive function (dependent variable) while considering confounding factors. Possible confounding and interaction factors include: age, gender, ethnicity, education, English as a second language, presence of chronic disease (including metabolic syndrome), socio-economic status, physical activity, body mass index, ApoE ε4 genotype, family history of dementia, smoking, alcohol intake and past dietary intake.

Further analysis will compare dietary patterns of participants with and without metabolic syndrome using multiple logistic regression analysis.