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Associations of artificial sweetener intake with cardiometabolic disorders and mortality: a population-based study

Published online by Cambridge University Press:  18 October 2024

Jun-yan Kan
Affiliation:
Department of Cardiology, Nanjing First Hospital, Nanjing Medical University, Nanjing, People’s Republic of China
Dong-chen Wang
Affiliation:
Department of Cardiology, Nanjing First Hospital, Nanjing Medical University, Nanjing, People’s Republic of China
Yu Chang
Affiliation:
Department of Cardiology, Nanjing First Hospital, Nanjing Medical University, Nanjing, People’s Republic of China
Zi-hao Jiang
Affiliation:
Department of Cardiology, Nanjing First Hospital, Nanjing Medical University, Nanjing, People’s Republic of China
Xiao-min Jiang
Affiliation:
Department of Cardiology, Nanjing First Hospital, Nanjing Medical University, Nanjing, People’s Republic of China
Hao Xie
Affiliation:
Department of Cardiology, Nanjing First Hospital, Nanjing Medical University, Nanjing, People’s Republic of China
Xin-xin Jia
Affiliation:
Admin Office, Nanjing First Hospital, Nanjing Medical University, Nanjing 210006, People’s Republic of China
Ming-xing Chen*
Affiliation:
Department of Cardiology, Northern Jiangsu People’s Hospital, Yangzhou 225000, People’s Republic of China
Yue Gu*
Affiliation:
Department of Cardiology, Nanjing First Hospital, Nanjing Medical University, Nanjing, People’s Republic of China
*
*Corresponding authors: Yue Gu, email: [email protected]; Dr Ming-xing Chen, email [email protected]
*Corresponding authors: Yue Gu, email: [email protected]; Dr Ming-xing Chen, email [email protected]
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Abstract

Artificial sweeteners are generally used and recommended to alternate added sugar for health promotion. However, the health effects of artificial sweeteners remain unclear. In this study, we included 6371 participants from the National Health and Nutrition Examination Survey with artificial sweetener intake records. Logistic regression and Cox regression were applied to explore the associations between artificial sweeteners and risks of cardiometabolic disorders and mortality. Mendelian randomisation was performed to verify the causal associations. We observed that participants with higher consumption of artificial sweeteners were more likely to be female and older and have above medium socio-economic status. After multivariable adjustment, frequent consumers presented the OR (95 % CI) for hypertension (1·52 (1·29, 1·80)), hypercholesterolaemia (1·28 (1·10, 1·50)), diabetes (3·74 (3·06, 4·57)), obesity (1·52 (1·29, 1·80)), congestive heart failure (1·89 (1·35, 2·62)) and heart attack (1·51 (1·10, 2·04)). Mendelian randomisation confirmed the increased risks of hypertension and type 2 diabetes. Moreover, an increased risk of diabetic mortality was identified in participants who had artificial sweeteners ≥ 1 daily (HR = 2·62 (1·46, 4·69), P = 0·001). Higher consumption of artificial sweeteners is associated with increased risks of cardiometabolic disorders and diabetic mortality. These results suggest that using artificial sweeteners as sugar substitutes may not be beneficial.

Type
Research Article
Copyright
© The Author(s), 2024. Published by Cambridge University Press on behalf of The Nutrition Society

Artificial sweeteners have been widely employed as sugar substitutes in the food industry(Reference Iizuka1). Because of their strong sweetness and low-calorie characteristics, artificial sweeteners were generally considered safe and highly appreciated by consumers for weight loss and glycaemic control(Reference Alharthi, Alaisayi and Alalawi2Reference Norén and Forssell4). Hence, artificial sweeteners are frequently introduced to patients with metabolic or CVD to replace added sugar within a balanced diet(Reference Gardner, Wylie-Rosett and Gidding5). In fact, several basic researches and clinical trials have focused on the associations between artificial sweetener consumption with physiological index, gut microbiota and disease risks(Reference Pham, Stevens and Rigda6,Reference Bian, Chi and Gao7) . Though substantial attention from scientific and public fields has been paid, the long-term health effects of artificial sweeteners remained controversial.

Over the past few decades, sweeteners such as aspartame, acesulfame potassium and sucralose have been approved by the US Food and Drug Administration. Meanwhile, with the accumulation of continuous cross-sectional studies and the initiation of large prospective cohorts, it has been made possible to study the long-term health effects of artificial sweeteners. A recent prospective study, which enrolled health professionals with type 2 diabetes, suggested that artificial sweetener consumption did not influence all-cause mortality, CVD incidence and CVD mortality and favoured replacing sugar with artificial sweeteners(Reference Ma, Hu and Alperet8). These results were confirmed in a recent cohort study based on the general population by Pacheco(Reference Pacheco, Tobias and Li9). Moreover, evidence from the Strong Heart Family Study indicated no significant associations of artificial sweetener consumption with incident diabetes, fasting insulin or glucose levels(Reference Jensen, Howard and Best10). However, results from the NutriNet-Santé cohort suggested that higher consumers of artificial sweeteners confronted higher risks of developing CVD, type 2 diabetes and cancer(Reference Debras, Chazelas and Sellem11Reference Debras, Chazelas and Srour13).

In this context, we aimed to study the associations of artificial sweetener consumption with cardiometabolic risk factors and mortality based on the National Health and Nutrition Examination Survey (NHANES). Moreover, Mendelian randomisation (MR) was performed to back up our results.

Methods

Study population

The NHANES (https://www.cdc.gov/nchs/nhanes/index.htm) is a continuous programme designed to assess the health and nutritional status of adults and children in the USA. Since 1999, the NHANES has examined nationally representative individuals every 2 years. Detailed information on demographic, socio-economic, dietary and health status were normatively collected. Meanwhile, examination and laboratory tests were administered by skilled medical personnel. In this study, we enrolled two cycles (2003–2006) of the NHANES with artificial sweetener consumption records. Participants meeting the following criteria were excluded: less than 20 years old, being pregnant and without complete information on artificial sweetener consumption (Fig. 1). After exclusion, a total of 6371 participants were included for further analysis.

Fig. 1. Flow chart of study participants selection.

Assessment of artificial sweetener consumption

The frequency of artificial sweetener intakes was fetched from the ‘FFQ – Raw Questionnaire Responses’ data file in the dietary data section. Participants were asked, ‘How often did you add artificial sweetener to your coffee or tea?’, without detailed artificial sweetener types. Answers from participants were encoded with twelve values, including ten frequencies (never, less than 1 time per month, 1–3 times per month, 1 time per week, 2–4 times per week, 5–6 times per week, 1 time per d, 2–3 times per d, 4–5 times per d, 6 or more times per d), blank and error. Thereinto, data representing blank and error were treated as missing values. Then, the frequency of artificial sweetener consumption was merged into three levels: less than 1 time per month was deemed as ‘rare’, more than or equal to 1 time per d was considered as ‘frequent’ and the middle was defined as ‘moderate’.

Assessment of covariates

In the NHANES, demographic data and standardised questionnaires were collected by trained interviewers. The definition and categorisation of baseline characteristics, health status and medical conditions have been described previously(Reference Kan, Chen and Tao14). Briefly, we included age, sex, race/ethnicity, family poverty income ratio (PIR), employment status, marital status, education, smoking status, drinking status, body measurement index and several CVD at baseline. Family PIR was calculated by dividing family income by poverty guidelines specific to the survey year, deemed as a measure of socio-economic status. In addition, intakes of cold cereal, coffee and hot tea were considered. The frequency of their consumption was divided by once per month, once per week and once daily.

Assessment of outcomes

The corresponding follow-up information of the NHANES participants is available from the National Center for Health Statistics. Currently, available mortality data are updated to 31 December 2019. The underlying cause of death records were derived from UCOD_113, which could be recoded into comparable ICD-10 (International Classification of Diseases-10th Revision) based groups(Reference Anderson, Miniño and Hoyert15). We examined all-cause mortality, death from CVD (I00-I09, I11, I13, I20-I51) and diabetes mellitus (E10-E14) as outcomes.

Statistical analyses

After participant selection, covariates with more than 30 % missing values were removed. Missing values were complemented using multiple imputations with five times iterations. The imputed data were evaluated with box-and-whisker plots.

The Shapiro–Wilk test was performed to assess the distribution of continuous variables for normality. Non-normally distributed variables were described as medians (interquartile ranges), and Kruskal–Wallis tests were applied for comparisons. Categorical variables were reported using counts (percentages) and compared using Pearson’s χ2 tests.

In the cross-sectional analysis, logistic regression models were computed to evaluate the associations between artificial sweetener consumption and the prevalence of hypertension, hypercholesterolaemia, diabetes, obesity, congestive heart failure, coronary artery disease (CAD), angina pectoris, myocardial infarction and stroke. We defined the rare artificial sweetener consumers as the reference group in the primary three-category model to obtain OR and 95 % CI for moderate consumers and frequent consumers. Furthermore, potential confounders such as age, sex, race, education, family PIR, smoking, alcohol usage and cereal, coffee and hot tea intakes were considered in the adjusted models.

Kaplan–Meier method with log-rank test was employed to analyse the three-categorised survival curves (rare, moderate, frequent) of all-cause mortality and cause-specific mortality from CVD and diabetes mellitus. Then, we tested the proportional hazards assumption by calculating Schoenfeld residuals. Associations between frequency of artificial sweetener addition and all-cause, CVD and diabetic mortality risks were assessed by Cox proportional hazards models. Respectively, we calculated hazard ratios (HR) and 95 % CI with the rare consumer group as the reference category in univariate and multivariate models. Potential covariates such as age, sex, race, education, family PIR, smoking, alcohol usage and cereal, coffee and hot tea intakes were adjusted in the multivariate Cox model.

Subgroup analyses were conducted to test the sensitivity of the above results, exploring potential interactions with clinical features. Diabetic mortality risk was tested between the frequent group and rare group with stratified factors, including sex, age brackets (< 65, ≥ 65 years old), ethnicity, family PIR, drinking, smoking, diabetes and obesity. Interaction effects between artificial sweetener consumption and these variables were statistically assessed. All analyses were performed using R version 4.2.2. All statistical tests were two-sided, with a pre-set significance threshold of P < 0·05.

Mendelian randomisation

The two-sample MR study was conducted to provide causal evidence(Reference Sekula, Del Greco and Pattaro16). The summary-level genome-wide association studies data were retrieved from the IEU OpenGWAS data portal (https://gwas.mrcieu.ac.UK/)(Reference Elsworth, Lyon and Alexander17). Exposure factors were sourced from the UK Biobank(Reference Sudlow, Gallacher and Allen18), including artificial sweetener intake in cereal/coffee/tea in the European population (64 949 individuals), South Asian population (1469 individuals) and African American or Afro-Caribbean population (1207 individuals). We included ischaemic heart disease, hypertension and type 2 diabetes as outcome factors according to the corresponding populations. The included genome-wide association studies datasets were summarised in online Supplementary Table S1. The ‘TwoSampleMR’ package was employed to perform the MR analysis. A relatively relaxed threshold (P < 1 × 10–5) was applied to select instrumental variables from the common SNP sites. Then linkage disequilibrium clumping (r2 < 0·01, clumping distance = 5000 kb) was performed to prove the dependence of the chosen SNP. Five models (MR Egger, Weighted median, inverse variance weighted, simple mode, weighted mode) were utilised by default to eliminate potential bias from the heterogeneity of MR methods. In addition, certain tests were performed to guarantee reliability: leave-one-out test for sensitivity, Steiger test for directionality, heterogeneity test and pleiotropy test. The ‘MR-PRESSO’ package was utilised to test for horizontal pleiotropy as well(Reference Verbanck, Chen and Neale19).

Results

Baseline characteristics

Of the total 6371 participants, 4691 (73·6 %) participants added artificial sweetener < 1 monthly, 849 (13·3 %) ≥ 1 monthly and < 1 daily, 831 (13·0 %) ≥ 1 daily (Table 1). Compared with participants who rarely consumed artificial sweeteners, higher consumers were more likely to be female, older, non-Hispanic, separated, have a higher education level and middle-to-high annual income and with metabolic disorders (hypercholesterolaemia, diabetes) and CVD (hypertension, congestive heart failure, CHD, angina pectoris, heart attack and stroke). In addition, participants who had more artificial sweeteners reported higher BMI, glycated Hb and total cholesterol.

Table 1. Baseline characteristics of study population

(Median values and interquartile ranges; numbers and percentages)

Continued variables are presented as the median and interquartile range, compared with Kruskal–Wallis tests. Category variables are presented as count and proportion, compared using Pearson’s χ2 tests. PIR, poverty income ratio.

Association of artificial sweetener intake and cardiometabolic disorders

As demonstrated in Table 2, frequent artificial sweetener consumers might confront increased risks of hypertension (OR = 1·52 (1·29, 1·80), P < 0·001), hypercholesterolaemia (OR = 1·28 (1·10, 1·50), P = 0·002), diabetes (OR = 3·74 (3·06, 4·57), P < 0·001), obesity (OR = 1·52 (1·29, 1·80), P < 0·001), congestive heart failure (OR = 1·89 (1·35, 2·62), P < 0·001) and heart attack (OR = 1·51 (1·10, 2·04), P = 0·009).

Table 2. OR (95% CI) for cardiometabolic disorders according to the frequency of artificial sweetener intake

(Percentages; odds ratios and 95 % confidence intervals)

Model 1: Logistic regression model without adjustment. Model 2: adjusted for age, sex, race, education, family poverty income ratio, drinking and smoking status. Model 3: adjusted for variables in model 2 and cold cereal, coffee and hot tea intakes.

However, the causal effect of the above results was limited due to the cross-sectional design of the NHANES programme. Thus, MR was applied for verification. As shown in Fig. 2, our IVW models indicate a positive correlation between artificial sweetener added to coffee with ischaemic heart disease (OR = 1·18 (1·10, 1·26), P < 0·001), hypertension (OR = 1·04 (1·01, 1·08), P = 0·011) and type 2 diabetes (OR = 1·11 (1·06, 1·16), P < 0·001) among African population. Similar results were obtained in other models like MR Egger and so forth. Moreover, these results were steady with leave-one-out analysis, and the direction of these causal associations was tested and consolidated. Notably, MR-PRESSO global analysis also indicated a potential pleiotropy for ischaemic heart disease (P = 0·008), but not for hypertension (P = 0·822) and type 2 diabetes (P = 0·302). However, causal associations were not found from artificial sweetener intake in cereal or tea nor in European and South Asian populations (online Supplementary Table S2).

Fig. 2. Scatter plots for the associations between artificial sweeteners added to coffee and the risk of ischaemic heart disease (above), hypertension (middle) and type 2 diabetes (below). MR, Mendelian randomisation.

Association of artificial sweetener intake and mortality

Kaplan–Meier curves and log-rank tests showed that participants who consumed the highest levels of artificial sweeteners were exposed to significantly higher risks of all-cause (P < 0·001) and diabetic mortality (P < 0·001) (Fig. 3(a) and (b)). While mortality due to CVD was not significantly influenced (Fig. 3(c)). In Cox proportional hazard regression, compared with the rare consumers, participants who reported the highest levels of artificial sweetener consumption had substantially increased risks of all-cause (HR = 1·34 (1·17, 1·53), P < 0·001) and diabetic mortality (HR = 3·83 (2·18, 6·72), P < 0·001) (Table 3). After controlling for demographic, behavioural and dietary factors, the risk of diabetic mortality remained significant (HR = 2·62 (1·46, 4·69), P = 0·001). Consistently, a positive association between artificial sweeteners and diabetic mortality was observed to hold among subgroups, without potential interaction effect (Fig. 4).

Fig. 3. Kaplan–Meier survival plots of artificial sweetener consumption and all-cause mortality, diabetes mortality and cardiovascular mortality. Kaplan–Meier analyses showed that participants consuming artificial sweeteners more than one time per d had higher rates of all-cause death (a) and diabetic death (b), but not cardiovascular death (c). DM, diabetes mellitus.

Table 3. HR (95% CI) for all-cause, CVD and diabetic mortality according to the frequency of artificial sweetener intake (Percentages; hazard ratios and 95 % confidence intervals)

Model 1: Cox proportional hazards model without adjustment. Model 2: adjusted for age, sex, race, education, marital status, family poverty income ratio, drinking and smoking status. Model 3: adjusted for variables in model 2 and cold cereal, coffee, hot tea, total energy intakes (kcal).

Fig. 4. Adjusted diabetes mortality in subgroups with artificial sweetener consumption more than one time per d and less than one time per month. PIR, poverty income ratio.

Discussion

Results from the current study indicated positive associations between artificial sweetener intake and higher risks of several cardiometabolic disorders, especially for hypertension and type 2 diabetes. Moreover, higher artificial sweetener consumers confronted an increased risk of mortality from diabetes, but not CVD.

To our knowledge, this study for the first time linked artificial sweetener intake with diabetic mortality. Previous large-scale cohort studies have revealed positive associations between artificial sweeteners with risks of several cardiometabolic disorders and all-cause and CVD mortality. Results from the Women’s Health Initiative cohort suggested that participants who had more than one serving per d had a greater likelihood of stroke, CHD and all-cause mortality(Reference Mossavar-Rahmani, Kamensky and Manson20). Despite the counterpart results in our study were not statistically significant, they shared the same tendency. Similar results were reported in the UK Biobank cohort(Reference Luo, He and Ma21) and NutriNet-Santé cohort(Reference Debras, Chazelas and Sellem11). Interestingly, the NutriNet-Santé cohort further suggested the specific effects of artificial sweeteners on individuals, like aspartame towards cerebrovascular events, acesulfame potassium and sucralose towards CHD. What’s more, Malik et al. reported that CVD mortality was significantly higher in the highest artificial sweetener intake category(Reference Malik, Li and Pan22). Malik’s work included two large prospective cohorts, the Nurses’ Health Study and the Health Professionals Follow-up Study, whereas the significant results were merely seen in the pooled analysis. The weak association hinted the existence of residual confounding.

Comparatively, the relationship between artificial sweetener consumption and diabetes is much more intricate. People with diabetes or at high risk of developing diabetes tend to use artificial sweeteners to prevent or manage diabetes(Reference Alharthi, Alaisayi and Alalawi2,Reference Gebremichael, Lassi and Begum23) . However, two prospective studies and an MR study recently have identified that higher consumers of artificial sweeteners had higher risks of developing type 2 diabetes, regardless of sex and artificial sweetener types(Reference Debras, Deschasaux-Tanguy and Chazelas12,Reference Fagherazzi, Gusto and Affret24,Reference Zhang, Tang and Shi25) . Our work verified this result and further indicated that artificial sweetener consumption might contribute to diabetes-related adverse outcomes. Notably, the inference from MR by Zhang et al. is similar, but not the same, with our results. We merely identified causal associations between artificial sweetener intake in coffee and type 2 diabetes among the African population, rather than the European population. This difference may result from the parameter setting of instrumental variable selection.

Meanwhile, the underlying mechanism of how artificial sweeteners influence cardiovascular and endocrine systems remained unclear. Pham et al. performed intraduodenal administration of sucralose in healthy older subjects and found no significant changes in blood pressure or superior mesenteric artery blood flow(Reference Pham, Stevens and Rigda6). A prospective study reported that consumption of artificial sweeteners during pregnancy and at follow-up increased glycated Hb, insulin, TAG and liver fat and lowered HDL(Reference Hinkle, Rawal and Bjerregaard26). Moreover, artificial sweetener was found to lower β-cell glucose sensitivity, total insulin secretion and β-cell rate sensitivity in the Maastricht Study(Reference den Biggelaar, Sep and Mari27). These clinical trials provide insights into the effective targets of artificial sweeteners. In addition, basic research into the biological effect has been launched. For example, early research focused on the influence of artificial sweeteners on apo A-I and HDL, indicating a pro-atherogenic property in artificial sweetener-treated apo A-I(Reference Jang, Jeoung and Cho28). Interestingly, Bian et al. reported a 4-week acesulfame potassium consumption could perturb the gut microbiome of CD-1 mice, activating genes related to carbohydrate absorption, metabolism and lipopolysaccharide synthesis(Reference Bian, Chi and Gao7). Similarly, sucralose was reported to change the composition of mice gut microbiota as well and affect the intestinal barrier function(Reference Zheng, Xiao and Ma29). In addition, sucralose regulates endothelial barrier function by activating the sweet taste receptor T1R3(Reference Harrington, Vang and Braza30). These studies suggested the multiple physiological effects of artificial sweeteners. Considering the incremental consumption of artificial sweeteners worldwide, further study is needed to elucidate its health effects.

Though this study had the advantages of comprehensive baseline information and long follow-up, certain limitations should be acknowledged. First, the artificial sweetener usage habits recorded in this study were based on cross-sectional studies, participants may change their frequency of artificial sweetener intake during follow-up. Meanwhile, there is a lack of information regarding artificial sweeteners in other food items and detailed artificial sweetener types. Second, the sample size is relatively small, considering the low incident rate of death due to diabetes. The number of events in some subgroups was too small for analysis. Third, SNP sites strongly associated with artificial sweetener intake are scarce. Thus, we employed a relaxed threshold in MR analysis. Additionally, using artificial sweetener intake as exposure might not well satisfy the gene-environment equivalence during MR analysis. The results should be interpreted with great caution.

Conclusions

In summary, we reported that greater consumers of artificial sweeteners are confronted with a higher risk of cardiometabolic disorders (hypertension, type 2 diabetes) and diabetic mortality. People who use artificial sweeteners to prevent and manage diabetes may not benefit from these sugar substitutes. Our results support public outreach to limit artificial sweetener consumption to avoid its adverse health effects.

Acknowledgements

The authors thank Qi-tao Chen for his help in polishing English writing.

This work was supported by the National Natural Science Foundation of China (grant nos. 82100474, 82100429) and the Scientific Research Project of Jiangsu Provincial Health Commission (grant no. M2021040).

Yue Gu and Ming-xing Chen conceived the study design and are responsible for the overall content. Jun-yan Kan and Dong-chen Wang analysed and interpreted the data. Yu Chang and Zi-hao Jiang wrote the manuscript. Xiao-min Jiang, Hao Xie and Xin-xin Jia edited the manuscript. All authors read and approved the final manuscript.

The authors declare that they have no competing interests.

Supplementary material

For supplementary material/s referred to in this article, please visit https://doi.org/10.1017/S000711452400223X.

Footnotes

These authors are co-first authors and equally contributed to this work.

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Figure 0

Fig. 1. Flow chart of study participants selection.

Figure 1

Table 1. Baseline characteristics of study population(Median values and interquartile ranges; numbers and percentages)

Figure 2

Table 2. OR (95% CI) for cardiometabolic disorders according to the frequency of artificial sweetener intake(Percentages; odds ratios and 95 % confidence intervals)

Figure 3

Fig. 2. Scatter plots for the associations between artificial sweeteners added to coffee and the risk of ischaemic heart disease (above), hypertension (middle) and type 2 diabetes (below). MR, Mendelian randomisation.

Figure 4

Fig. 3. Kaplan–Meier survival plots of artificial sweetener consumption and all-cause mortality, diabetes mortality and cardiovascular mortality. Kaplan–Meier analyses showed that participants consuming artificial sweeteners more than one time per d had higher rates of all-cause death (a) and diabetic death (b), but not cardiovascular death (c). DM, diabetes mellitus.

Figure 5

Table 3. HR (95% CI) for all-cause, CVD and diabetic mortality according to the frequency of artificial sweetener intake (Percentages; hazard ratios and 95 % confidence intervals)

Figure 6

Fig. 4. Adjusted diabetes mortality in subgroups with artificial sweetener consumption more than one time per d and less than one time per month. PIR, poverty income ratio.

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