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Electronic Cigarette Use and Myocardial Infarction Among Adults in the US Population Assessment of Tobacco and Health


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Electronic Cigarette Use and Myocardial Infarction Among Adults in the US Population Assessment of Tobacco and Health

Dharma N. Bhatta and Stanton A. Glantz

Originally published 18 Jun 2019https://doi.org/10.1161/JAHA.119.012317Journal of the American Heart Association. 2019;8

https://www.ahajournals.org/doi/10.1161/JAHA.119.012317?fbclid=IwAR34_ZKD7TnpD9J5vCKXIzTL7MTYUivnjxJSRs0k-ZHddM9L0WSNtXRS7kQ&

 

Conclusions

Some‐day and every‐day e‐cigarette use are associated with increased risk of having had a myocardial infarction, adjusted for combustible cigarette smoking. Effect of e‐cigarettes are similar as conventional cigarette and dual use of e‐cigarettes and conventional cigarettes at the same time is risker than using either product alone.

 

What Are the Clinical Implications?

E‐cigarettes should not be promoted or prescribed as a less risky alternative to combustible cigarettes and should not be recommended for smoking cessation among people with or at risk of myocardial infarction.

 

Abstract

Background

E‐cigarettes are popular for smoking cessation and as an alternative to combustible cigarettes. We assess the association between e‐cigarette use and having had a myocardial infarction (MI) and whether reverse causality can explain the observed cross‐sectional association between e‐cigarette use and MI.

 

Methods and Results

Cross‐sectional analysis of the Population Assessment of Tobacco and Health Wave 1 for association between e‐cigarette use and having had and MI. Longitudinal analysis of Population Assessment of Tobacco and Health Waves 1 and 2 for reverse causality analysis. Logistic regression was performed to determine the associations between e‐cigarette initiation and MI, adjusting for cigarette smoking, demographic and clinical variables. Every‐day (adjusted odds ratio, 2.25, 95% CI: 1.23–4.11) and some‐day (1.99, 95% CI: 1.11–3.58) e‐cigarette use were independently associated with increased odds of having had an MI with a significant dose‐response (P<0.0005). Odds ratio for daily dual use of both products was 6.64 compared with a never cigarette smoker who never used e‐cigarettes. Having had a myocardial infarction at Wave 1 did not predict e‐cigarette use at Wave 2 (P>0.62), suggesting that reverse causality cannot explain the cross‐sectional association between e‐cigarette use and MI observed at Wave 1.

 

Conclusions

Some‐day and every‐day e‐cigarette use are associated with increased risk of having had a myocardial infarction, adjusted for combustible cigarette smoking. Effect of e‐cigarettes are similar as conventional cigarette and dual use of e‐cigarettes and conventional cigarettes at the same time is risker than using either product alone.

 

Clinical Perspective

What Is New?

Both e‐cigarettes and combustible cigarettes are independently associated with increased risk of myocardial infarction.

Dual use of e‐cigarettes and combustible cigarettes is riskier than using either product alone and switching from combustible cigarettes to e‐cigarettes is not associated with lower risk of myocardial infarction than continuing to smoke; complete cessation is the only way to reduce risk of myocardial infarction.

 

These results are unlikely becauseof reverse causality, where smokers who had myocardial infarctions started using e‐cigarettes in an effort to quit smoking.

 

What Are the Clinical Implications?

 

E‐cigarettes should not be promoted or prescribed as a less risky alternative to combustible cigarettes and should not be recommended for smoking cessation among people with or at risk of myocardial infarction.

Introduction

 

Cardiovascular disease is the leading cause of death in the United States1 and tobacco smoking is a major modifiable risk factor for cardiovascular disease, including myocardial infarction.2 The risk of myocardial infarction is 2‐ to 5‐fold higher among young smokers compared with never smokers,2, 3 with a non‐linear dose‐response curve with even the low levels of exposure associated with smoking a single cigarette a day4 or breathing secondhand smoke conferring substantial risk.5

 

E‐cigarettes are promoted as a smoking cessation device and less dangerous way to self‐administer nicotine than conventional cigarettes6, 7 and people with cardiovascular disease are using e‐cigarettes as a smoking cessation aid.8 Like conventional cigarettes, e‐cigarettes deliver nicotine as an inhaled aerosol of nicotine and ultrafine particles.9 Fine particles increase cardiovascular risk.10 E‐cigarettes and combustible cigarettes have similar effects on endothelial function which increases the risk of cardiovascular disease.11, 12, 13, 14, 15 E‐cigarettes increase oxidative stress and the release of inflammatory mediators,11, 16 induce platelet activation, aggregation, and adhesion17 and alters cardiovascular function in mice.18, 19, 20 Acute exposure to electronic cigarettes with nicotine increases aortic stiffness21 and cardiac sympathetic tone (reflected in heart rate variability) in a way associated with increased cardiac risk.13 Nevertheless, the 2018 National Academies of Science, Engineering, and Medicine report Public Health Consequences of E‐Cigarettes22 observed that “there are no epidemiological studies evaluating clinical outcomes such as coronary heart disease …. This lack of data on e‐cigarettes and clinical and subclinical atherosclerotic outcomes represents a major research need.” Since then, 2 studies, 1 using data from the National Health Interview Survey23 and another using data from the Behavioral Risk Factors Surveillance Survey,24 found cross‐sectional associations between e‐cigarette use and having had a myocardial infarction among daily e‐cigarette users controlling for cigarette smoking and other risk factors. Nevertheless, this finding remains controversial, because of concerns about reverse causality based on the possibility that after having a myocardial infarction smokers switched to e‐cigarettes, which would induce a spurious association between e‐cigarette use and myocardial infarction.25, 26 We use the Population Assessment of Tobacco and Health27 (PATH) data set to test for the relationship between e‐cigarette use and myocardial infarction, controlling for cigarette use, demographic and clinical variables and use the longitudinal data from PATH to test the reverse causality hypothesis.

 

Methods

Study Population and Design

We used PATH Waves 1 and 2 (Figure S1), a nationally representative population‐based longitudinal cohort study to collect data on uses of tobacco products, health outcomes, risk perception, and attitudes.27 The restricted use PATH data set is available at the University of Michigan National Addiction & HIV Data Archive Program.28 The Wave 1 data set contained 32 320 adults aged ≥18 years and 28 362 adults in Wave 2, of whom 26 447 completed a Wave 1 interview. Wave 1 data were collected from September 2013 to December 2014 and Wave 2 data were collected 1 year later (from October 2014 to October 2015). PATH uses a 4‐stage stratified probability sample technique. The weighted response rate at Wave 1 household screener was 54.0%; among screened households, overall weighted response rate at Wave 1 adult interview was 74.0%. The weighted retention rate for continuing adult at Wave 2 was 83.1%, and the weighted recruitment rate including youth aged <18 years at Wave 1 and ≥18 years (and so counted as adults at Wave 2) was 85.7%.28 Informed consent was obtained by PATH. The University of California San Francisco (UCSF) Committee on Human Research approved this study.

 

Outcome Variables

Wave 1: Participants who responded “Yes” to the question “Has a doctor, nurse, or other health professional ever told you that you had a heart attack (myocardial infarction)?” were considered as having had a myocardial infarction.

Wave 2: Participants who responded “Yes” to the question “In the past 12 months, has a doctor, nurse, or other health professional told you that you had a heart attack (myocardial infarction)?” were considered as having had a myocardial infarction.

 

Independent Variables

 

Electronic cigarette use

Respondents who reported that they have ever used e‐cigarettes, have used fairly regularly, and currently use every day were classified as “Every‐day users.” Respondents who reported that they have ever used e‐cigarettes, have used fairly regularly, and currently use some days were considered as “Some‐day users.” Respondents who reported that they have ever used e‐cigarettes and currently do not use them were considered “Former users.” Respondents who reported that they have never used e‐cigarettes, even once or twice were considered “Never users.” Current experimental e‐cigarette users (current e‐cigarette users but never used e‐cigarettes fairly regularly) were not included in the main analysis but were considered some‐day users in a sensitivity analysis.

 

Cigarette smoking

Respondents who reported that they smoked at least 100 cigarettes in their lifetime and currently smoke every day were classified as “Every‐day smokers.” Respondents who reported that they smoked at least 100 cigarettes in their lifetime and currently smoke some days were classified as “Some‐day smokers.” Respondents who ever smoked cigarettes and have not smoked in the past 12 months or currently do not smoke at all were classified as “Former smokers.” Respondents who reported that they have never smoked a cigarette, even 1 or 2 puffs were classified as “Never smokers.” Respondents who were current smokers but who had not smoked 100 cigarettes (experimental smokers) were excluded from the main analysis, but included in a sensitivity analysis as some‐day smokers.

 

Demographic variables

Demographic variables were assessed at Wave 1: age, body mass index (BMI), sex (men or women), race/ethnicity (white, black, Asian, and others), poverty level/income (below poverty: <100% of poverty line, at or above poverty: ≥100% of poverty line [poverty was calculated using this formula: [effective family income]/[poverty guideline]×100=family income as a percentage of the household size poverty guideline.]) and education.

 

Clinical variables

Wave 1: Respondents who answered “Yes” to the question “Has a doctor, nurse, or other health professional ever told you that you had a high blood pressure?” were considered as having “high blood pressure.” Respondents who answered “Yes” to the question “Has a doctor, nurse or other health professional ever told you that you had a high cholesterol?” were considered as having “high cholesterol.” Respondents who answered “Yes” to the question “Has a doctor, nurse, or other health professional ever told you that you had a diabetes, sugar diabetes, high blood sugar, or borderline diabetes?” were considered as having “diabetes mellitus.”

 

Wave 2: Respondents who answered “Yes” to the question “In the past 12 months, has a doctor, nurse or other health professional told you that you had a high blood pressure?” were considered as having “high blood pressure.” Respondents who answered “Yes” to the question “In the past 12 months, has a doctor, nurse, or other health professional told you that you had a high cholesterol?” were considered as having “high cholesterol”. Respondents who answered “Yes” to the question “In the past 12 months, has a doctor, nurse, or other health professional told you that you had a diabetes, sugar diabetes, high blood sugar, or borderline diabetes?” were considered as having “diabetes mellitus.”

 

Analysis

We calculated weighted estimates of e‐cigarette and cigarette use and clinical and demographic variables at Wave 1 for the overall sample. We used Wave 1 sampling weights for analysis of Wave 1 and Wave 2 sampling weights for analysis of Wave 228 accounting for the complex survey design for all the outcomes.29

 

Multivariable logistic regressions were performed to examine the associations between e‐cigarette use (former, some day and every day) and myocardial infarction at Wave 1 controlling for cigarette smoking (former, some day and every day), age, BMI, sex, poverty level, race/ethnicity, education, and clinical variables.

 

We tested for interaction between e‐cigarette use and cigarette smoking in a logistic regression by combining some‐day and every‐day users into “current e‐cigarette use” and “current smoking,” then ran the logistic regression with these variables, their interaction, and the demographic and clinical variables. The P value for the interaction was 0.671. Likewise, we analyzed interaction for “former e‐cigarette use” and “former smoking”, and P value for this model was 0.192. As a result, interaction terms were omitted from the remaining analysis.

 

We tested for dose‐response by replacing the categorical use variables with continuous variables (0=never, 1=former, 2=some day, 3=every day) in logistic regressions including the demographic and clinical variables.

 

We assessed the possibility of reverse causality accounting for the observed association between having had a myocardial infarction at Wave 1 being due to people who had a myocardial infarction preferentially trying to quit smoking with e‐cigarettes. Specifically, we used logistic regression to predict every day e‐cigarette use at Wave 2 as a function of having had a myocardial infarction at Wave 1 adjusting for age, BMI, sex, poverty level, and race/ethnicity among only every day, and only current (every day and some day) cigarette smoker at Wave 1 (excluding all e‐cigarette users) as well as in the entire longitudinal sample.

 

We used “survey package” in R software for statistical analyses.

 

Results

Table 1 shows the descriptive statistics at Wave 1 baseline; 643 (2.4%) adults reported that they had a myocardial infarction. Table 2 shows the descriptive statistics stratified by myocardial infarction status at Wave 1 and first myocardial infarctions between Waves 1, 2, and 3 and Table S1 shows the descriptive statistics stratified by e‐cigarette use at Wave 1. Among the adults who had myocardial infarctions as of Wave 1, 10.2% reported that they were former e‐cigarette users, 1.6% were some‐day e‐cigarette users and 1.5% were every‐day e‐cigarette users, 58.8% adults reported that they were former cigarette smokers, 3.4% were some‐day cigarette smokers and 20.4% were every‐day cigarette smokers. The number of e‐cigarette users who had first myocardial infarctions between Waves 1 and 2 (only 6 some‐day and 2 every‐day e‐cigarette users) and Waves 2 and 3 (only 1 some‐day and 3 every‐day e‐cigarette users) was small, so, as required by PATH reporting rules, we combined some‐day and every‐day e‐cigarette users in Table 2 for the first myocardial infarction between Waves 1 and 2, and Waves 2 and 3.

 

As expected, any cigarette smoking, age, BMI, sex, poverty level, education, and high blood pressure, high cholesterol, and diabetes mellitus were significantly associated with increased risk of myocardial infarction.

 

There was a significant dose‐response for both e‐cigarette use (P<0.0005) and smoking (P=0.019) and myocardial infarction controlling for demographic and clinical variables (detailed results not shown).

 

The longitudinal analysis did not reveal any statistically significant associations between e‐cigarette use at Wave 1 and having had a first myocardial infarction by Wave 2, perhaps because of the small numbers of first myocardial infarctions in e‐cigarette users between Waves 1 and 2 (Table S2). Daily cigarette smoking was also not significantly associated with having had a first myocardial infarction at Wave 2.

 

The sensitivity analysis including current experimental e‐cigarette user with some‐day e‐cigarette user and current experimental cigarette smokers with some‐day cigarette smokers yielded similar results as the main analysis (Table S3).

Reverse Causality

 

There were 1990 respondents who started using e‐cigarettes between Waves 1 and 2 (Table 4). Having had a myocardial infarction at Wave 1 did not predict every‐day e‐cigarette use at Wave 2 among overall follow‐up sample (P=0.687), every‐day cigarette smokers at Wave 1 (P=0.675), or current cigarette smokers at Wave 1 (P=0.634), adjusting for demographic and clinical variables. Similar results were obtained for any e‐cigarette use (every day or some day) at Wave 2 (Table S4).

 

Click here to see tables

 

Discussion

This study confirms earlier23, 24 findings that e‐cigarette use is an independent risk factor for having had a myocardial infarction controlling for cigarette smoking, demographic and clinical risk factors. The magnitudes of the effects in this study are similar to the updated analysis by Alzahrani and Glantz30 using the 2014, 2015, and 2016 from the National Health Interview Survey (some‐day e‐cigarette user [odds ratio: 1.99, 95% CI: 1.11–3.58 in this study versus 1.49: 1.08–2.09 in Alzahrani et al] and every‐day e‐cigarette user [2.25: 1.23–4.11 versus 2.14: 1.41–3.25]). Odds of myocardial infarction among former e‐cigarette users are not significantly elevated in either study. The increased odds of myocardial infarction are similarly and significantly associated with smoking in both studies, with higher estimates in the present study (former [1.48: 1.01–2.15 versus 1.70: 1.51–1.91], some day [2.38: 1.40–4.06 versus 2.36; 1.80–3.09] and every day [2.95: 1.91–4.56 versus 2.72: 2.29–3.24]). Vindhyal et al31 reported that e‐cigarette use is significantly associated with MI (odds ratio [OR] 1.56 [1.45–1.68]), stroke (OR 1.30 [1.20–1.40]), and circulatory problems (OR 1.44 [1.25–1.65]) using the 2014, 2016, and 2017 National Health Interview Survey. Ndunda and Muutu24 found that compared with non‐users, e‐cigarette users (without specifying frequency of use, but controlling for smoking and other risk factors) the odds of having had a myocardial infarction (OR 1.59 [1.53–1.66]) that was lower than in this study, although the CIs overlapped. They also found higher risks for angina or coronary heart disease (OR 1.4 [1.35–1.46]) and stroke (OR 1.71 [1.64–1.8]) using 2016 Behavioral Risk Factor Surveillance System.

 

Both the present and earlier23, 24 results are based on cross‐sectional analysis, which raises the possibility of reverse causality,25, 26 specifically that after having had a myocardial infarction people might preferentially attempt to quit smoking using e‐cigarettes. In a cross‐sectional analysis of the National Health Interview Survey, Stokes et al8 reported that individuals with cardiovascular disease who recently quit smoking or recently attempt to quit were more likely to use e‐cigarettes than those who did not report a recent quit attempt, which may indicate that e‐cigarettes were being used for smoking cessation. We used the longitudinal data in PATH to test directly for reverse causality by testing whether having had a myocardial infarction at Wave 1 predicted e‐cigarette use at Wave 2 among people who were cigarette smokers at Wave 1 (Table 4). The results did not approach statistical significance (P>0.62 for all outcomes), strongly suggesting that reverse causality is not an issue. In addition, the presence of a statistically significant dose‐response is consistent with a causal effect.

 

Our results on the lack of reverse causality are consistent with Gaalema et al32 who concluded based on longitudinal analysis of the first 2 waves of PATH, that having a myocardial infarction was not a significant predictor of initiating non‐combusted tobacco (mostly e‐cigarettes) use (P=0.20). Furthermore, they found, “cardiac status was significantly negatively associated with switching completely from combusted to non‐combusted products. While 9.2% of those with no change in health status switched (from combusted tobacco, mostly cigarettes) to non‐combusted use, none of those experiencing a new MI switched (P=0.0015).” Thus, any differential misclassification is in the direction opposite to what would be required for reverse causality to explain our results, which strengthens our conclusion that e‐cigarette use is associated with the risk of having had an MI. Our finding is also consistent with Alzahrani et al's26 cross‐sectional analysis of reverse causality using the National Health Interview Survey, which found a non‐significant association between MI and e‐cigarette use when controlling for covariates.

 

Like Alzahrani et al,23, 30 we found that the increased odds of having had a myocardial infarction associated with e‐cigarette use were independent of the increased odds associated with smoking. This result means that dual use of e‐cigarettes and conventional cigarettes, the most common use pattern for e‐cigarette users, is more dangerous than use of either product alone (69% of current e‐cigarette users were also smoking cigarettes in our sample at Wave 1, which is similar to the 70% Stokes et al8 reported among people with cardiovascular disease in the National Health Interview Survey). For example, the total odds of having had a myocardial infarction among every‐day cigarette smokers who also use e‐cigarettes every day (dual users)—the most common use pattern (Table 1)—is (odds of myocardial infarction among every‐day smokers)×(odds of myocardial infarction among every‐day e‐cigarette user)=2.95×2.25=6.64 compared with a never cigarette smoker who has never used e‐cigarettes (which is similar from additional regression analysis estimating the effect directly, Adjusted Odds Ratio (AOR): 5.06, 95% CI: 1.99–12.83, Table S5). Odds of having had a myocardial infarction for individuals who switched from every‐day combustible cigarette smoking to every‐day e‐cigarette use would change by a factor of ([odds of myocardial infarction among former combustible cigarette smokers]×[odds of myocardial infarction among every‐day e‐cigarette user])/(odds of myocardial infarction among every‐day combustible cigarette smoker)=3.33/2.95=1.13, which is virtually no benefit in terms of myocardial infarction risk. More importantly, the total odds of having had a myocardial infarction for an individual who switched from every‐day combustible cigarette smoking to every‐day e‐cigarette use compared with quitting smoking would be ([odds of myocardial infarction among former smokers]×[odds of myocardial infarction among every‐day e‐cigarette user])/(odds of myocardial infarction among former cigarette smokers)=(1.48×2.25)/1.48=2.25.

 

As discussed above, we cannot infer temporality from the cross‐sectional finding that e‐cigarette use is associated with having had an MI and it is possible that first MIs occurred before e‐cigarette use. PATH Wave 1 was conducted in 2013 to 2014, only a few years after e‐cigarettes started gaining popularity on the US market around 2007. To address this problem we used the PATH questions “How old were you when you were first told you had a heart attack (also called a myocardial infarction) or needed bypass surgery?” and the age when respondents started using e‐cigarettes and cigarettes (1) for the very first time, (2) fairly regularly, and (3) every day. We used current age and age of first MI to select only those people who had their first MIs at or after 2007 (Table S6). While the point estimates for the e‐cigarette effects (as well as other variables) remained about the same as for the entire sample, these estimates were no longer statistically significant because of a small number of MIs among e‐cigarette users after 2007. Note that this analysis does not capture reinfarctions occurring after 2007, whose risk could be increased by e‐cigarette use as it is for continued smoking conventional cigarettes.33, 34

 

One could argue that the cleanest study would have been one that only examined the association of sole e‐cigarette use with myocardial infarction. In contrast, most e‐cigarette users are dual users with cigarettes so it is important to study the effects of e‐cigarette use simultaneously with cigarette use. Our analysis quantified the additional risk of MI associated with e‐cigarette use in addition to cigarette smoking among dual users. Limiting the analysis to sole e‐cigarette users would not only be less clinically relevant, but would substantially reduce the sample size and the power of the analysis to detect an effect.

Limitations

 

While PATH is a longitudinal study, there were only 8 people who used e‐cigarettes and had first myocardial infarctions during this follow‐up, so there was not enough power to detect an effect. Confirming this problem, every‐day and former‐conventional cigarette smoking were not significant either. While longitudinal studies are more desirable than cross‐sectional studies, the reality is that it will be years before enough myocardial infarctions have occurred to do a meaningful analysis. In the meantime, millions of people are using e‐cigarettes and clinicians are being asked about them and this cross‐sectional analysis can be used to inform decision making about these products.

 

Response for both e‐cigarette and combustible cigarette use were self‐reported, which could lead to recall bias. Participants with myocardial infarction might over‐report e‐cigarette and cigarette use, but previous work found that compared with biochemical monitoring with cotinine levels, self‐reporting in myocardial infarction survivors tended to understate the prevalence of smoking.35 Myocardial infarction was self‐reported which also could lead recall bias, but the questions “Has a doctor, nurse, or other health professional ever told you that you had a heart attack (myocardial infarction)?” and “In the past 12 months, has a doctor, nurse, or other health professional told you that you had a heart attack (myocardial infarction)?” have been found to have high agreement (81%–98%) with medical records.36, 37

 

Other possible risk factors including family history of myocardial infarction, angina, and heavy alcohol use are not available in the PATH data set. There is no information on the duration since smoking or e‐cigarette cessation. In the main analysis, it also is unknown whether the reported myocardial infarction occurred before or after the respondents’ initiated e‐cigarettes and cigarettes use.

Conclusions

 

As one would expect based on what is known about the biological effects of e‐cigarette use, in the cross‐sectional analysis some‐day and every‐day e‐cigarette use is associated with increased risk for having myocardial infarction, adjusted for combustible cigarette smoking, demographic and clinical variables. This result is unlikely because of reverse causality. Former, some‐day, and every‐day combustible cigarette smoking is also independently associated with myocardial infarction among adults in the United States. Dual use of the e‐cigarette and combustible cigarettes results in higher risk of myocardial infarction than using either product alone and switching from cigarettes to e‐cigarettes was not associated with any benefits in terms of reduced myocardial infarction risk. E‐cigarettes should not be promoted or prescribed as a less risky alternative to combustible cigarettes and should not be recommended for smoking cessation among people with or at risk of myocardial infarction.

 

Sources of Funding

This work was supported by grants R01DA043950 from the National Institute on Drug Abuse, P50CA180890 from the National Cancer Institute and the Food and Drug Administration Center for Tobacco Products, U54HL147127 from the National Heart, Lung, and Blood Institute and the Food and Drug Administration Center for Tobacco Products, and the University of California San Francisco (UCSF) Helen Diller Family Comprehensive Cancer Center Global Cancer Program. The content is solely the responsibility of the authors and does not necessarily represent the official views of National Institutes of Health or the Food and Drug Administration. The funding agencies played no role in study design, collection, analysis, and interpretation of data, writing the report, or the decision to submit for publication.

Disclosures

None.

Footnotes

*Correspondence to: Stanton A. Glantz, PhD, Center for Tobacco Control Research and Education, University of California, San Francisco, 530 Parnassus Ave, Suite 366, San Francisco, CA 94143‐1390. E‐mail: stanton.glantz@ucsf.edu

 

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