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Involuntary tobacco smoke exposures from conception to 18 years increase midlife cardiometabolic disease risk: a 40-year longitudinal study

Published online by Cambridge University Press:  08 January 2024

Zhongzheng Niu
Affiliation:
Department of Epidemiology and Environmental Health, School of Public Health and Health Professions, The State University of New York at Buffalo, Buffalo, NY, USA
Lina Mu
Affiliation:
Department of Epidemiology and Environmental Health, School of Public Health and Health Professions, The State University of New York at Buffalo, Buffalo, NY, USA
Stephen L. Buka
Affiliation:
Department of Epidemiology, Brown University School of Public Health, Providence, RI, USA
Eric B. Loucks
Affiliation:
Department of Epidemiology, Brown University School of Public Health, Providence, RI, USA
Meng Wang
Affiliation:
Department of Epidemiology and Environmental Health, School of Public Health and Health Professions, The State University of New York at Buffalo, Buffalo, NY, USA RENEW Institute, The State University of New York at Buffalo, Buffalo, NY, USA Department of Environmental and Occupational Health Sciences, School of Public Health, University of Washington, Seattle, WA, USA
Lili Tian
Affiliation:
Department of Biostatistics, School of Public Health and Health Professions, The State University of New York at Buffalo, Buffalo, NY, USA
Xiaozhong Wen*
Affiliation:
Division of Behavioral Medicine, Department of Pediatrics, Jacobs School of Medicine and Biomedical Sciences, The State University of New York at Buffalo, Buffalo, NY, USA
*
Corresponding author: Xiaozhong Wen; Email: xiaozhongwen@hotmail.com
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Abstract

Few population studies have sufficient follow-up period to examine early-life exposures with later life diseases. A critical question is whether involuntary exposure to tobacco smoke from conception to adulthood increases the risk of cardiometabolic diseases (CMD) in midlife. In the Collaborative Perinatal Project, serum-validated maternal smoking during pregnancy (MSP) was assessed in the 1960s. At a mean age of 39 years, 1623 offspring were followed-up for the age at first physician-diagnoses of any CMDs, including diabetes, heart disease, hypertension, or hyperlipidemia. Detailed information on their exposure to environmental tobacco smoke (ETS) in childhood and adolescence was collected with a validated questionnaire. Cox regression was used to examine associations of in utero exposure to MSP and exposure to ETS from birth to 18 years with lifetime incidence of CMD, adjusting for potential confounders. We calculated midlife cumulative incidences of hyperlipidemia (25.2%), hypertension (14.9%), diabetes (3.9%), and heart disease (1.5%). Lifetime risk of hypertension increased by the 2nd -trimester exposure to MSP (adjusted hazard ratio: 1.29, 95% confidence interval: 1.01–1.65), ETS in childhood (1.11, 0.99–1.23) and adolescence (1.22, 1.04–1.44). Lifetime risk of diabetes increased by joint exposures to MSP and ETS in childhood (1.23, 1.01–1.50) or adolescence (1.47, 1.02–2.10). These associations were stronger in males than females, in never-daily smokers than lifetime ever smokers. In conclusion, early-life involuntary exposure to tobacco smoke increases midlife risk of hypertension and diabetes in midlife.

Type
Original Article
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
© The Author(s), 2024. Published by Cambridge University Press in association with The International Society for Developmental Origins of Health and Disease (DOHaD)

Introduction

Heart disease, stroke, and diabetes, together known as cardiometabolic disease (CMD), cause 18 million deaths in the globe each year, more than any other causes. 1 Although CMD is mainly diagnosed in a later life, cumulating evidence has suggested that its disease process initiates in early life. Reference Ross and Glomset2,Reference Ross and Glomset3 This early initiation has also been associated with various early-life environmental exposures. Reference Bateson, Barker and Clutton-Brock4 Of particular interests are involuntary exposures to tobacco smoke, including in utero exposure to maternal smoking during pregnancy (MSP) and environmental tobacco smoke (ETS) exposure after birth. Reference Raghuveer, White and Hayman5 In utero exposure to MSP has been associated with low birth weight, childhood obesity, and decreased kidney volume, while ETS exposure after birth may further potentiate the risk of diabetes and hypertension. Reference de Jonge, Harris and Rich-Edwards6Reference West, Juonala and Gall10 However, there is little research directly linking early-life involuntary exposure to tobacco smoke with later-life CMD, mostly due to the challenge of long follow-up. Reference Raghuveer, White and Hayman5,Reference McConnell, Shen and Gilliland11 In addition, MSP and ETS are correlated, because mothers who smoked during pregnancy are likely to continue smoking after delivery and thus expose the offspring to ETS, generating a “double-hit”. Reference Tong, Dietz and Morrow12 However, whether early-life exposure to the “double-hit” of both MSP and ETS may have additive effect on CMD remains unknown.

We a prior selected sex and offspring’s own smoking as potential effect modifiers. Previous studies have suggested sex differences in the susceptibility of exposure to maternal stressors during pregnancy where females were more likely to be protected by estrogens and earlier linear growth compared to males. Reference Osmond, Barker and Winter13 In addition, cardiovascular responses to maternal stressors during pregnancy (e.g., undernutrition) and early-life stressors (emotional and physical stimuli) differ by sex, where males had higher resting vascular resistance while females had higher cardiac sympathetic activation. Reference Jones, Beda and Osmond14 Moreover, risk of midlife CMD is also higher in males than females. Reference Virani, Alonso and Aparicio15 Similarly, one’s own smoking has been an established risk factor for CMD. Reference Virani, Alonso and Aparicio15,Reference Benjamin, Muntner and Alonso16 Thus, we also stratified the analyses by adult smoking status to explore potentially different pathways with or without adult smoking.

We analyzed data from a 40-year longitudinal study, the New England Family Study (NEFS), that collected detailed information on MSP in the 1960s and then followed the adult offspring in the 2000s for CMD occurrence and a detailed history of ETS exposure from birth to 18 years. Reference Gilman, Martin and Abrams17,Reference Niswander and Gordon18 Although the prevalence of smoking was much higher in the 1960s (over 50%) compared to the present (about 10%), Reference Cornelius, Loretan and Jamal19 the biological mechanism underlying the association of early-life involuntary exposure to smoking with midlife CMD risk should not change with time substantively, and therefore findings based on this historical cohort remain relevant, especially to test the developmental origins of health and disease (DOHaD) hypotheses. We hypothesized that (1) the risk of CMD increased with in utero exposure to MSP and early-life exposure to ETS, and (2) the increased risk could be more striking when exposed both in utero and in early life, among males or active smokers.

Methods

Study population

Participants were offspring born to mothers who were enrolled at two New England sites (Boston, MA and Providence, RI, total N = 15,721) of the Collaborative Perinatal Project (CPP) from 1959 to 1966. The CPP was a multicenter, national-wide birth cohort study (N = 55,908) on prenatal and perinatal factors of children’s health. Reference Niswander and Gordon18 Detailed information on mothers’ health and behaviors was collected, including their smoking habits in each trimester of pregnancy. In 2001–2004, a follow-up project, the New England Family Study (NEFS), randomly selected 4579 adult offspring born to mothers of the CPP to fill a screening questionnaire, among whom 3121 mailed back the questionnaire. Eventually, 1674 finished the follow-up questionnaire and 1623 with complete information made to the final analytical sample. Compared to the remaining unselected 11,142 who were also born to mothers of CPP at New England sites, the final analytical sample had similar distributions of maternal smoking and other key covariates, such as maternal age at delivery. Reference Gilman, Martin and Abrams17,Reference Paradis, Shenassa and Papandonatos20 There is a higher proportion of female offspring in the NEFS than in the original cohort, possibly due to a lower response rate in males than in females, as has been seen in other studies. Reference Otufowora, Liu and Young II21 All participants provided informed consent at enrollment. The study was reviewed by Institutional Review Boards at Harvard School of Public Health, Brown University, and University at Buffalo.

Maternal smoking during pregnancy

At each prenatal visit, mothers reported whether they smoked cigarettes since the last visit and, if so, the average number of cigarettes smoked per day. For women enrolled in the second (49.4%) or third (18.6%) trimester, their smoking behaviors before enrollment were imputed using the information collected from the earliest prenatal visits. A validation study demonstrated strong agreement (Kappa = 0.83) between serum cotinine and self-reported smoking in a subsample of the CPP participants. Reference Klebanoff, Levine and Clemens22 We converted the number of cigarettes to packs (1 pack = 20 cigarettes) in each trimester as the trimester-specific quantity of in utero exposure to MSP and then averaged over the three trimesters as the whole pregnancy exposure in further analyses.

Environmental tobacco smoke exposure

At the adult follow-up telephone interview, trained staff used a questionnaire to assess each participant’s exposure to ETS in early life. The questionnaire had similar questions for two periods: birth to 10 years (childhood) and 11–18 years (adolescence). Participants answered if they lived together with the following potential caretakers: the biological mother, biological father, other female, and other male caregivers, in each year from birth to 18 years. If they lived together, participants further answered ‘Did your (fill in type of caretaker) ever smoke (cigarettes, pipes, cigars) in your home for a year or longer? If YES, how old were you then. (circle all ages that apply, from birth to 1, then each year from 1 to 18).’ Participants also answered ‘About how many CIGARETTES did your (fill in type of caretaker) smoke per day, on average? (1 pack = 20 cigarettes). (Selection from None, 0.5, 1, 1.5, 2 or more packs); During these years that your (fill in type of caretaker) smoked in the home, about how many hours per day were you exposed to his/her smoke, on average? (Fill in exact hours).’. The questionnaire also included other questions to help the participant to recall each smoker’s behavior: if family photos from childhood/adolescence often showed the smoker’s smoking, and in which situations the smoker smoked when the participant was around (e.g., during meals and while driving). In addition to the four possible caregivers listed above, a fifth smoker’s smoking behavior and the relationship with the participant were asked in a similar manner, but the information was not included in the analyses because very few participants (<1%) reported a fifth smoker. Because the pack of smoked cigarettes and the hour of exposure to each smoker were asked for the whole periods in childhood and adolescence, we calculated the average ETS exposure quantity (hour-pack) from each caregiver in each of these two periods using the following formula: ETS quantity = (number of years smoked in the home * average pack per day smoked * hours per day exposed)/year in the period. We then combined the ETS quantity in hour-packs/day across all caregivers as the final ETS exposure in childhood and adolescence, respectively. Retrospective recalling of childhood and adolescence exposure to ETS has been widely used in life course studies, with high agreement in the status, duration, and severity of ETS exposure between participants’ recall and the responses from their surrogates (e.g., parents). Reference Cummings, Markello and Mahoney23 In addition, the questions that we used have been validated and recommended to assess ETS exposure in this field. Reference Avila-Tang, Elf and Cummings24

Cardiometabolic disease

At the adult follow-up, participants filled a questionnaire on their health status and medical history. Participants were asked if a doctor had ever told them that they had any of the following CMDs: high blood pressure (hypertension), high cholesterol (hypercholesterolemia), stroke, heart attack, angina, congestive heart failure, or diabetes. Considering the severity of the diseases and the small number of cases, we combined stroke, heart attack, angina, coronary heart disease, and congestive heart failure into one group named “heart disease”. For hypertension and diabetes, a second question was asked about whether the condition was only diagnosed during pregnancy. Pregnancy-induced hypertension and gestational diabetes were not considered as CMD diagnoses in current analyses. If a CMD was reported, further questions were asked on the age at the first diagnosis and current medication use.

Covariates

In the CPP, mothers reported their race and perinatal characteristics, including age at prenatal enrollment (year), education (<9th, 10th–12th, and >12th grades), marital status (married/other), and parity. We calculated their pre-pregnancy body mass index (BMI, Kg/m2) using self-reported pre-pregnancy weight and height at prenatal visits in the original CPP. Birth weight (grams) and gestational duration (weeks) were obtained from birth records. At the adult follow-up, the offspring participants reported their age, race, and current active smoking status (yes/no).

Statistical analyses

We used frequencies and proportions to describe the distributions of categorical variables and Chi-squared tests to compare the distribution of categorical variables by maternal smoking status during pregnancy (yes/no). We used the exact probability test to compare the lifetime incidence rates of CMD by maternal smoking status during pregnancy. Reference Martin and Austin25 The potentially non-linear relationship between MSP or ETS exposure and CMD risk was tested by incorporating a spline term of exposure for the risk of CMD in a generalized additive model. Given none of the spline terms reached statistical significance (Supplemental Table S1), we treated MSP or ETS as a continuous variable. We used Cox proportional hazards regression models to estimate the hazard ratios (HRs) and 95% confidence interval (CI) for incident hypertension, hypercholesterolemia, diabetes, and heart disease by each pack/day increment of in utero exposure to MSP and by each hour-pack/day increment in ETS exposure in childhood and adolescence. Survival time was based on the duration from birth to the age at the first health-professional diagnosis or age at the adult follow-up if none of these conditions was diagnosed. For ETS exposure, the reported HRs were scaled for an interquartile-range increase in hour-pack/day among those with exposure to facilitate interpretation, i.e., 9.8 hour-pack/day for childhood ETS exposure and 8.0 hour-pack/day for adolescence ETS exposure. To avoid reverse causality, CMD cases that were diagnosed before 18 years were excluded from the analyses (N = 24 for hypercholesterolemia, 17 for hypertension, and 7 for diabetes). No cases of heart disease occurred before 18 years. We checked the proportional hazards assumption by testing the statistical significance of the exposures’ interactions with the survival time.

The analyses included a set of potential confounders based on the literature review and the hypothesized causal structure analyses using directed acyclic graphs (Supplemental Figures S1S2). Reference Greenland, Pearl and Robins26 Different sets of confounders have been identified according to the exposure period. A general set of confounders was adjusted for all exposure periods, including study site, maternal age, race, education, marital status, offspring’s sex and race. For in utero MSP exposure, pre-pregnancy BMI and parity were further adjusted. For ETS exposures in childhood or adolescence, maternal smoking during the whole pregnancy (average pack/day) and birth weight were further adjusted; and for ETS exposure in adolescence, both in utero MSP exposure over the whole pregnancy and ETS exposure in childhood were further adjusted. We deemed offspring current smoking as a potential mediator on the path from exposure to outcome, therefore we did not adjust for adult current smoking, which could underestimate the total effect.

In addition to adjusting for in utero exposure in the analyses of childhood and adolescent exposure, we also estimated the potential effect modification of in utero exposure. Specifically, we calculated the P-value for the product term of in utero exposure during the whole pregnancy (pack/day) and ETS exposure (hour-pack/day) in childhood and adolescence. We further calculated the stratum-specific hazard ratio of childhood and adolescent ETS exposure by maternal smoking status during pregnancy (yes/no).

We a priori selected two potential effect modifiers, i.e., offspring’s sex and own active smoking behavior, giving their important roles in the CMD risk. Reference Arnett, Blumenthal and Albert27 Specifically, we calculated the P-value for interaction between sex and in utero, childhood, or adolescence exposure; and estimated the stratum-specific hazard ratio by offspring sex (male/female). Similarly, we calculated the stratum-specific hazard ratio by offspring’s smoking status (ever/never-daily smoking).

For the sensitivity analyses to assess the potential dose-response relationship, we restricted the analytic sample by excluding those without MSP/ETS exposure in each period.

All analyses were conducted in SAS 9.4 (Cary, NC).

Results

As shown in Table 1, mothers were enrolled at an average age of 25 years (SD 5.8). Most of the mothers were White (86.4%), had 10th–12th-grade education (63.7%), were married (89.9%), and had normal BMI (18.5–25 Kg/m2, 73.4%). The median daily cigarette consumption was 3.0 cigarettes in the first trimester and increased to 3.5 and 3.8 cigarettes in the second and the third trimester, respectively. The prevalence of low birth weight (<2500 g) and preterm birth (<37 weeks) were 8.1% and 7.9%, respectively. The offspring were exposed to ETS for a median of 4.0 (Q1, Q3: 0.3, 10.0) hour-packs/day in childhood and 2.0 (Q1, Q3: 0, 7.5) hour-packs/day in adolescence. Offspring were followed-up at an average age of 39.1 years (SD: 1.9), 40.7% of them were males, and 50.2% were daily smokers. Detailed descriptions and histograms of MSP/ETS exposures are shown in Supplemental Figure S3.

Table 1. Maternal and offspring characteristics in 1623 participants of the NEFS study

As shown in Table 2, risk for hypertension significantly increased by 1.29 times (adjusted HR [aHR], 95% CI: 1.01–1.65) for each pack increment of in utero exposure to MSP in the second trimester. The increased risk was similar in the first (aHR: 1.27, 95% CI: 0.99–1.63) and the third (aHR: 1.23, 95% CI: 0.96–1.28) trimester, although not significant. In utero exposure to MSP in each trimester was also associated with increased risk of diabetes, although not significantly. There is no significant association of in utero exposure to MSP in each trimester with hypercholesterolemia or heart disease.

Table 2. Cox regression model for associations of in utero exposure to maternal smoking with adult cardiometabolic disease

HRs measure the effect of a single pack/day increase in maternal smoking during pregnancy on the hazard of adult cardiometabolic disease. Adjusted HR were controlled for study site, maternal age, race, education, marital status, pre-pregnancy BMI, parity, offspring’s sex and race.

Interquartile range increment of one hour-pack/day in exposure to ETS in childhood (aHR: 1.11, 95% CI: 0.99–1.23) and adolescence (aHR: 1.22, 95% CI: 1.04–1.44) were both associated with hypertension, even after adjusting for in utero exposure to MSP and earlier ETS exposure (for adolescence) (Table 3). When stratified by in utero exposure to MSP, risk of hypertension by both childhood and adolescent ETS exposure remained significant only in those with in utero MSP exposure, although the P-value for interaction was >0.05. Risk of diabetes significantly increased with both childhood (aHR: 1.23, 95% CI: 1.01–1.50) and adolescence (aHR: 1.47, 95% CI: 1.02–2.10) ETS exposure among those with joint in utero exposure to MSP.

Table 3. Cox regression model for associations of childhood and adolescence exposure to ETS with adult cardiometabolic disease

Adjusted HR were controlled for study site, maternal age, race, education, marital status, maternal smoking during pregnancy (average pack/day), offspring’s sex, race and birth weight; For ETS exposure in adolescence, ETS exposure in childhood was additionally adjusted.

* P-interaction tests the significance of the product term of ETS with maternal smoking during the whole pregnancy (yes/no).

a HRs measure the effect of an IQR increase in daily exposure to ETS on the hazard of adult cardiometabolic disease (IQR = 9.8 hour-packs/day for ETS exposure in childhood, 8.0 in adolescence).

In sensitivity analyses in a subsample with any exposure to MSP and ETS (excluding unexposed participants), there was no meaningful changes in the main effect estimation for the association of MSP or ETS exposure with CMD risk (Supplemental Table S2).

There is a significant interaction between sex and both in utero exposure to MSP and childhood ETS exposure with the risk of hypertension (Table 4). For sex-specific analysis, associations of in utero exposure to MSP, childhood and adolescent ETS with hypertension were more striking in males than females. No significant sex differences in the associations were observed for other CMDs.

Table 4. Sex-stratified associations of early-life exposure to in utero maternal smoking or ETS with adult cardiometabolic disease

All models were adjusted for study site, maternal age, race, education, marital status, offspring’s race; for intrauterine exposures, pre-pregnancy BMI, parity were also adjusted; for ETS, maternal smoking during pregnancy (average pack/day) and birthweight, were adjusted; and for ETS exposure in adolescence, ETS exposure in childhood was additionally adjusted.

a HRs measure the effect of a single pack increase in maternal smoking during pregnancy or an IQR increase in daily exposure to ETS on the hazard of adult cardiometabolic disease (IQR = 9.8 hour-packs/day for ETS exposure in childhood, 8.0 in adolescence).

There is a significant interaction between adult offspring’s own smoking status (ever/never-daily smoking) and both in utero exposures to MSP and ETS exposure with the risk of diabetes (Table 5). Among never-daily smokers, both in utero exposure to MSP in the first (aHR: 2.23, 95% CI: 1.18–4.22) or the second (aHR: 2.35, 95% CI: 1.24–4.47) trimester and ETS exposure in childhood (aHR: 1.38, 95% CI: 1.12–1.71) or adolescence (aHR: 1.45, 95% CI: 1.01–2.08) were associated with increased risk of diabetes. The associations with CMDs were all non-significant among ever-daily smokers.

Table 5. Offspring smoking-stratified associations of early-life exposure to in utero maternal smoking or childhood/adolescence ETS with adult cardiometabolic disease

All models were adjusted for study site, maternal age, race, education, marital status, offspring’s sex, race, and age at adult follow-up; for intrauterine exposures, pre-pregnancy BMI, parity, birth weight category, preterm, or post-term were also adjusted; for ETS, maternal smoking during pregnancy (average pack/day) and birth weight were also adjusted; and for ETS exposure in adolescence, ETS exposure in childhood was additionally adjusted.

a HRs measure the effect of a single pack increase in maternal smoking during pregnancy or an IQR increase in daily exposure to ETS on the hazard of adult cardiometabolic disease (IQR = 9.8 hour-packs/day for ETS exposure in childhood, 8.0 in adolescence).

Discussion

In a 40-year longitudinal cohort, we found involuntary exposures to tobacco smoke from conception to adolescence were associated with increased risk of hypertension in midlife. The risk of hypertension was even higher, and the risk of diabetes was also increased with joint exposure to both in utero MSP and childhood/adolescent ETS. Such associations were overall stronger among males than females and among never-daily smokers than ever-daily smokers. We did not find any significant association of early-life involuntary exposure to tobacco smoke with midlife hyperlipidemia or heart disease.

Our findings on the association of in utero exposure to MSP with increased risk of hypertension in adulthood were consistent with some previous studies, Reference de Jonge, Harris and Rich-Edwards6,Reference Cupul-Uicab, Skjaerven and Haug28 but not all of them. Reference Dior, Lawrence and Sitlani29,Reference Kataria, Gaewsky and Ellervik30 A meta-analysis that combined four previous studies found high study heterogeneity (I 2 > 95%, P < 0.0001) and a non-significant combined association, suggesting critical roles of study design (prospective vs. retrospective) and exposure assessment accuracy in elucidating the association of in utero exposure to MSP with adult hypertension. Reference Kataria, Gaewsky and Ellervik30 Our study provides important contribution in this aspect given our prospective collection of MSP, which was not likely to be biased by offspring’s health outcomes decades later. We also found the point estimates were generally comparable across the three trimesters of pregnancy, suggesting the whole pregnancy could be important for the association of maternal smoking with future risk of hypertension in offspring. Note in our 1960s pregnancy cohort, only a small proportion (<5%) of mothers changed smoking behavior over pregnancy. Research using recent cohorts in which more women quit smoking at various gestational weeks is needed to further examine whether sensitive windows exist.

The risk of hypertension also increased with exposure to ETS postnatally from birth to 18 years. In previous studies with postnatal ETS exposure, Reference West, Juonala and Gall10,Reference Gall, Huynh and Magnussen31 in utero exposure status was often unknown. Because pregnant women who smoked during pregnancy were likely to continue smoking after giving birth, children exposed to in utero maternal smoking were also more likely to be exposed to postnatal ETS. In utero exposure could potentially confound the association of postnatal ETS exposure with adult hypertension risk. In the present study, we first adjusted for in utero exposure to maternal smoking when postnatal ETS was the main exposure and found no meaningful changes in the point estimate of the association between ETS and CMD. Further, when the analyses on postnatal ETS were stratified by in utero exposure, the increased risk of hypertension mostly remained among offspring with in utero exposure but not among those without. These findings suggested the importance of accounting for earlier exposure when assessing the effect of postnatal ETS exposure.

In addition to hypertension, the risk of diabetes also increased when the offspring were jointly exposed to in utero maternal smoking and postnatal ETS. To the best of our knowledge, we are the first to report such a possible synergetic effect, although the individual effect has been reported previously. Reference Dior, Lawrence and Sitlani29,Reference Juonala, Magnussen and Venn32 Two previous studies reported association of in utero exposure to maternal smoking with the increased risk of diabetes (including type 2 and gestational diabetes). Reference Dior, Lawrence and Sitlani29,Reference Juonala, Magnussen and Venn32 Another two studies showed early-life ETS exposure was associated with risk factors of diabetes, including higher BMI and increased risk of obesity. Reference McConnell, Shen and Gilliland11,Reference Jaakkola, Rovio and Pahkala33 Other than hypertension and diabetes, we also found a non-significantly increased risk of heart disease with ETS exposure in male adolescents, likely because the number of heart disease was small. Nevertheless, our findings were consistent with previous retrospective studies that reported associations of childhood or adolescence ETS exposures with increased carotid artery intima-media thickness, Reference Chen, Yun and Fernandez34 brachial artery flow-mediated dilatation, Reference Juonala, Magnussen and Venn32 carotid atherosclerotic plaque, Reference West, Juonala and Gall10 and risk of CHD and stroke. Reference Pistilli, Howard and Safford35

We found offspring’s sex could modify the association of in utero and postnatal ETS exposure with CMD. One possible explanation for this sex difference could be the protective effects of hormones and the healthier lifestyle in the female. Reference Salerni, Di Francescomarino and Cadeddu36 We also found offspring’s own lifetime daily smoking status modified the association of in utero and postnatal ETS exposure with midlife risk of hypertension and diabetes. Although adult smoking could be a mediator on the path from MSP/ETS exposure to midlife CMD, our findings on the significant associations among never-daily smokers suggest the underlying mechanisms may be independent of adult smoking. This is also supported by the insignificant associations among ever daily smokers. Another possible explanation for such effect modification is that smokers were less likely to participate research studies, Reference Seltzer, Bosse and Garvey37 especially those with CMD. Therefore, interpretation of our findings among smokers should take extra caution.

A few plausible mechanisms may explain the association of in utero exposure to maternal smoking with adult hypertension, such as upregulated maternal blood pressure tone, nicotine and other harmful substances, placental dysfunction that induce oxidative stress, inflammation, arterial endothelium injury, and epigenetic modification. Reference Geelhoed, El Marroun and Verburg38Reference Rogers40 Similarly, early-life exposure to ETS may potentiate the vulnerability of children because children have a higher respiration rate relative to body size than adults, partially developed detoxification mechanisms, and sensitive cardiovascular and endocrine system development during the rapid growth period. Reference Raghuveer, White and Hayman5,Reference Groner, Huang and Nagaraja41

Cumulative evidence has suggested that a small disturbance of the cardiovascular system in early life could be amplified over time and subsequently accelerate the development of cardiovascular disease in later life. Reference Allen, Siddique and Wilkins42,Reference Kishi, Teixido-Tura and Ning43 Therefore, protecting children from involuntary tobacco smoke is an important primordial prevention strategy of cardiovascular disease. Banning smoking in public places mitigates ETS in the general population, Reference Frazer, Callinan and McHugh44 but studies also reported an increasing trend of ETS exposure in children, possibly because their parents switched to smoking more at home. Reference Ho, Wang and Lo45,Reference Homa, Neff and King46 Other intervention strategies such as parental smoking cessation, smoke-free home, and indoor air filtration warrant consideration. Reference Rice, Brigham and Dineen47,Reference Wen, Eiden and Justicia-Linde48

This study was strengthened by a comprehensive measure of involuntary tobacco smoke exposure from conception to 18 years and the longitudinal follow-up. This study had several potential limitations. As reported previously, female offspring were over-represented in the adult follow-up, thus could introduce a potential collider bias. Reference Paradis, Shenassa and Papandonatos20 However, controlling sex as a confounder and stratification analyses by sex could potentially reduce this bias. Information on maternal smoking during pregnancy was self-reported, although measurement error was unlikely to differ by midlife CMDs substantially. Information on ETS exposure was recalled by the adult offspring, thus recall bias might exist given they were aware of their CMD diagnoses. This is a common limitation among life course studies. Prior publications indicated that use of recommended questions and survey methods could yield reasonably accurate information on ETS exposure years and the number of exposure pack-years. Reference Avila-Tang, Elf and Cummings24 Our questionnaire utilized these recommended questions and there were additional efforts such as using family photos to facilitate participants to recall early-life exposure. CMD status and age at first diagnosis were self-reported and thus subject to measurement errors. Previous validation studies suggested an acceptable level of reliability of self-reported CMD outcomes in the US population. Reference Barr, Tonkin and Welborn49,Reference Bergmann, Byers and Freedman50 Residual confounding might exist given potential measurement errors in some controlled confounders such as time-varying socioeconomic status. Shared environment could affect both MSP/EST and offspring CMD risk. Although we have adjusted key factors that could reflect some aspects of home and neighborhood environment (e.g., study site, education, age, marital status, race), residual confounding by other factors such as physical activity and diet was not adjusted. We did not adjust for multiple comparisons given that our analyses were hypothesis-driven. Reference Rothman51 Thus, we could not rule out the possibility of false positive results. Although the overall sample size was fairly large, the number of CMD cases was modest, given the relatively young age (∼40s) of adult offspring.

Conclusion

In summary, we found in utero exposure to maternal smoking during pregnancy as well as exposure to ETS in childhood and adolescence might increase midlife risk of hypertension. In addition, joint exposure to both maternal smoking during pregnancy and ETS in childhood and adolescence might increase the risk of diabetes. Males and never-daily smokers seemed to have even higher risk of midlife CMD if they were exposed to tobacco smoke in early life. Future studies are needed to replicate our findings.

Supplementary material

The supplementary material for this article can be found at https://doi.org/10.1017/S2040174423000375

Acknowledgments

This work was supported by the American Heart Association (AHA) pre-doctoral fellowship awarded to Zhongzheng Niu (Grant number: 20PRE35120245). We acknowledge the participants and other collaborators from the Early Determinant of Health Study and the New England Family Study. Dr. Wen’s time effort was supported through the Health Resources and Services Administration (HRSA) of the US Department of Health and Human Services (HHS) under R40MC31880 entitled “Socioeconomic disparities in early origins of childhood obesity and body mass index trajectories”; Clinical and Translational Science Award Pilot Study support from National Center for Advancing Translational Sciences, National Institutes of Health (NIH) grant UL1TR001412; and R21 exploratory research support from the Eunice Kennedy Shriver National Institute of Child Health and Human Development, NIH grant R21HD091515 (all awarded to Xiaozhong Wen). The information, content and/or conclusions are those of the author and should not be construed as the official position or policy of, nor should any endorsements be inferred by AHA, NIH, HRSA, HHS or the US Government. The sponsors had no role in writing the manuscript or the decision to submit it for publication.

Author contribution

Zhongzheng Niu: Conceptualization, Methodology, Software, Formal analysis, Data Curation, Writing – Original Draft, Review & Edit; Lina Mu: Conceptualization, Methodology, Writing – Review & Edit, Supervision; Stephen L. Buka: Conceptualization, Methodology, Writing – Review & Edit; Eric B. Loucks: Conceptualization, Methodology, Writing – Review & Edit; Meng Wang: Conceptualization, Methodology, Writing – Review & Edit; Lili Tian: Conceptualization, Methodology, Writing – Review & Edit; Xiaozhong Wen: Conceptualization, Methodology, Writing – Review & Edit, Supervision.

Financial support

All authors have no financial relationships relevant to this article to disclose.

Competing interests

All authors have no conflicts of interest to disclose.

Ethical standard

The authors assert that all procedures contributing to this work comply with the Helsinki Declaration of 1975, as revised in 2008, and have been approved by the institutional committees (UB IRB).

References

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Figure 0

Table 1. Maternal and offspring characteristics in 1623 participants of the NEFS study

Figure 1

Table 2. Cox regression model for associations of in utero exposure to maternal smoking with adult cardiometabolic disease

Figure 2

Table 3. Cox regression model for associations of childhood and adolescence exposure to ETS with adult cardiometabolic disease

Figure 3

Table 4. Sex-stratified associations of early-life exposure to in utero maternal smoking or ETS with adult cardiometabolic disease

Figure 4

Table 5. Offspring smoking-stratified associations of early-life exposure to in utero maternal smoking or childhood/adolescence ETS with adult cardiometabolic disease

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