Study design and sample

Among 11 673 Japanese people who underwent their annual health checkups between April 2019 and March 2020 at the Health Planning Center of Nihon University Hospital, located in the centre of Tokyo, we included 8947 apparently healthy participants in this study.

The exclusion criteria were as follows: unwilling to provide consent for participation in the study; positive history of ASCVD; treatment for psychiatric disorders, liver disease, kidney disease and lung disease; current intake of lipid-modifying, antihypertensive, antidiabetic and antihyperuricemic drugs; serum TAG level ≥ 400 mg/dl or absence of data on the frequency of fish consumption and leucocytes count; and blood leucocytes count ≥9000 cells/μl, suggesting the presence of a potentially infectious condition. Fig. 1 shows the flow diagram for the selection of study participants. This study is a sub-analysis of our previous study^{(Reference Tani, Imatake and Suzuki16)}.

Fig. 1. Flow diagram of participant selection. ASCVD, atherosclerotic CVD.

This study complied with the Declaration of Helsinki. The study design and objectives were approved by the Institutional Review Board of Nihon University Hospital (approval number: 20200405). The requirement for written informed consent was waived because this was a retrospective cross-sectional study, and an opt-out recruitment procedure was followed. The study was also registered with UMIN (http://www.umin.ac.jp/) Study ID: UMIN 000 043 206.

Questionnaire on health behaviours

Trained interviewers conducted health behaviour surveys via face-to-face interviews with the participants at our institute. The surveys comprised comprehensive questions to assess the participants’ demographic and socio-economic characteristics, such as age, occupation, marital status, lifestyle behaviours, medication and family history. The individuals undergoing health checkups were administered a lifestyle questionnaire. The questions listed below are similar to the ones used in our previous studies^{(Reference Tani, Imatake and Suzuki17)}.

1. 1. Smoking habit: Do you smoke habitually?: No/Yes/I have quit smoking/I quit smoking () years ago.

2. 2. Drinking habit: Please specify the frequency of your drinking: Every day/sometimes/I used to drink previously, but have stopped drinking/I stopped drinking () years ago/I drink rarely/I cannot drink; How much do you drink per d when you drink? (ethanol equivalent (g/d)): <20 g/20 to <40 g/40 to <60 g/≥60 g; How many days per week do you drink?^{(Reference Tani, Imatake and Suzuki17)}

3. 3. Aerobic exercise habit: Have you engaged in an exercise that makes you sweat slightly for ≥30 min a day, at least twice a week for ≥1 year?

4. 4. Intensive physical activity: Do you walk or engage in similar physical activity for 1 h or more per d in daily life?

5. 5. Sleep habit: How many hours a day, on average, do you sleep?

6. 6. Fish consumption: How many days in a week, on average, have you eaten fish in the past 1 month?

Fish consumption was assessed in weekly frequency in the questionnaire (not at all, once, twice, three times, four times, five times, or six times a week, or approximately every day). The questionnaire is a modified version of the Questionnaire on Specific Health Examination, used for specific health guidance after health checkups under the jurisdiction of the Ministry of Health, Labour and Welfare (MHLW) of Japan⁽¹⁸⁾. The questions listed above are part of a questionnaire that is relevant to this study (online Supplementary Table 1). Furthermore, based on this questionnaire, we excluded participants who met the exclusion criteria at the screening stage (i.e. history of the disease, the disease is being treated, and presence or absence of medications) to determine eligibility for participation in the study.

Assessment of the estimated weekly average amount of fish consumption

The National Health and Nutrition Survey of Japan estimated the average daily amount of fish consumption according to age group by estimating the ‘net food supply per person per year of fishery products for human consumption’ based on domestic fish production, imports and exports, changes in stocks, and population among others. These data were obtained from the survey conducted by the MHLW of Japan (online Supplementary Table 2)^(19,20) . Based on this survey record, we calculated the estimated average weekly amount of fish consumption as follows:

$$\matrix{ {{\rm{he}}\;{\rm{estimated}}\;{\rm{average}}\;{\rm{weekly}}\;{\rm{amount}}\;{\rm{of}}\;{\rm{fish}}\;{\rm{intake}}} \hfill\cr {\; = \;{\rm{average}}\;{\rm{daily}}\;{\rm{amount}}\;{\rm{of}}\;{\rm{fish}}\;{\rm{consumption}}\;{\rm{according}}\;{\rm{to}}\;{\rm{age}}} \hfill\cr {\; \times \;{\rm{average}}\;{\rm{weekly}}\;{\rm{number}}\;{\rm{of}}\;{\rm{days}}\;{\rm{of}}\;{\rm{fish}}\;{\rm{consumption}}} \hfill\cr } $$

Accordingly, we divided the average weekly amount of fish consumption into seven categorical variables: (1) <50 g/week; (2) ≥50 g/week but <100 g/week; (3) ≥100 g/week but <150 g/week; (4) ≥150 g/week but <200 g/week; (5) ≥200 g/week but <250 g/week; (6) ≥250 g/week but <300 g/week and (7) ≥300 g/week. We have already proven the validity of the estimated fish intake formula in our previous study^{(Reference Tani, Imatake and Suzuki16)}.

Health examinations and blood samples

We measured the anthropometric variables (i.e. height, weight and waist circumference) of the participants in the standing position, using standardised techniques and equipment. We calculated the BMI by dividing the body weight (kg) by height squared (kg/m²) and the waist circumference, using a non-stretchable tape around the participants’ umbilicus in the late exhalation phase^{(Reference Tokunaga, Matsuzawa and Ishikawa21)}. We measured the blood pressure twice, with a 3-min interval between the two measurements, using a standard mercury sphygmomanometer after a 5-min rest period; we used the average of the first and second measurements for our assessment. Fasting blood samples were collected early in the morning after the participants had fasted for 8 h. The leucocytes count was determined using a Beckman Coulter STKS (Beckman Coulter, Fullerton, CA). The serum C-reactive protein level was measured by a nephelometric assay (Behring Diagnostic). The estimated glomerular filtration rate was calculated using the abbreviated MDRD (Modification of Diet in Renal Disease) study formula modified by a Japanese coefficient^{(Reference Matsuo, Imai and Horio22)}. The serum total cholesterol, TAG and HDL-cholesterol levels were measured using enzymatic methods. Furthermore, the Friedewald formula was used to estimate the serum level of LDL^{(Reference Niedbala, Schray and Foery23)}, and the serum level of non-HDL-cholesterol was calculated by subtracting the serum HDL-cholesterol from the serum total cholesterol. The Hb A1c value was measured by HPLC. Notably, the homoeostasis model assessment-insulin resistance (HOMA-IR), or the insulin resistance score, was calculated as fasting insulin level (mU/ml) × fasting blood glucose level (mg/dl)/405.

Statistical analysis

Data were expressed as means and standard deviation for continuous variables and as percentages for discrete variables concerning participant characteristics. For cases showing significantly skewed distribution, the data were expressed as the median and interquartile range (IQR). Through ANOVA, continuous variables were compared according to sleep duration as five categorical variables (<5 h, 5–6 h, 6–7 h, 7–8 h and ≥ 8 h). We used the Kruskal–Wallis test for non-parametric multigroup comparison. We subsequently performed a χ ² test to compare categorical variables. To investigate the overall relationship between fish consumption, sleep duration and leucocytes count, we examined four items as follows, multilaterally: (1) characteristics of study participants, including fish consumption according to sleep duration; (2) factors influencing sleep duration; (3) association of sleep duration and leucocytes count with fish consumption; and (4) relationship between sleep duration and leucocytes count. Furthermore, we performed a univariate linear regression analysis using sleep duration as the dependent variable, and participant characteristics, ASCVD risk factors, and lifestyle behaviours, including the weekly fish consumption, as independent variables. Determinants deemed significant via a univariate linear regression analysis with P < 0·05 were entered into the multivariate linear regression analysis model. Regression analysis was performed using linear regression and Spearman’s and Pearson’s correlation coefficients. We also performed univariate and multivariate linear regression analyses using the study participants’ leucocytes count as the independent variable and fish consumption and participant characteristics as the dependent variables. Habitual fish consumption is reported to be positively associated with healthy lifestyle behaviours (e.g. aerobic exercise and lack of a smoking habit)^{(Reference Tani, Matsuo and Imatake12,Reference Wennberg, Tornevi and Johansson13)} . Thus, two-way ANOVA (interaction test) was used to confirm the interaction between the amount of fish consumption and lifestyle behaviours, which were independent determinants of sleep duration in univariate and multivariate linear regression analysis. Similarly, to assess whether fish consumption and sleep duration interact with the leucocytes count, we performed a two-way ANOVA with leucocytes count as the independent variable and fish consumption and sleep duration as the dependent variables. We also performed Jonckheere–Terpstra and Mantel–Haenszel trend tests. All statistical analyses were performed using SPSS software (IBM) for Windows (version 24).