Background
Maternal smoking during pregnancy (MSDP) is associated with numerous adverse outcomes in children. These occur in physical, cognitive, and behavioral domains, including stillbirth [
1], lowered birth weight [
2], childhood asthma [
3], obesity [
4], intelligence [
5], hyperactivity, impulsivity, and conduct problems [
6-
10]. Hypotheses explaining these associations include direct causation (e.g., cigarette components directly damaging developing fetal structures and physiological systems) and shared vulnerability [
11-
13] (e.g., genetic and/or environmental factors increasing rates of MSDP and childhood outcomes). In the realm of childhood behavioral outcomes, consistent findings from multiple prospective observational studies [
14], controlling for plausible confounders, support an argument for a direct causal relationship (e.g., via physiological effects) rather than one solely underpinned by shared vulnerability. This is complimented by animal and human research [
15] demonstrating that MSDP can disrupt neurodevelopment via effects on maturing neurotransmitter systems and brain architecture in regions associated with stress and mood regulation (e.g., the hippocampus [
16] and somatosensory cortex [
17]).
Despite these findings, however, debate continues regarding whether these associations represent causal relationships [
18-
20]. As noted by several authors [
19,
21], MSDP is associated with numerous social and environmental factors (e.g., teenage motherhood, lower maternal education [
11], increased single motherhood [
22]) that influence childhood outcomes. In addition, genes that influence the likelihood of MSDP [
23] may also affect childhood outcomes through maternal-child genetic inheritance. For this reason, studies utilizing quasi-experimental designs [
19] (e.g., siblings with discordant exposures [
24], children from
in vitro fertilization [
25]), predominantly investigating MSDP-childhood externalizing behavior associations, have been undertaken in an attempt to control for unmeasured genetic and environmental confounders. These studies have generally demonstrated attenuation of previously observed MSDP-childhood externalizing behavior associations [
11,
21,
26], though exceptions exist [
27]. Although these approaches have advantages over traditional observational methods [
19] and should be pursued further [
19,
28], they are not without problems [
29]. For example, most studies utilizing discordant sibling and
in vitro fertilization analysis have fewer participants, reducing power to detect true associations. Additionally, discordant samples are a highly selected group [
29], with factors that underpin maternal behavioral change also potentially impacting on childhood outcomes. Further, siblings share on average only 50% of alleles, and therefore differential effects, even ones protective of adverse behavioral outcomes, could be influenced by variations in the other 50% of the inherited alleles. It is therefore unlikely that any single study design will be completely capable of determining causal inference, and a range of approaches will be required. In contrast to the effort expended in exploring the MSDP-childhood externalizing behavior association, fewer studies have explored the association between MSDP and childhood internalizing (anxiety and depressive) behaviors. Those that have investigated this association report both positive and null results [
30-
34]. Limitations of these studies, such as small sample sizes, limited controls for potential confounders, and variable reporting of smoking, amongst other issues, may have contributed to these inconsistencies.
Anxiety and depressive disorders represent a significant contribution to the global burden of disease [
35]. In contrast to many potential risk factors associated with childhood outcomes (e.g., genetics), MSDP is potentially preventable. For this reason, a greater understanding of the MSDP-childhood internalizing behavior association is very relevant for public health. We therefore aimed to build on previous observational studies to investigate the MSDP-childhood internalizing behavior association in a very large and well-characterized prospective study. We tested hypotheses that i) there would be a dose-response effect, such that higher cigarette consumption would be associated with higher internalizing behaviors, and ii) that early pregnancy, as a phase of rapid neurodevelopment, would be a sensitive period. If such an association existed in a large observational study, further investigation via a genetically informed design would have significant merit.
Methods
Study design and participants
The Norwegian Mother and Child Cohort Study (MoBa) is a prospective population-based study that aimed to recruit all women who gave birth in Norway between 1999 and 2009 [
36]. The sampling frame consisted of women who attended for routine ultrasound examination at approximately 17 weeks of gestation. Participation rates were 38.7% of those invited. For this study, information was available on 107,379 children (51.2% boys) who were born to 89,962 participating mothers. Only one child was included when the mother had twins or triplets to reduce problems with dependency between observations. The twin/triplet registered first in the data files was included in the analyses. Of these respondents, we were able to utilize information from 90,040 mother-child pairs where smoking information was available. Mothers completed detailed questionnaires on their health and social status at gestational weeks 17 (questionnaire 1) and 30 (questionnaire 3), and questionnaires on the health and development of their children at multiple time points after birth, including at ages 18 months (questionnaire 5), 36 months (questionnaire 6), and 5 years (questionnaire 7). Of those who agreed to participate in MoBa, the response rates were 94.9% for questionnaire 1 (early pregnancy), 91.0% for questionnaire 3 (late pregnancy), 72.5% for questionnaire 5 (18 month follow-up), 58.5% for questionnaire 6 (36 month follow-up), and 53.0% for questionnaire 7 (5 year follow-up). All participants provided written informed consent, and ethics approval was obtained from The Regional Committee for Medical Research Ethics in South-Eastern Norway.
Exposure: maternal smoking
Mothers self-categorized their current and past smoking status (daily, occasional, or non-smoking) and also reported the number of cigarettes they smoked per day or week, at gestational weeks 17 (‘early pregnancy’) and 30 (‘late pregnancy’). We subsequently dichotomized MSDP (smoking/non-smoking). Mothers who reported smoking any cigarettes per day or week were considered smokers even if they self-categorized as non-smokers. Mothers who provided smoking data from early and late pregnancy were categorized into four groups: smoking only in early pregnancy, smoking only in late pregnancy, smoking throughout pregnancy, and no smoking in pregnancy. We calculated a smoking frequency for all women in early pregnancy by using self-reported daily cigarette consumption or, where not available, dividing self-reported weekly cigarette consumption by seven. These data were used to categorize early pregnancy smokers into four groups: no smoking in early pregnancy, 1 to 9 cigarettes per day, 10 to 19 cigarettes per day, and 20+ cigarettes per day. For the final analysis, we also incorporated data from questionnaire 1 to create a dichotomous variable (yes/no) coding whether women had smoked in previous pregnancies.
Outcome: childhood anxiety and depressive (internalizing) behaviors
Mothers reported their child’s internalizing behaviors by answering questions taken from a condensed 25 question version of The Childhood Behavior Checklist (CBCL) [
37] at ages 18 months, 36 months, and 5 years.
At 18 months, internalizing behaviors were assessed using five items from the internalizing scale of CBCL. Mothers rated on a 1 to 3 scale (1: ‘Not true’, 2: ‘Somewhat or sometimes true’, 3: ‘Very true or often true’) the extent to which their child’s behavior was consistent with the following statements over the previous 2 months:
1.
“Clings to adults or too dependent”
2.
“Gets too upset when separated from parents”
4.
“Disturbed by any change in routine”
The first three items are from the anxious/depressed subscale of the internalizing scale, the fourth from the emotionally reactive subscale, and the fifth from the somatic complaints subscale. A mean score of the five items was computed to represent overall internalizing behaviors.
At 36 months, internalizing behaviors were assessed using nine items from the CBCL, including the five items used at 18 months plus four additional items:
1.
“Constipated doesn’t move bowels”
2.
“Stomach aches or cramps (without medical cause)”
3.
“Vomiting, throwing up (without medical cause)”
4.
“Sudden changes in moods or feelings”
The first three items are from the somatic complaints subscale and the fourth from the emotionally reactive subscale. Again, each item was rated 1 to 3, with a mean score of the nine items computed to represent overall internalizing behaviors.
At 5 years, internalizing behaviors were assessed using 11 items from the CBCL, including the five items used at 18 months plus six additional items:
1.
“Feelings are easily hurt”
2.
“Nervous, high-strung, or tense”
3.
“Self-conscious or easily embarrassed”
4.
“Unhappy, sad, or depressed”
5.
“Stomach aches or cramps (without medical cause)”
6.
“Vomiting/throwing up (without medical cause)”
The first four items were from the anxious/depressed subscale, and last two from the somatic complaints subscale. Each item was rated 1 to 3 (1: ‘Never/rarely’, 2: ‘Sometimes’, 3: ‘Often/typical’) and a mean score of the 11 items was computed to represent overall internalizing behaviors. Mean inter-item correlations were used as estimates of internal consistency. Clark and Watson [
38] argue that the mean inter-item correlation is a useful index of internal consistency for such scales, and recommend that this should be in the range 0.15 to 0.20 for broad constructs. Correlations measured 0.14, 0.13, and 0.16 at 18 months, 36 months, and 5 years, respectively, which were very close to this optimal range. Factor analysis suggested that scale items were best explained by one factor at each time point (results available on request). The CBCL possesses good predictive validity in the Norwegian population [
39], with the Norwegian translation performed by Nøvik [
39,
40] used in this study.
Covariates
We statistically controlled for a series of potential confounding variables, including paternal smoking, maternal education, maternal age, maternal depressive and anxiety symptoms, maternal alcohol consumption, parity, gestational age at birth, and smoking in previous pregnancies. Information on these covariates was obtained from questionnaire 1.
Paternal smoking status was assessed from the fathers’ questionnaire undertaken during pregnancy and dichotomized. Where fathers had not participated, their smoking status was obtained from the mother’s report of their smoking status. Maternal education, utilized as a proxy for socioeconomic status, was assessed by self-report on a 5-point scale (1: ≤9 years of schooling; 2: 1 to 2 years of high school; 3: technical high school or junior college education; 4: 1 to 4 years in college or university; 5: >4 years in college or university). Maternal age in early pregnancy was calculated from information provided by the medical birth register. Maternal depressive and anxiety symptoms were assessed in early pregnancy by self-report of the Hopkins Symptom Checklist 5 (HSCL-5). This scale is a short version of the Hopkins Symptom Checklist 25 (HSCL-25), consisting of five items (“Feeling fearful”, “Nervousness or shakiness inside”, “Feeling hopeless about the future”, “Feeling blue”, and “Worrying too much about things”) rated on a 4-point scale (from not bothered to very bothered). The HSCL-5 correlates strongly with the HSCL-25 [
41,
42]. Cronbach’s alpha in the current sample was 0.80. Maternal alcohol consumption was assessed on a 7-point scale ranging from never to approximately 6 to 7 times a week. Information on parity, child’s gender, and gestational age at birth was obtained from the Norwegian birth register. Mothers provided information on previous pregnancies in questionnaire 1, including the number of previous pregnancies and individual pregnancy details including birth status, breastfeeding status, weight gain during pregnancy, and a dichotomous tick box for “Smoked during pregnancy”.
We performed correlations of all potential confounding factors to assess their relationship between exposures (MSDP characteristics) and outcomes (internalizing behaviors). Due to rules regarding the publication of covariate effects derived from MoBa data we are unable to report correlation data in its entirety. However, of our potential confounding factors, only child gender did not display associations between exposure and outcome and hence was not included in adjusted models.
Statistical analyses
All statistical analyses were performed in SPSS version 20. Only subjects without missing data points were included in each individual analysis. The internalizing scale was log-transformed due to a non-normal distribution (right or positively skewed). A right skewed distribution meant that most respondents reported low levels of internalizing problems – as one would expect in a community sample. The log-transformed scale was then standardized for ease of interpretation. Standardizing allowed comparison of results across analyses using internalizing behavior at different time points as outcomes. ANOVA was performed to compare level of internalizing symptoms among children of mothers who did not smoke to the level of such symptoms among children of the different groups of smokers (e.g., early in pregnancy, late in pregnancy, and throughout pregnancy). The ANOVAs were performed using generalized estimating equations (GEE) with the “sandwich estimator” because of violations of the assumptions of linear models about homogeneity of variance and independence between observations. This estimator provides robust standard errors, especially when N and the number of independent observations are large [
43]. We used an unstructured correlation matrix, as this does not put any
a priori restrictions on the modelling of these correlations, while an independent correlation matrix treats related observations (e.g., siblings) as not more correlated than other observations. Both of these are possible models for siblings’ data and were checked. The one with the best fit to the data was selected – the independent correlation matrix. We interpreted that correlations between siblings’ data were not found to be a major concern in our analyses. GEE was still preferred over usual ANOVA as GEE allows using models with unequal variances in different groups.
Basic descriptive statistics and Pearson correlations of study variables were performed. We used ANOVA models to examine mean differences between MSDP status and childhood internalizing behaviors at 18 months, 36 months, and 5 years. Model A was unadjusted, Model B was adjusted for paternal smoking, maternal alcohol consumption, maternal depressive and anxiety symptoms, maternal age, maternal education level, parity, and gestational age at birth, and Model C further adjusted for retrospective reporting of smoking in previous pregnancies. For each model and subsequent analysis, only participants reporting all required data were included.
We hypothesized that the impact of smoking on internalizing behaviors would be largest in early pregnancy, as this is a time of rapid neurodevelopment [
44]. Therefore, we tested the association between timing of MSDP (early only, late only, throughout, or no smoking) on internalizing behaviors at 18 months, 36 months, and 5 years. We then compared the effect size of smoking only in early pregnancy and smoking only in late pregnancy with the effect size of smoking throughout pregnancy at each time point. We hypothesized that if the effect size of smoking in a particular stage of pregnancy (e.g., early or late) was significantly weaker than the effect size of smoking throughout pregnancy, then this would suggest exposure to MSDP at this stage contributed less to internalizing behavior expression than exposure in the alternative stage of pregnancy. We undertook significance testing between comparing the effects of early pregnancy smoking and late pregnancy smoking with smoking throughout pregnancy by using the standard error (SE) of the difference as advised by Cohen et al. [
45]. This procedure involves calculating the SE of the difference between effect sizes (SE
diff = sqrt (SE
B12 + SE
B22)) and then dividing the difference between effects by this SE
diff to obtain z-scores for the differences.
Further, we tested whether a dose-response relationship existed between daily maternal cigarette consumption in early pregnancy and internalizing behaviors in children at 18 months, 36 months, and 5 years. Linear models comparing three categories of smoking frequency (20+ per day, 10 to 19 per day, 1 to 9 per day) were compared to non-smokers and adjusted for Model B covariates.
Finally, we undertook a subsample analysis of mother-child pairs where information was available regarding smoking in previous pregnancies (n = 65,439) to test MSDP-childhood internalizing behavior associations at ages 18 months, 36 months, and 5 years adjusting for Model B covariates plus smoking in previous pregnancies (Model C).
As discussed in the introduction, MSDP and childhood behavioral outcomes are associated with various genetic and environmental factors that are challenging to measure in observational studies. If uncontrolled, these factors may contribute to spurious associations being observed between MSDP and childhood behaviors. MSDP could influence childhood internalizing behavior expression in two ways. First, MSDP could influence internalizing behavior expression through direct effects on the developing fetus. Second, MSDP and internalizing behaviors could be indirectly linked through a series of shared genetic and environmental factors unrelated to the direct smoking effects. In contrast to MSDP, smoking in a past pregnancy can only be associated with a current child’s internalizing behaviors through effects mediated by shared genetic and environmental factors (as no direct smoking effects are possible). Therefore, given a portion of these indirect factors (e.g., maternal genetics, maternal education level) will be consistent between past and current pregnancies, controlling for this variable is likely to capture some of the indirect effects influencing the MSDP-internalizing behavior association.
Although limitations exist for this approach, by controlling for as many indirect effects as possible, we aimed to approximate the direct impact of MSDP (e.g., by disruption of normal neurodevelopment) on the current child’s internalizing behaviors.
Discussion
In this large, well-characterized prospective study, MSDP was associated with increased internalizing behaviors in children, adjusting for a broad range of possible confounders. A dose-dependent effect of MSDP was evident. There was a larger adverse impact of smoking in early pregnancy than in late pregnancy. Finally, smoking in previous pregnancies was associated with increased internalizing behaviors in subsequently born children at age 18 months, suggesting this variable may capture some portion of residual confounding (e.g., genetic risk, environmental influences) not included in models. Controlling for this variable did not, however, eliminate the observed association.
Our data builds significantly on previous observational literature that has demonstrated inconsistent results. For example, analysis of 2,758 mother-child pairs from the RAINE study revealed that children displayed higher internalizing behaviors between ages 2 and 14 if their mother failed to quit smoking by week 18 of pregnancy (OR 1.55,
P = 0.006), also after controlling for a range of potential confounders [
34]. Children of women who quit prior to gestational week 18, irrespective of their previous smoking levels, did not display different levels of internalizing behaviors than children of non-smoking mothers. These results contrast with outcomes from two large cohorts, where adjustment for confounders eliminated the association. In assessment of The Generation R study (n = 4,680), effects of MSDP on childhood internalizing behaviors at 18 months were completely confounded by adjustment for parental educational level, family income, national origin, parental psychopathology, and child gender [
46]. In the Avon Longitudinal study (n = 4,394), MSDP was not associated with increased internalizing behaviors in children aged 4 years, after controlling for a range of potential confounders including socioeconomic status, parental psychopathology, and alcohol consumption [
32].
The inconsistency in published studies may reflect power issues, varying ages of assessment, and differences in included confounders or populations assessed. For example, the overall risk of behavioral problems in the Generation R Study sample was lower than that of the normal Dutch population, potentially limiting capacity to find small associations [
46]. Our study found the largest impact of MSDP appeared in children aged 18 months, with magnitude of associations diminishing over time. This observation may reflect an evolution from a greater impact of genetic and intrauterine factors immediately after birth, towards an increasing impact of prevailing psychosocial factors on internalizing behavior expression as children grow up. These data are concordant with studies demonstrating positive associations between MSDP and internalizing behaviors when assessing younger (e.g., 1 to 3 years) [
33,
34] but not older (e.g., age >4) [
9,
32,
47] children, although exceptions exist [
30,
46,
48].
Most toxins display a dose-dependent relationship. Our finding of the greatest impact on internalizing behaviors occurring in mothers who smoked 20+ cigarettes per day is therefore concordant with expected patterns. Our data additionally demonstrated the largest effect on childhood internalizing behaviors in those who smoked during early rather than late pregnancy. These findings are consistent with animal models that demonstrate prenatal nicotine exposure is associated with long term increases in anxiety behaviors [
49]. It is hypothesized that increased anxiety behaviors observed in animals exposed to MSDP may at least partially relate to nicotine and other cigarette smoke components directly interfering with normal neurodevelopmental processes
in utero [
16,
50]. Germane to first trimester effects of MSDP, nicotinic acetylcholine receptors are expressed very early (prior to neurulation) in gestation and serve a critical role in facilitating key aspects of neurodevelopment, including neurogenesis, planned apoptosis, and axonal and synaptic growth [
16]. Abnormal activation of these receptors via exogenous nicotine has been demonstrated to interfere with these key neurodevelopmental processes, including in brain regions associated with mood and anxiety control [
17,
51]. These changes appear to be associated with later behavioral problems in animal models, including increased anxiety states [
52], but it is not yet known if this applies to humans [
53].
Despite this, whether our results represent a causal relationship is not yet determined. Causal assumptions from observational data are vulnerable to unmeasured confounding [
18,
26,
28]. Although our observed associations sustained even after statistically (not experimentally) controlling for numerous important confounders, including maternal mental health, alcohol consumption, demographics, socioeconomic status, and paternal smoking, it remains possible that the dose-dependent MSDP-internalizing behavior association may still have resulted from unmeasured and uncontrolled genetic and environmental confounding (e.g., parental genetic factors) [
19,
21]. As genetic or adequate same-sibling data were not available in MoBA, we were unable to undertake a quasi-experimental design that could attempt to control for these genetic and environmental factors. Therefore, we attempted to address potential residual confounding by controlling the observed association for smoking in past pregnancies. We hypothesized that smoking in past pregnancies would act as a proxy that captures some residual genetic and environmental confounding as i) there was an observed positive association between smoking in a previous pregnancy and the current child’s internalizing behaviors after controlling for other included covariates, ii) genetic factors predisposing the mother to MSDP should be consistent across both pregnancies, and iii) many of the environmental factors influencing the likelihood of MSDP not captured through the measured confounding variables should be consistent across past and current pregnancies. Although this approach does not completely control for residual genetic and environmental confounding (e.g., parental genetic influences, changes to environmental circumstances between pregnancies), we believe this approach brings us one step closer to the true relationship. Including this variable into analysis, we found that the strength of association between MSDP in the current pregnancy and childhood internalizing behaviors at age 18 months decreased, but remained significant. Future studies utilizing aforementioned quasi-experimental designs in a large population would be of great benefit in further assessing the role of residual confounding.
Limitations and directions for future research
Although this study has numerous strengths, including longitudinal follow-up of a very large and well-characterized cohort, the results should be interpreted in light of some limitations. The inability to confirm a causal association is common to all observational studies. In addition, our study was limited by maternal self-report of internalizing behaviors and smoking. Although previous investigations demonstrate that self-report of smoking correlates highly with measured cotinine levels in pregnancy [
54], the lack of multiple informants for assessment of childhood internalizing symptoms (e.g., paternal, teacher, or clinician reports) to correlate the maternal reports is a limitation. We were unable to control for numerous paternal factors in addition to postnatal factors, including child-rearing proficiency, rates of breastfeeding [
55], and exposure to environmental cigarette smoke that may have influenced expression of childhood internalizing behaviors. There was loss to follow-up throughout the study that may have distorted the findings, with children lost to attrition mainly having younger and less educated mothers, with higher rates of depression and anxiety symptoms, higher parity, and increased rates of smoking in early pregnancy. Monte Carlo simulations have shown that even though estimates of mean levels are sensitive to selective attrition, estimates of associations between variables are generally robust against selective attrition and that this is true even when non-response is related to unmeasured variables [
56]. Although the MoBa study is a very large cohort and therefore confers substantial power to detect effects, for some analyses, such as those involving later ages of follow-up (e.g., 36 months and 5 years) and the dose dependence analysis (with relatively few mothers reporting certain behaviors, e.g., smoking >20 cigarettes per day), reduced availability of data may have reduced power to detect associations. MoBa utilized condensed versions of the CBCL scale to assess internalizing behaviors, which is a limitation, although factor analysis of the scales suggested that scale items were best explained by a single factor at each time point (results available on request). In addition, reporting of smoking in past pregnancies in Model C was retrospective, introducing the possibility of reporting bias. The MoBa cohort has a relatively low response rate that may represent a potential issue for generalizability to the Norwegian population, although the sample size remains substantial. In a comparison performed between data acquired in MoBa between 2000 and 2006 and data from the Norwegian Medical Birth Registry, maternal participants in MoBa were more likely to be older, less likely to be single, have lower parity, have lower rates of previous stillbirths, and less likely to suffer maternal asthma [
57]. In addition, MoBa participants were more likely to be non-smokers, more likely to use folic acid, and less likely to suffer from gestational diabetes and placental abruption [
57]. Although it is difficult to predict in what way these factors could bias our observations, we believe it is likely these factors (e.g., lower smoking rates) would be more likely to underestimate rather than overestimate associations.
Competing interests
SM, KG, EBK, and SØ declare no conflicts of interest in relation to this work. FJ has received grant/research support from the Brain and Behavior Research Institute, the National Health and Medical Research Council, Australian Rotary Health, the Geelong Medical Research Foundation, the Ian Potter Foundation, Eli Lilly, and the University of Melbourne and has been a paid speaker for Sanofi-Synthelabo, Janssen Cilag, and Eli Lilly. She is supported by an NHMRC Training Fellowship (#628912). JP has received speaker fees from Amgen, Eli Lilly, and Sanofi-Aventis and funding from the Geelong Region Medical Research Foundation, Barwon Health, Perpetual Trustees, the Dairy Research and Development Corporation, the University of Melbourne, the Ronald Geoffrey Arnott Foundation, ANZ Charitable Trust, the American Society for Bone and Mineral Research, Amgen (Europe) GmBH, and the NHMRC. MB has received grant/research support from the NIH, Cooperative Research Centre, Simons Autism Foundation, Cancer Council of Victoria, Stanley Medical Research Foundation, MBF, NHMRC, Beyond Blue, Rotary Health, Geelong Medical Research Foundation, Bristol Myers Squibb, Eli Lilly, Glaxo SmithKline, Meat and Livestock Board, Organon, Novartis, Mayne Pharma, Servier, and Woolworths, has been a speaker for Astra Zeneca, Bristol Myers Squibb, Eli Lilly, Glaxo SmithKline, Janssen Cilag, Lundbeck, Merck, Pfizer, Sanofi Synthelabo, Servier, Solvay, and Wyeth, and served as a consultant to Astra Zeneca, Bristol Myers Squibb, Eli Lilly, Glaxo SmithKline, Janssen Cilag, Lundbeck Merck, and Servier.
Authors’ contributions
SM and KG had full access to all the data in the study and take responsibility for the integrity of the data and the accuracy of the data analysis. SM, KG, and SØ designed the study methodology and performed the statistical analysis. SM, KG, SØ, EBK, FJ, JP, and MB provided expert input into data analysis, interpretation of results, and drafting of the final manuscript. All authors have read and approved the final manuscript for publication.