Data sources

This is a secondary dataset analysis of the GWAS datasets. GWAS datasets were obtained from the IEU OpenGWAS project (https://gwas.mrcieu.ac.uk). The GWAS dataset for smoking initiation was derived from GWAS analysis and included 311629 cases and 321173 controls of European ancestry⁸. Smoking initiation phenotypes included age of initiation of regular smoking, a binary phenotype indicating whether an individual had ever smoked regularly, and heaviness of smoking measured with cigarettes per day. The GWAS dataset for atrial fibrillation was derived from another analysis and included 60620 cases and 970216 controls of European ancestry⁹. Atrial fibrillation phenotypes included the duration of long-lasting atrial fibrillation, the age of onset of atrial fibrillation, and atrial fibrillation caused by other diseases. These phenotypes are mainly displayed through electrocardiogram-related data.

Screening of IVs

The genome-wide association study data identified SNPs with exposure variables (p<5.0×10^-8). To ensure the independence of SNPs and eliminate the confounding effect of linkage disequilibrium (LD), clumping was conducted using the TwoSampleMR package in R software. The parameters were set to r² <0.001 and a distance threshold of 10000 kb. In order to ascertain that the selected IVs satisfy the independence assumption, the remaining SNPs were subjected to an association test with other phenotypes using PhenoScanner (http://www.phenoscanner.medschl.cam.ac.uk). The association hypothesis was further tested by calculating the F-statistic to assess the presence of weak IV bias in the selected IVs. The absence of weak IV bias was confirmed by an F-statistic value >10, where:

F = R² (N-2)/ (1-R²)¹⁰.

Research design

MR studies must satisfy three core assumptions¹¹: association, independence, and exclusivity. These assumptions are as follows: 1) the IVs must be strongly associated with the exposure factor; 2) the IVs should not be associated with any confounders that are associated with the exposure or outcome; and 3) the IVs can only influence the outcome variable through the exposure factor. Supplementary file Figure 1 illustrates the principles of MR.

Statistical analysis

To ensure that the effect of SNPs on exposure and outcome corresponded to the same alleles, the summary statistics of the exposure and outcome datasets were harmonized. Associations were inferred using TSMR analyses involving the IVW method, weighted median, MR Egger regression, and simple and weighted mode methods. OR and 95% CI were calculated for the association between smoking initiation and atrial fibrillation. The IVW method was primarily used for Mendelian randomization. The IVW method combined the Wald ratio estimates of the effects of different SNPs when each genetic variation met the IV hypothesis. This provided a consistent estimate of the effect of exposure on the outcome. The reliability of the IVW method’s results is highest when there is no horizontal pleiotropy of the IVs. The weighted median provided a consistent estimate of the effect when at least half of the SNPs were effective IVs. MR-Egger regression confirmed horizontal pleiotropy for IVs, with its intercept representing the effect estimate. MR-Egger regression is based on the assumption of instrument strength independent of direct effect (InSIDE). When horizontal pleiotropy is present in the IVs, the MR-Egger regression can still provide an unbiased estimate of the association. To improve the accuracy of the results, compared to the MR-Egger method, we performed complementary analyses using the weighted median method and the simple mode and weighted mode. To detect and correct horizontal pleiotropy by removing outliers, we used the Mendelian randomization pleiotropy residual sum and outlier (MR-PRESSO) test¹². Statistical analysis was performed using R (version 4.3.1) and R packages (TwoSampleMR and MR-PRESSO). The test level α was 0.05 (p<0.05), for the difference to be statistically significant. All tests were two-tailed.

Effects of smoking initiation on atrial fibrillation

Smoking initiation was the exposure factor, and atrial fibrillation was the outcome variable. The screening criteria yielded a total of 85 SNPs included in the study as IVs. Each F-statistic associated with instrumental exposure was >10, effectively eliminating weak IVs from biasing the results (Supplementary file Table 1). The horizontal pleiotropy test results, obtained using the Egger-intercept method, resulted in p=0.371 (Egger intercept= -0.005), indicating that the IVs did not significantly affect the outcome through pathways other than exposure (Table 1, Figure 1).

Figure 1

Scatter plot of the effect of smoking initiation on atrial fibrillation, IEU OpenGWAS 2018–2019 (N=372249)

Without horizontal pleiotropy, the results of the TSMR were analyzed using the IVW method of the random-effects model. The IVW method suggested that the presence of smoking initiation was associated with a 1.11-fold increased likelihood of atrial fibrillation (IVW result: OR=1.11; 95% CI: 1.02–1.20, p=0.013). The following results were obtained: MR Egger, OR=1.33; 95% CI: 0.89–1.99, p=0.175; weighted median, OR=1.09; 95% CI: 0.99–1.12, p=0.094; simple mode, OR=1.17; 95% CI: 0.90–1.52, p=0.248; and weighted mode, OR=1.16; 95% CI: 0.92–1.46, p=0.224 (Table 2, Figures 1 and 2).

Figure 2

Forest plot of the effect of smoking initiation on atrial fibrillation, IEU OpenGWAS 2018–2019 (N=372249)

The funnel plot indicates that all SNPs were largely symmetrical, suggesting minor differences between IVs. Although Cochran’s Q test indicated heterogeneity (MR-Egger regression: Cochran’s Q=138.51, p<0.001; IVW: Cochran’s Q=139.86, p<0.001), the results of the random-effects IVW method indicated that there was indeed an association between smoking initiation and AF (Table 1, Figure 3). Furthermore, the MR-PRESSO method consistently yielded estimates before and after outlier correction.

Figure 3

Funnel plot of the effect of smoking initiation on atrial fibrillation, IEU OpenGWAS 2018–2019 (N=372249)

The leave-one-out sensitivity analysis demonstrated that excluding each SNP in turn produced IVW analysis results comparable to those including all SNPs. Furthermore, no SNPs were identified as having a substantial impact on the association estimates. No variants strongly associated with the potential confounders were found in the instrumental variables using PhenoScanner V2, indicating that the TSMR analysis results were robust (Figure 4).

Figure 4

Sensitivity analysis of the effect of smoking initiation on atrial fibrillation, IEU OpenGWAS 2018–2019 (N=372249)

Reverse TSMR analysis

In reverse TSMR, atrial fibrillation was the exposure factor, and smoking initiation was the outcome variable. A total of 109 SNPs were included in this study. All SNPs were found to be significantly associated with atrial fibrillation (p<5×10^-8), with F-statistics exceeding 10 (Supplementary file Table 2). The results of the horizontal pleiotropy test, with p>0.05 (Egger intercept = -0.001, p=0.367) (Table 1), indicates no horizontal pleiotropy for the IVs. The following MR results were obtained: IVW, OR=1.00; 95% CI: 0.99–1.02, p=0.684; MR Egger, OR=1.02; 95% CI: 0.99–1.05, p=0.326; weighted median, OR=1.02; 95% CI: 1.00–1.04, p=0.090; simple mode, OR=1.01; 95% CI: 0.96–1.05, p=0.825; and weighted mode, OR=1.01; 95% CI: 0.99–1.03, p=0.392 (Table 3, Supplementary file Figures 2 and 3). The results of the heterogeneity test indicate the presence of significant heterogeneity among the selected IVs (MR Egger regression: Cochran’s Q=230.09, p<0.001; IVW: Cochran’s Q=231.85, p<0.001) (Table 1, Supplementary file Figure 4). Furthermore, no outliers or instances of directed pleiotropy were identified in the IVs as analyzed by MR-PRESSO. The leave-one-out sensitivity analysis demonstrated that individual SNP did not influence the genetic results (Supplementary file Figure 5).

Limitations

This study has some limitations. First, the MR results were based on the GWAS dataset derived from individuals with European ancestry, preventing the extrapolation of our results to other ethnicities. Further research is needed to determine whether a relationship exists in other populations. Second, genetic polymorphisms may lead to correlations between the SNPs used for analysis and other traits, resulting in confounding bias that can affect inference. Third, the strength of the IV depends on the sample size of the GWAS. Conducting a large-scale GWAS is necessary to identify additional genetic variations for MR. Fourth, we could not address potential pleiotropy that may have remained undetected, which may impact the perceived credibility of our results. Fifth, the proportion of smokers among males is significantly higher than that among females. However, the data utilized in this study were derived from public databases, making it unsuitable for subgroup analysis of specific factors such as gender. Finally, studies focusing on smoking initiation and atrial fibrillation utilized in this TSMR analysis may have included the same participants. However, we were unable to determine the number of overlapping participants in the datasets, limiting our ability to mitigate potential bias due to sample overlap.