Study population

This is a cross-sectional study with 886 participants of the SUN project. The SUN cohort is a multipurpose, ongoing and dynamic cohort of Spanish university graduates started in December 1999, and it is permanently open. The design and methods used in the SUN project have been published in detail elsewhere^{(Reference Carlos, De La Fuente-Arrillaga and Bes-Rastrollo26)}. In brief, baseline and follow-up information are collected through postal or web-based questionnaire every 2 years. The study protocol was supported by the Institutional Review Board of the University of Navarra and registered at clinicaltrials.gov as NCT02669602.

Voluntary completion of the baseline epidemiological survey implied informed consent, as participants received detailed information about the whole study.

In May 2008, 1921 participants (>55 years old at baseline questionnaire) of the SUN project were invited to participate in a genetic sub-study^{(Reference Galbete, Contreras and Martínez27)}. Among them, 1085 participants accepted the invitation and received a kit to collect saliva, and 953 of them correctly returned saliva samples. In our analysis, we excluded sixty-seven participants because they were outside of Willett predefined limits for energy intake (<3347 or >16 736 kJ/d for men, and <2092 or >14 644 kJ/d for women)^{(Reference Willett28)}. Thus, the final available sample included 886 older adults (645 males and 241 females) (online Supplementary Fig. S1).

Dietary assessment

In our study, dietary intake was assessed at baseline with a semi-quantitative FFQ of 136 food items validated and re-evaluated^{(Reference De La Fuente-Arrillaga, Vázquez Ruiz and Bes-Rastrollo29,Reference Martin-Moreno, Boyle and Gorgojo30)} in Spain, which assessed food habits in the previous year. This questionnaire had the following nine possible response categories: never/almost never, 1–3/month, 1/week, 2–4/week, 5–6/week, 1/d, 2–3/d, 4–6/d and >6/d, and standard portion sizes were specified. Nutrient intake was calculated by multiplying the frequency of consumption by the nutrient content of the specified portion, using data from Spanish food composition tables^{(Reference Moreiras31,Reference Mataix32)} by a trained dietitian.

Telomere length assessment

Genomic DNA was extracted from each participant’s saliva samples collected in the kit Orange® DNA Self-Collection kit-OG250, according to the manufacturer’s instruction. DNA samples were stored at −80 ºC. A monochrome multiplex real-time quantitative PCR was used for TL measurements assay according to the method of Cawthon^{(Reference Cawthon33)}. In brief, telomere repeat amplification (T) is compared with a single copy gene product (S) in a single reaction well on clear, 384-well plates in a CFX384 Touch-Real-time PCR system (BioRad). Then, average TL is correlated with T/S ratio. PCR reactions were run adding 10 µl master mix containing QuantiTectSybr Green PCR kit (Qiagen); the primers (Sigma Aldrich; purified by HPLC) which sequences were telg (5′- ACACTAAGGTTTGGGTTTGGGTTTGGGTTTGGGTTAGTGT-3′), telc (5′- TGTTAGGTATCCCTATCCCTATCCCTATCCCTATCCCTAACA-3′), albu (5′- CGGCGGCGGGCGGCGCGGGCTGGGCGGAAATGCTGCACA-GAATCCTTG-3′) and albd (5′-GCCCGGCCCGCCGCGCCCGTCCC GCCGGAAAAGCATGGTCGCCTGTT-3′); followed by 2 µl of each experimental DNA samples (10 ng); nuclease-free water to complete the final volume. Final concentration of combined telomere primers (telc and telg) and albumin primers (albu and albd) was 900 nM each.

For quality control, each sample was run in triplicate. In addition, a seven-point standard curve made from reference DNA samples (point 1, 150 ng/ml; point 2, 75 ng/ml; point 3, 37·5 ng/ml; point 4, 18·75 ng/ml; point 5, 9·38 ng/ml; point 6, 4·69 ng/ml; point 7, 2·34 ng/µl) was included for each plate using a 2-fold dilution series of DNA ranging from 150 to 2·34 ng/ml. TL was expressed as a T:S ratio using the calibration curve (linearity agreement R ² > 0·99) to relative quantification.

Assessment of other variables

The baseline questionnaire collected information on socio-demographic (e.g. sex, age, college degree, employment status), anthropometric variables (e.g. BMI, weight change during the past 5 years) and health-related habits (e.g. smoking status, alcohol intake, special diets, time spent watching television and sitting, physical activity) and history of illnesses and medical conditions. BMI was calculated dividing self-reported weight by the square of self-reported height. Physical activity data (metabolic equivalents of task (MET) h/week) were reported from a previously validated questionnaire that answers the time spent on seventeen activities, multiplying by a multiple of the RMR (MET score) according to previously published guidelines^{(Reference Ainsworth, Haskell and Whitt34)}.

Assessment of dietary patterns

The 136 food items included in the FFQ were classified into thirty predefined candidate food groups.

The grouping scheme was based on the similarity of nutrients profile or culinary usage among the foods, and it was somewhat similar to that used in previous studies with participants of the SUN project^{(Reference Donazar-Ezcurra, Lopez-Del Burgo and Martinez-Gonzalez35,Reference Zazpe, Sánchez-Tainta and Toledo36)} .

The PCA was applied to these food groups in order to identify the major dietary patterns that could explain the maximum proportion of the variance from the original groups. Sampling adequacy was supported by Kaiser–Meyer–Olkin value > 0·6^{(Reference Kaiser37)}. The number of factors retained was based on eigenvalues >1, the inflexion point on the scree plot, interpretability and variance explanation of each pattern solution. Food groups which received absolute loadings factors ≥0·30 were considered relevant components of the dietary patterns (Table 1). Absolute values <0·30 are not listed in Table 1.

Table 1. Factor loadings for the two major dietary patterns (n 886)*

* The first factor (Western dietary pattern) and the second factor (Mediterranean dietary pattern) explained 8·4 and 6 % of the total variance, respectively. Dietary patterns are labelled on the basis of factor loadings with 0·3 or greater.

† |r| < 0·10.

‡ |r| ≥ 0·10 but ≤0·29.

Two factors were retained based on the factor loadings of the pre-selected candidate food groups, the first factor was named ‘Western dietary pattern (WDP)’ and the second factor was named ‘MDP’. Factor scores were calculated for each subject as the sum of standardised consumption of each food group weighted by the coefficient of each factor score. Then, WDP and MDP were categorised into quintiles. The second, third and fourth quintiles were grouped to simplify the results. Supplementary analyses of the main result were performed with ungrouped quintiles (online Supplementary Tables S1 and S2).

Statistical analysis

Sample size was estimated for the comparison between extreme quintiles, assuming a minimum of 150 subjects in each quintile (total 300 subjects in the comparison), with the aim of detecting a mean between-quintile difference (β-coefficient) of 0·03 in TL, assuming a sd of 0·08 for this difference. Under these assumptions, the statistical power will be 0·90 if a two-tailed α error = 0·05 is assumed.

Inverse probability weighting was used to evaluate age- and sex-adjusted baseline characteristics of participants distributed into quintiles of adherence to WDP and MDP (Table 2). We used percentages for categorical variables and means and standard deviations for continuous variables. TL variable was adjusted for age through the residual method^{(Reference Willett28)}.

Table 2. Baseline characteristics* of the 886 older adults of the Seguimiento Universidad de Navarra project according to quintiles (Q) of the Western and Mediterranean dietary patterns

(Percentages; mean values and standard deviations)

MET, metabolic equivalents of task.

* Age- and sex-adjusted baseline characteristics through inverse probability weighting except age and sex.

† To convert kcal to kJ, multiply by 4·184.

Generalised linear models were used to evaluate the associations between each of the four upper quintiles of adherence to each dietary pattern and TL in comparison with the lowest quintile. β-Coefficients and their 95 % CI were calculated to evaluate this association, and they represent the multivariable-adjusted differences between TL in each of the four upper quintiles and the lowest quintile (reference category).

We defined short telomeres as a residual TL below the 20th percentile^{(Reference Ojeda-Rodríguez, Zazpe and Alonso-Pedrero19,Reference Vera, Bernardes de Jesus and Foronda38)} . Logistic regression models were performed to assess the relationship between adherence to the four upper quintiles of each dietary pattern and the risk of having short telomeres, keeping the lowest quintile as the reference category.

In addition, tests of linear trend across successive quintiles were performed by assigning to each participant the value of the median in his/her quintile and considering these variables as continuous variables.

Potential confounders have been included as covariates: age, sex, year of cohort entry (four categories: 1999–2001, 2002–2004, 2005–2007, 2008), energy intake (continuous), BMI (≤20, 20–21, 22–25, ≥25 kg/m² and a quadratic term for BMI), smoking status (never/ever), alcohol intake (abstainer, <5 or <10 g/d, 5–25 g/d or 10–50 g/d, >25 g/d or >50 g/d for women and for men, respectively), leisure-time physical activity (MET task h/week, continuous), average daily time of television watching (h/d, continuous), average daily time spent sitting (h/week, continuous), following special diet at baseline (yes/no), weight gain in the past 5 years previous to entering the cohort (<3 kg/≥3 kg), years of education (continuous), prevalence of dyslipidaemia and CVD (yes/no), dietary fibre intake, MUFA intake, PUFA intake, SFA intake and trans-fat intake (continuous).

To evaluate the robustness of our results, several sensitivity analyses were conducted by rerunning all multiple linear models under different stratifications: sex, age at baseline (<75 /≥75 years old), BMI (≤25/>25 kg/m²) and smoking status (never smokers and former or current smokers). Likelihood ratio tests were used to calculated P values for interaction.

Finally, several sensitivity analyses were carried out to assess possible sources of bias in the estimation of the association between adherence to the WPS or the MPS and the TL. Thus, we repeated the analyses after including only men or only women, only health professionals or only non-health professionals, excluding participants with dyslipidaemia or CVD at baseline, using the 5th and 95th percentiles as allowed limit for total energy intake, excluding participants with special diet at baseline, excluding participants with nine or more missing values in the baseline FFQ and finally excluding ever smokers.

We used STATA 12.0 for Windows (version 12.0; StataCorp LP) for statistical analyses. The statistical significance level was P < 0·05.