Sugar-sweetened beverages increases the risk of hypertension among children and adolescence: a systematic review and dose–response meta-analysis

A systematic search using PubMed, Scopus, Embase and Cochrane electronic databases was performed to find the studies evaluated the association between sugar-sweetened beverages intake and hypertension up to 1 April 2020. No language and time restrictions were applied. Moreover, hand-searching from reference lists of all relevant papers, previous reviews and meta-analyses was performed to cover all relevant publications. Strategy search was created using a combination of the MeSH (Medical Subject Headings) terms from the PubMed database and free text words.

For the search purpose, we used MeSH (Medical Subject Heading) and non-MeSH keywords including the following: (“Child”[Mesh]) OR child[Title/Abstract]) OR childhood[Title/Abstract]) OR pediatric*[Title/Abstract]) OR adolescen*[Title/Abstract]) OR youth[Title/Abstract]) OR teenager[Title/Abstract]) OR children)) AND ((SSB[Title/Abstract]) OR Sugar-Sweetened Beverage*[Title/Abstract])) AND ((((((((“Hypertension”[Mesh]) OR hypertension[Title/Abstract]) OR HTN[Title/Abstract]) OR blood pressure [Title/Abstract]) OR systolic blood pressure[Title/Abstract]) OR diastolic blood pressure [Title/Abstract]) OR SBP [Title/Abstract]) OR DBP[Title/Abstract]) (Additional file 1: Table S2). The reviewed literatures were inserted into the EndNote software (version X8, for Windows, Thomson Reuters, Philadelphia, PA, USA). For each electronic database, search strategy was adopted.

In the current systematic review and meta-analysis, observational studies with the design of cross-sectional, case control or cohort evaluating the association between sugar-sweetened beverages (SSB) and hypertension (HTN), systolic blood pressure (SBP) and diastolic blood pressure (DBP) were included. The studies were included if they were (a) observational studies (b) original research as publication type; (c) reported SSB (sodas/soft drinks, carbonated beverages, non-100% fruit juice drinks, syrup-based drinks, flavored water with sugar, sports and energy drinks, chocolate milk, yogurt drinks, lemonades, Coca-Cola, Sprite, orange juice, Nutrition Express, and Red Bull and sweetened teas) intake as exposure and HTN, SBP and DBP as outcome variable; and (d) studies conducted in children and adolescents (less than 19 years of age) (e) if they reported the mean ± standard deviation (SD) of SBP or DBP or the odds ratio (OR) of HTN in subjects of the highest versus lowest SSBs category. Since there is no official definition for SSBs, they were defined as any type of above- mentioned drinks. Initially, retrieved citations were merged, duplications were eliminated and the review process was facilitated. Accordingly, the titles and abstracts of all articles were evaluated independently by 2 reviewers (MAF, LN). Full-texts of relevant articles were retrieved if meeting the eligibility criteria, and then were re-evaluated. Any disagreements were discussed and resolved by consensus.

The quality of cross-sectional studies was assessed by Agency for Healthcare Research and Quality (AHRQ) checklist [30]. There was no quality criteria for inclusion of the studies in the current meta-analysis. The items were scored “1” if the answer was “YES,” and “0” if the answer was “NO” or “UNCLEAR.” The final quality assessments scores were as follows: low quality = 0–3; moderate quality = 4–7; high quality ≥ 8. The details of the studies’ quality assessment are presented in Additional file 1: Table S3.

Data were collected according to a standard data extraction form. The following information was extracted from each study: (1) authors name; (2) publication year; (3) country of study; (4) study design; (5) age range and/or mean; (6) participants’ gender; (7) number of case and controls; (8) dietary assessment tool; (9) setting; (10) type and quantity of SSB; (11) covariates used in adjustment; (12) outcome values.

Our search strategy identified 1661 potentially relevant articles. Thereafter 857 manuscripts were remained for full text screening after removing duplicates and exclusion according to the title and abstract reading. Totally, 671 manuscripts were excluded because of their irrelevant subject, inappropriate design, being reviews including meta-analysis or systematic reviews, conferences and seminars, not relevant age groups, not evaluating the association of studied parameters. A final number of 14 manuscripts were included in the current meta-analysis (Fig. 1).

The characteristics of included studies are presented in Table 1. A total of 14 studies with 93,873 participants were included in the current meta-analysis [8‐11, 13, 15, 19, 23, 24, 26, 27, 37‐39]. The studies had been performed between 2009 and 2020. Totally, eleven studies reported higher SBP in higher SSB intake categories versus lower consumers [8, 10, 11, 13, 15, 19, 23, 24, 37‐39]; similarly, DBP was higher among high SSB consumers compared with low consumers in six studies [10, 11, 15, 23, 24, 38]. Two studies reported no significant difference between SBP and DBP of different SSB categories [26, 27]. Four studies reported the odds of hypertension in higher SSB consumers compared with lower consumers [9, 13, 23, 24]. Different kinds of sugar-sweetened beverages were included in the self-reported SSB intake questionnaires form including: sugar sweetened sodas, carbonated beverages, caloric and sport drinks, lemonades, yogurt drinks, sweetened teas, non-100% fruit juices, cordials and other types. The age range was from 5 to 22 years old while most of the studies were performed in apparently healthy children and adolescents [8‐11, 13, 15, 19, 23, 24, 27, 38, 39] and one study was performed in children with T₁DM [26] and one in severe obesity [37]. The setting of the studies was community [8, 11, 15, 23, 39], school [9, 10, 13, 24, 27, 38], home [19] and clinic [26, 37]. The study by Chan TF et al. [13] that was conducted in two genders separately and the study by DeBoer EC et al. [19] that was performed in two age groups (5–6 years and 11–12 years) were included as two separate studies. The geographical locations of the studies were Australia [8], USA [19, 26, 39], Iran [15], Norway [37], China [9, 11, 23, 24], Brazil [10], Taiwan [13, 38] and Malaysia [27]. Almost all of the studies were cross sectional [9‐11, 13, 23, 24, 26, 27, 37‐39] and in three cohort studies the cross-sectional baseline data was used [8, 15, 19].

The results of the comparison of SBP and DBP between highest versus lowest SSB consumption categories have been presented in Figs. 2 and 3. As presented, high SSB consumption was associated with 1.67 mmHg increase in SBP in children and adolescents (WMD: 1.67; CI 1.021–2.321; P < 0.001). While, the change in DBP was not significant (WMD: 0.313; CI −0.131, 0.757; P = 0.108). Odds of hypertension in highest versus lowest SSB consumers has been shown in Fig. 4. High SSB consumers were 1.36 times more likely to develop hypertension compared with low SSB consumers (OR: 1.365; CI 1.145–1.626; P = 0.001). A significant between study heterogeneity was observed for studies that had evaluated SBP (I² = 99.8; P < 0.001) and for DBP (I² = 99.4; P < 0.001). However, there was no heterogeneity for the studies that had evaluated the odds of hypertension (I² = 0.0; P = 0.976). For finding the source of heterogeneity, we performed subgroup analysis and the results are shown in Additional file 1: . Tables S4 and S5. As shown in these tables, subgrouping according to setting, baseline value of SBP, health status, region, gender and study quality reduced the heterogeneity for studies that evaluated the SBP values. While for DBP, the SSB dosage, setting, region, sample size, baseline DBP values, study quality, gender and design reduced the heterogeneity. Moreover, Subgroup analyses showed that a higher SSB consumption lead to a higher SBP among children and adolescents with baseline SBP greater than 110 mmHg (WMD: 0.743; CI 1.330–4.157; P < 0.001). Additionally, SSB intake might increase SBP in the studies with a sample size > 2000 (WMD: 2.720; CI 2.581–2.859; P < 0.001), school based studies (WMD: 2.780; CI 2.727–2.832; P < 0.001). Higher SSB intake also resulted in greater increase in SBP among apparently healthy subjects (WMD: WMD: 1.848; CI 0.888–2.808; P < 0.001). Accordingly, the subgrouping revealed that the high SSB intake is associated with high DBP in school based studies (WMD: 1.76; CI 1.431–2.089; P < 0.001), studies with high baseline DBP values (WMD: 0.494; CI 0.001–0.987; P = 0.049), performed in apparently healthy children or adolescents (WMD: 0.476; CI 0.023– 0.929; P = 0.039), studies with sample size greater than 2000 (WMD: 0.957; CI 0.531–1.384; P < 0.001) and studies that performed in Asia (WMD: 0.542; CI 0.024–1.060; P = 0.04).

The details of dose–response meta-analysis are shown in Table 2 and the results for the SBP and DBP are presented in Figs. 5 and 6, respectively. According to the results of dose–response meta-analysis, no evidence of departure from linearity was observed for the association between dose of SSB with mean change in SBP (P-nonlinearity = 0.707) or DBP (P-nonlinearity = 0.180).

The funnel plots are presented in Additional file 1: Figure S1a, b, c. No evidence of publication bias was observed neither for the meta-analysis of the comparison of SBP or DBP in highest versus lowest SSB categories according to Begg’s and Egger’s meta-bias tests [SBP: Begg test (P = 0.547) and Egger test (P = 0.267); DBP: Begg test (P = 0.115) and Egger test (P = 0.592)], nor for the meta-analysis of the association of hypertension with SSB intake [e.g. Begg test (P = 0.327) and Egger test (P = 0.127)].