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Autism risk following antidepressant medication during pregnancy

Published online by Cambridge University Press:  22 May 2017

A. Viktorin*
Affiliation:
Department of Psychiatry, Icahn School of Medicine, Mount Sinai, New York, NY, USA The Seaver Autism Center, Research and Treatment at Mount Sinai, New York, NY, USA Department of Medical Epidemiology and Biostatistics, Karolinska Institutet, Stockholm, Sweden
R. Uher
Affiliation:
Department of Psychiatry, Dalhousie University, Halifax, Nova Scotia, Canada
A. Reichenberg
Affiliation:
Department of Psychiatry, Icahn School of Medicine, Mount Sinai, New York, NY, USA The Seaver Autism Center, Research and Treatment at Mount Sinai, New York, NY, USA
S. Z. Levine
Affiliation:
Department of Community Mental Health, University of Haifa, Haifa, Israel
S. Sandin
Affiliation:
Department of Psychiatry, Icahn School of Medicine, Mount Sinai, New York, NY, USA The Seaver Autism Center, Research and Treatment at Mount Sinai, New York, NY, USA Department of Medical Epidemiology and Biostatistics, Karolinska Institutet, Stockholm, Sweden
*
*Address for correspondence: A. Viktorin, Department of Psychiatry, Icahn School of Medicine, Mount Sinai, One Gustave L Levy Place, Box #1230, New York, NY 10029, USA. (Email: [email protected])
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Abstract

Background

Previous studies have examined if maternal antidepressant medication during pregnancy increase the risk of autism spectrum disorder (ASD) in the offspring, but the results have been conflicting.

Methods

In a population-based cohort of 179 007 children born in 2006 and 2007 and followed through 2014 when aged 7 and 8, we estimated relative risks (RRs) of ASD and 95% confidence intervals (CIs) from Cox regression in children exposed to any antidepressant medication during pregnancy, and nine specific antidepressant drugs. Analyses were adjusted for potential confounders and were conducted in the full population sample, and in a clinically relevant sub-sample of mothers with at least one diagnosis of depression or anxiety during life.

Results

The adjusted RR of ASD in children of mothers who used antidepressant medication during pregnancy was estimated at 1.23 (95% CI 0.96–1.57), and at 1.07 (95% CI 0.80–1.43) in women with a history of depression or anxiety. Analyses of specific antidepressants initially revealed increased RRs of offspring ASD confined to citalopram and escitalopram (RR: 1.47; 95% CI 0.92–2.35) and clomipramine (RR: 2.86; 95% CI 1.04–7.82).

Conclusion

Medication with antidepressants during pregnancy does not appear to be causally associated with an increased risk of ASD in the offspring. Instead, the results suggest that the association is explained by factors related to the underlying susceptibility to psychiatric disorders. Based on these findings, the risk of ASD in the offspring should not be a consideration to withhold treatment with commonly used antidepressant drugs from pregnant women.

Type
Original Articles
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 in any medium, provided the original work is properly cited.
Copyright
Copyright © Cambridge University Press 2017

Introduction

It has been suggested that antidepressant medication in pregnant women may increase the risk of autism spectrum disorder (ASD) in the offspring. This hypothesis has been examined in several studies, yet the results have been mixed; some studies have observed an increased risk (Croen et al. Reference Croen, Grether, Yoshida, Odouli and Hendrick2011; Rai et al. Reference Rai, Lee, Dalman, Golding, Lewis and Magnusson2013; Gidaya et al. Reference Gidaya, Lee, Burstyn, Yudell, Mortensen and Newschaffer2014; Harrington et al. Reference Harrington, Lee, Crum, Zimmerman and Hertz-Picciotto2014; Boukhris et al. Reference Boukhris, Sheehy, Mottron and Bérard2016), and others have not (Hviid et al. Reference Hviid, Melbye and Pasternak2013; Sorensen et al. Reference Sorensen, Gronborg, Christensen, Parner, Vestergaard, Schendel and Pedersen2013; Clements et al. Reference Clements, Castro, Blumenthal, Rosenfield, Murphy, Fava, Erb, Churchill, Kaimal and Doyle2015; Castro et al. Reference Castro, Kong, Clements, Brady, Kaimal, Doyle, Robinson, Churchill, Kohane and Perlis2016; Malm et al. Reference Malm, Brown, Gissler, Gyllenberg, Hinkka-Yli-Salomaki, McKeague, Weissman, Wickramaratne, Artama, Gingrich and Sourander2016).

Pharmacotherapy plays a central role in the management of the depressive illness, and untreated depression has been associated with poor health outcomes in both mothers and offspring (Lecrubier, Reference Lecrubier2001; Marmorstein et al. Reference Marmorstein, Malone and Iacono2004; O'Hara & McCabe, Reference O'Hara and McCabe2013; Meltzer-Brody & Stuebe, Reference Meltzer-Brody and Stuebe2014). With the introduction of selective serotonin re-uptake inhibitors (SSRIs), the last two decades have seen a substantial increase in prescriptions of antidepressant drugs (Olfson & Marcus, Reference Olfson and Marcus2009), also in pregnant women (Andrade et al. Reference Andrade, Raebel, Brown, Lane, Livingston, Boudreau, Rolnick, Roblin, Smith, Willy, Staffa and Platt2008; Bakker et al. Reference Bakker, Kolling, van den Berg, de Walle and de Jong van den Berg2008). Although SSRI antidepressants are typically well tolerated (Cipriani et al. Reference Cipriani, Furukawa, Salanti, Geddes, Higgins, Churchill, Watanabe, Nakagawa, Omori, McGuire, Tansella and Barbui2009), the risk of adverse effects on the developing fetus has not been resolved.

An association between maternal antidepressant medication during pregnancy and offspring ASD could either be due to: (1) a direct effect of the drug or (2) factors that confound the antidepressant treatment and the outcome studied.

Previous reported associations between maternal antidepressant medication during pregnancy and ASD in the offspring have been limited to studies of antidepressant medications as a whole (Croen et al. Reference Croen, Grether, Yoshida, Odouli and Hendrick2011; Rai et al. Reference Rai, Lee, Dalman, Golding, Lewis and Magnusson2013; Sorensen et al. Reference Sorensen, Gronborg, Christensen, Parner, Vestergaard, Schendel and Pedersen2013; Clements et al. Reference Clements, Castro, Blumenthal, Rosenfield, Murphy, Fava, Erb, Churchill, Kaimal and Doyle2015; Castro et al. Reference Castro, Kong, Clements, Brady, Kaimal, Doyle, Robinson, Churchill, Kohane and Perlis2016), or SSRI antidepressants as a whole (Hviid et al. Reference Hviid, Melbye and Pasternak2013; Gidaya et al. Reference Gidaya, Lee, Burstyn, Yudell, Mortensen and Newschaffer2014; Harrington et al. Reference Harrington, Lee, Crum, Zimmerman and Hertz-Picciotto2014; Boukhris et al. Reference Boukhris, Sheehy, Mottron and Bérard2016; Malm et al. Reference Malm, Brown, Gissler, Gyllenberg, Hinkka-Yli-Salomaki, McKeague, Weissman, Wickramaratne, Artama, Gingrich and Sourander2016). The risk of offspring ASD associated with specific antidepressant drugs is still unknown. If the risk is confined to certain drugs, the proportion of mothers treated with these drugs in prior studies may explain the varying results. Furthermore, recent studies indicate that psychiatric disorders share genetic determinants (International Schizophrenia Consortium et al. Reference Purcell, Wray, Stone, Visscher, O'Donovan, Sullivan and Sklar2009; Lichtenstein et al. Reference Lichtenstein, Yip, Bjork, Pawitan, Cannon, Sullivan and Hultman2009; Sullivan et al. Reference Sullivan, Daly and O'Donovan2012; Jokiranta et al. Reference Jokiranta, Brown, Heinimaa, Cheslack-Postava, Suominen and Sourander2013). Pregnant women suffering from a mental illness during pregnancy, for which antidepressants may be prescribed, likely carry genetic susceptibility that could be inherited by the child (Jokiranta et al. Reference Jokiranta, Brown, Heinimaa, Cheslack-Postava, Suominen and Sourander2013). As such, the genetic susceptibility, rather than the medication, may completely or partially explain the increased risk of ASD in children of mothers using antidepressants during pregnancy. Yet, previous studies have not thoroughly examined to what extent the risk of offspring ASD may be influenced by underlying susceptibility to mental illness.

The aim of the study was to examine the association between maternal antidepressant medication during pregnancy and ASD in the offspring, investigating any antidepressant medication, and specific antidepressant drugs. We performed an analysis using one of the most comprehensive databases for offspring ASD and parental disorder and medication data available. This allowed us to investigate specific antidepressant drugs used during pregnancy, and use detailed adjustment for parental psychiatric diagnoses. Moreover, we investigated both the full cohort and a clinically relevant sub-sample of mothers with any diagnosis of depression and/or anxiety in their lifetime.

Methods

Population

A birth cohort based on all live-born children conceived from July 1, 2005 and born in 2006 and 2007 was established by linkage of Swedish National registers using the unique individual Swedish national registration number (Ludvigsson et al. Reference Ludvigsson, Otterblad-Olausson, Pettersson and Ekbom2009). Offspring and mothers were identified in the Swedish Medical Birth Register that covers 99% of all births nation-wide since 1973 and provides information on gestational age at birth that were used to calculate the beginning of pregnancy (Cnattingius et al. Reference Cnattingius, Ericson, Gunnarskog and Kallen1990). In Sweden, 95% of all pregnant women receive early second trimester ultrasonography, which provide the gestational age of the fetus with an error margin of ±7 days (Hogberg & Larsson, Reference Hogberg and Larsson1997). The fathers were identified using the Multi-Generation Register (Ekbom, Reference Ekbom2011). To be included, the children had to have complete information on gestational age at birth and the identity of the father. The study was approved by the Regional Ethics Committee in Stockholm, Sweden.

Exposures

The Swedish Prescribed Drug Register holds information on all dispensed prescription drugs in Sweden since July 1, 2005 along with drug name, prescription- and dispensation dates, and the Anatomical Therapeutic Chemical Classification System (ATC) code (WHO, 2006; Wettermark et al. Reference Wettermark, Hammar, Fored, Leimanis, Otterblad Olausson, Bergman, Persson, Sundstrom, Westerholm and Rosen2007). We identified dispensations of all psychotropic drugs prescribed in Sweden, including antidepressants, anxiolytics, stimulants, mood stabilizers, antipsychotics, and sedatives (online Supplementary Tables S1 and S2). The offspring were classified as unexposed to antidepressants if they were born to mothers without any dispensation of an antidepressant with a medication period overlapping the pregnancy. Since the number of antidepressant dispensations was reduced during pregnancy, compared with prior or after (online Supplementary Fig. S1), it was assumed that a single antidepressant dispensation overlapping pregnancy could represent medication that was halted prior the pregnancy. Therefore, antidepressant-exposed offspring were grouped into those born to a mother with either: (1) one single medication dispensation overlapping the pregnancy or (2) two or more dispensations of antidepressants with medication periods overlapping pregnancy (online Supplementary Fig. S2).

Ascertainment of ASD

The children were followed from birth through 2014 when aged 7 or 8. A clinically ascertained diagnosis of offspring ASD was identified in the Swedish Patient Register (Ludvigsson et al. Reference Ludvigsson, Andersson, Ekbom, Feychting, Kim, Reuterwall, Heurgren and Olausson2011; Sandin et al. Reference Sandin, Schendel, Magnusson, Hultman, Suren, Susser, Gronborg, Gissler, Gunnes, Gross, Henning, Bresnahan, Sourander, Hornig, Carter, Francis, Parner, Leonard, Rosanoff, Stoltenberg and Reichenberg2016). This register includes all inpatient psychiatric admissions since 1973 and all outpatient specialist admissions since 2001, and provides admission dates along with the main and eight secondary diagnosis codes in accordance with the International Classification of Disease (ICD). Autism spectrum disorder was defined by having at least one in- or outpatient specialist care admission between birth and end of follow-up at December 31, 2014 with an ICD-10 code according to: F84.0, F84.1, F84.2, F84.3, F84.4, F84.5, F84.8, or F84.9. The ASD diagnoses in the Swedish Patient Register has previously been validated (Idring et al. Reference Idring, Rai, Dal, Dalman, Sturm, Zander, Lee, Serlachius and Magnusson2012), and published on extensively (Sandin et al. Reference Sandin, Schendel, Magnusson, Hultman, Suren, Susser, Gronborg, Gissler, Gunnes, Gross, Henning, Bresnahan, Sourander, Hornig, Carter, Francis, Parner, Leonard, Rosanoff, Stoltenberg and Reichenberg2016).

Covariates

To adjust for potential temporal trends, the birth date of the offspring was included as number of days from January 1, 2005 to the birth date of the child. Maternal and paternal age at childbirth was categorized into below 20, 20–29, 30–39, and above 40 years of age. Maternal and paternal susceptibility to mental illness were ascertained based on having at least one psychiatric diagnosis in the Swedish Patient Register within several psychiatric disorder sub-groups at any time in life (online Supplementary Table S3). The father's medication with any psychotropic drugs overlapping the pregnancy was also included, as well as mother's dispensations of other psychotropic medication that overlapped the pregnancy.

Statistical analysis

Relative risks (RRs) of ASD and the associated Wald-type two-sided 95% confidence intervals (CIs) were estimated by the hazard ratios from Cox regression models. The Cox regression models were fitted using days since birth as the underlying time scale. Each child was followed from birth until a diagnosis of ASD, death as identified in the Statistics Sweden register of vital statistics, or end of follow-up at December 31, 2014 – whichever came first. The RR of ASD was calculated in: (1) offspring born to mothers with a single-drug dispensation with a medication period overlapping the pregnancy and (2) offspring born to mothers with at least two dispensations with medication periods overlapping the pregnancy, compared with offspring born to mothers without a dispensation with a medication period overlapping the pregnancy.

Analyses were conducted in: (A) the complete sample to provide a public health perspective and in (B) a clinically relevant sub-sample of children born to mothers with at least one diagnosis of depression or anxiety in their lifetime, since most individuals who receive treatment with antidepressants also suffer from those disorders. In this sub-sample, the control group corresponds to mothers who are more likely to be considered for antidepressant treatment, and may share a similar genetic susceptibility of mental illness as the medicated mothers.

First, we examined children of mothers medicated during pregnancy with any type of antidepressant. The RRs of ASD were calculated in a sequence of models with increasing degree of adjustment for potential confounding factors according to: model 1 crude analyses without covariate adjustment; model 2 analyses adjusted for including offspring birthdate, mother's and father's dispenses of other psychotropic medications during pregnancy, and maternal and paternal age; model 3 analyses with additional adjustment for any depressive diagnosis in the mother's life time; and model 4 analyses further adjusted for any diagnosis of specific psychiatric disorder sub-groups in either the mother and/or father's life time. The psychiatric disorder sub-groups included depression, anxiety disorders, schizophrenia, bipolar disorder, substance use disorder, compulsive disorder, attention-deficit hyperactive disorder, ASD, intellectual disability, and any other psychiatric diagnosis (online Supplementary Table S3).

Secondly, we further calculated the RR of ASD among children of mothers treated exclusively with one of the nine most prevalent antidepressants in the sample: sertraline, citalopram and escitalopram, fluoxetine, venlafaxine, paroxetine, clomipramine, amitriptyline and nortriptyline, duloxetine, and mirtazapine, compared with children of mothers not treated with antidepressants during pregnancy. These analyses were adjusted for all included covariates, corresponding to model 4 in the analyses of any antidepressant. For the analyses examining specific drugs, to protect against an inflated error rate as a result of performing many statistical tests, we additionally present multiplicity-corrected p values using the Bonferroni–Holm procedure (Holm, Reference Holm1979).

All tests of statistically significance were done at the nominal 5% level of significance. Data management and statistical analyses were done using SAS 9.4 and STATA/IC 14, respectively.

Sensitivity analyses

The proportional hazards assumption for the Cox regression models was examined using Schoenfeld residuals (Grambsch & Therneau, Reference Grambsch and Therneau1994). To account for potential within-family correlations in the data due to multiple births from the same parents, we used bootstrap techniques (Efron & Tibshirani, Reference Efron and Tibshirani1994). The analyses were separately repeated for the outcome autistic disorder (ICD-10 F84.0). Potential sex specificity of associations was tested by analyses of male and female offspring separately. Analyses were also conducted separately for SSRI antidepressants, non-SSRI antidepressants, and non-antidepressant psychotropic drugs. The role of socioeconomic status was examined by including an analysis adjusted for education length as a potential confounder. To further examine the effect of the underlying disorder susceptibility, we compared: (a) children born to mothers treated with antidepressants during pregnancy (N = 3982), to (b) children born to mothers with no psychotropic medication but diagnosed with: (1) at least one of type psychiatric disorder, (2) at least two psychiatric disorders, or (3) at least three psychiatric disorders according to online Supplementary Table S3.

Results

Table 1 presents descriptive data for the cohort. Among the 180 444 children conceived from July 1, 2005 and born up until December 31, 2007 in the Medical Birth Register, 1437 (0.7%) did not have complete data and were excluded from the statistical analyses. Table 1 presents descriptive statistics for the 179 007 included children and their parents. At least one diagnosis of any psychiatric illness was observed in 47 204 (13.2%) parents. Autism spectrum disorder was observed in 1641 (0.9%) of the children, and among those, 1004 (61.0%) had a diagnosis of autistic disorder. Among the offspring, 2379 (1.3%) were born to a mother with a single antidepressant dispensation with a medication period overlapping pregnancy, and 3982 (2.2%) were born to a mother with at least two antidepressant dispensations with medication periods overlapping pregnancy.

Table 1. Cohort subject characteristics

a A clinically relevant sub-sample consisting of 18 551 children, of which 361 had been diagnosed with autism spectrum disorder. All mothers, both medicated and non-medicated, had at least one diagnosis of depression or an anxiety disorder in their lifetime (online Supplementary Table S3). Thereby, the offspring of mothers with medication during pregnancy is contrasted with offspring of mothers that may share similar underlying factors.

b Children of mothers with no antidepressant dispensation with a medication period overlapping pregnancy.

c Children of mothers with at least two antidepressant dispensations with medication periods overlapping pregnancy (online Supplementary Fig. S1 examples A1 and A2).

d Children of mothers with a single antidepressant dispensation with a medication period overlapping pregnancy.

Due to the ambiguity of drug exposure in children to mothers with only a single antidepressant dispensation overlapping pregnancy, the results focus on the children with at least two dispensations overlapping pregnancy, as compared with children without exposure to antidepressants. Results in the offspring of mothers with only a single dispensation overlapping pregnancy are presented in the online supplement (online Supplementary Fig. S3).

Risk of ASD

In the full population sample, the crude RR of ASD in children of mothers with at least two dispensations of antidepressants overlapping pregnancy compared with unexposed children was estimated at 2.46 (95% CI 1.97–3.05). With adjustment for all included potential confounders, the RR was reduced to 1.23 (95% CI 0.96–1.57). In analyses confined to children of mothers with at least one diagnosis of depression or anxiety in their lifetime, the crude RR of ASD in children of mothers with at least two dispensations of antidepressants overlapping pregnancy was estimated at 1.30 (95% CI 0.99–1.71). With adjustment for potential confounders, the RR was reduced to 1.07 (0.80–1.43) (Table 2).

Table 2. Relative risks of autism spectrum disorder due to exposure to any type of antidepressants a

ASD, autism spectrum disorder; CI, confidence interval.

a The sample consists of 179,007 children born during 2006 and 2007, of which 1,641 had been diagnosed with ASD. The figure presents relative risks of ASD and two-sided 95% confidence intervals in children of mothers with at least two dispensations of a specific antidepressant drug overlapping the pregnancy, compared with unexposed children. The analyses are adjusted for all included covariates, as in model 4 in Figure 1.

b The clinical sub-sample consists of 18 551 children, of which 361 had been diagnosed with autism spectrum disorder. All mothers, both medicated and non-medicated, had at least one diagnosis of depression or an anxiety disorder in their lifetime (online Supplementary Table S3). Thereby, the offspring of mothers with medication during pregnancy is contrasted with offspring of mothers that may share similar underlying factors.

c Analyses not adjusted for covariates.

d Analyses adjusted for birthdate, maternal and paternal age, the father's psychotropic medication that overlapped the pregnancy, and the mother's one-time dispensations of psychotropic medication that overlapped the pregnancy.

e Analyses adjusted for the factors listed in footnote d, and for any diagnosis of depression in the mother's lifetime (yes/no) (see online Supplementary Table S3 for specific diagnosis codes).

f Analyses adjusted for the factors listed in footnote d, and for any diagnosis of specific psychiatric disorder sub-groups in either the mother and/or father's life time (yes/no), including depression, anxiety disorders, substance use disorder, bipolar disorder, compulsive disorder, attention deficit hyperactivity disorder, autism spectrum disorder, intellectual disability, schizophrenia, and ‘other psychiatric diagnosis’ (see Supplementary Table S3 for specific diagnosis codes).

Risk of ASD associated with specific medications

In the full population sample, the adjusted RRs of ASD in children of mothers with at least two dispensations of specific antidepressants overlapping pregnancy compared with unexposed children was estimated at 1.35 (95% CI 0.87–2.08) for sertraline, 1.71 (95% CI 1.16–2.51) for citalopram and escitalopram, 1.04 (95% CI 0.53–2.02) for fluoxetine, 1.22 (95% CI 0.54–2.75) for venlafaxine, 1.40 (95% CI 0.52–3.76) for paroxetine, 3.27 (95% CI 1.33–8.00) for clomipramine, 0.59 (95% CI 0.08–4.20) for amitriptyline and nortriptyline, and 1.53 (95% CI 0.38–6.23) for mirtazapine (Table 3).

Table 3. Relative risks of autism spectrum disorder due to exposure to specific antidepressants a

ASD, autism spectrum disorder; N, number of children; CI, confidence interval; NA, not available.

a The sample consists of 179 007 children born during 2006 and 2007, of which 1641 had been diagnosed with ASD. The figure presents relative risks of ASD and two-sided 95% CIs in children of mothers with at least two dispensations of a specific antidepressant drug overlapping the pregnancy, compared with unexposed children. The analyses are adjusted for all included covariates, as in model 4 in Table 2.

b The clinical sub-sample consists of 18 551 children, of which 361 had been diagnosed with ASD. All mothers, both medicated and non-medicated, had at least one diagnosis of depression or an anxiety disorder in their lifetime (online Supplementary Table S3). Thereby, the offspring of mothers with medication during pregnancy is contrasted with offspring of mothers that may share similar underlying factors.

c Multiplicity-corrected p values using the Bonferroni–Holm procedure: Holm (Reference Holm1979). A simple sequentially rejective multiple test procedure. Scandinavian Journal of Statistics 6, pp. 65–70.

Within the sub-sample where both the medicated and non-medicated women had at least one diagnosis of depression or anxiety in their lifetime, the adjusted RRs of ASD in children of mothers with at least two dispensations of specific antidepressants overlapping pregnancy compared with unexposed children was estimated at 1.17 (95% CI 0.71–1.95) for sertraline, 1.47 (95% CI 0.92–2.35) for citalopram and escitalopram, 1.08 (95% CI 0.53–2.21) for fluoxetine, 0.88 (95% CI 0.32–2.38) for venlafaxine, 1.21 (95% CI 0.38–3.80) for paroxetine, 2.86 (95% CI 1.04–7.82) for clomipramine, and 1.00 (95% CI 0.14–7.24) for mirtazapine (Table 3).

None of the analyses examining specific drugs, in the full sample and in the clinically relevant sub-sample, revealed statistically significant p values after multiplicity correction using the Bonferroni–Holm procedure (Holm, Reference Holm1979).

Sensitivity analyses

Inspection of the Schonfeld residuals did not suggest any violation of the proportional hazards assumption (online Supplementary Fig. S4). Analyses confined to specifically SSRI antidepressants, non-SSRI antidepressants, and non-antidepressant psychotropic drugs revealed results quantitatively similar to the analyses of any antidepressant (online Supplementary Fig. S5). Confidence intervals of selected point estimates (RRs) calculated using bootstrap revealed close to identical results as the parametric Wald estimates (online Supplementary Fig. S6). Analyses confined to autistic disorder showed results similar to that of ASD (online Supplementary Fig. S7). Analyses of male and female offspring separately did not reveal any sex-specific association (online Supplementary Fig. S8). The complementary analysis adjusting for education as a marker of socioeconomic status did not affect our results (online Supplementary Fig. S9). Analyses with comparison groups without psychotropic medication, but with increasing number of diagnosed psychiatric diagnoses revealed that the RR of ASD in the offspring was closely correlated with the number of different psychiatric disorders diagnosed in the mothers (online Supplementary Figs. S11 and S12).

Discussion

In this population-based, prospective cohort study of 179 007 children and their parents, we observed an increased RR of ASD in offspring of mothers treated with antidepressant medication during pregnancy compared with offspring of mothers not treated with antidepressants during pregnancy. However, detailed adjustments for confounding by parental psychiatric liability attenuated this risk. Moreover, when the analyses were restricted to mothers ever diagnosed with depression or anxiety, a likely target group for antidepressant medication, the association between antidepressants in pregnancy and ASD were attenuated even further and close to none.

To our knowledge, this is the first study to examine the RR of offspring ASD associated with specific types of antidepressant drugs compared with children unexposed to antidepressants. Among the nine studied drugs, only the SSRI antidepressants citalopram and escitalopram, and the tricyclic antidepressant clomipramine displayed an increased RR of ASD in the offspring. While these findings could suggest that these particular medications may have a causal effect associated with increased risk of ASD in the offspring, these positive associations could also be due to residual confounding. Citalopram and escitalopram have similar mechanisms of action as sertraline and paroxetine, yet only citalopram and citalopram displayed an elevated RR of ASD in the offspring. Furthermore, this increase in RR was modest, not statistically significant in the clinically relevant sub-sample, and not statistically different from the results of the other specific antidepressants studied. The results of the present study strongly suggest that the associations between antidepressant treatment during pregnancy and offspring ASD are gradually attenuated with increasing covariate adjustment. Although the present study adjusts for a broad set of factors that may confound the association, the ability to capture confounding is not complete. Mothers treated with different antidepressant medications may be different in other aspects that the current study cannot adjust for. This is exemplified by clomipramine that is not recommended as a first line of treatment of depression, which therefor may be given to women with a more severe or complex form of depression. Further analysis of this treatment group indeed revealed an increased prevalence of both compulsive disorder and schizophrenia compared with women treated with other antidepressants (online Supplementary Fig. S10).

To further investigate the role of psychiatric disorders in the association between antidepressant treatment during pregnancy and ASD in the offspring, we compared children exposed to antidepressants to children of mothers not using psychotropic medication during pregnancy, but with increasing mean number of psychiatric disorders (online Supplementary Fig. S11). These analyses revealed that a higher mean number of different psychiatric disorders diagnosed during the mothers’ lifetime was correlated with the RR of ASD in the offspring. This was also observed in analyses of specific antidepressant drugs (online Supplementary Fig. S12)

Nevertheless, the relationship between treatment with specific antidepressants during pregnancy and the risk of ASD in the offspring should be examined in additional samples to shed more light on the association and the specific underlying disorders.

Prior research into the association between maternal antidepressant medication during pregnancy and offspring ASD has delivered mixed and inconclusive results (Croen et al. Reference Croen, Grether, Yoshida, Odouli and Hendrick2011; Hviid et al. Reference Hviid, Melbye and Pasternak2013; Rai et al. Reference Rai, Lee, Dalman, Golding, Lewis and Magnusson2013; Sorensen et al. Reference Sorensen, Gronborg, Christensen, Parner, Vestergaard, Schendel and Pedersen2013; Gidaya et al. Reference Gidaya, Lee, Burstyn, Yudell, Mortensen and Newschaffer2014; Harrington et al. Reference Harrington, Lee, Crum, Zimmerman and Hertz-Picciotto2014; Clements et al. Reference Clements, Castro, Blumenthal, Rosenfield, Murphy, Fava, Erb, Churchill, Kaimal and Doyle2015; Boukhris et al. Reference Boukhris, Sheehy, Mottron and Bérard2016; Castro et al. Reference Castro, Kong, Clements, Brady, Kaimal, Doyle, Robinson, Churchill, Kohane and Perlis2016; Malm et al. Reference Malm, Brown, Gissler, Gyllenberg, Hinkka-Yli-Salomaki, McKeague, Weissman, Wickramaratne, Artama, Gingrich and Sourander2016). The present findings may resolve this earlier ambiguity. Our findings of attenuated associations with incremental covariate adjustment are in line with several earlier studies (Hviid et al. Reference Hviid, Melbye and Pasternak2013; Sorensen et al. Reference Sorensen, Gronborg, Christensen, Parner, Vestergaard, Schendel and Pedersen2013; Clements et al. Reference Clements, Castro, Blumenthal, Rosenfield, Murphy, Fava, Erb, Churchill, Kaimal and Doyle2015; Castro et al. Reference Castro, Kong, Clements, Brady, Kaimal, Doyle, Robinson, Churchill, Kohane and Perlis2016; Malm et al. Reference Malm, Brown, Gissler, Gyllenberg, Hinkka-Yli-Salomaki, McKeague, Weissman, Wickramaratne, Artama, Gingrich and Sourander2016). The present findings are, however, at odds with number of previous studies that report statistically significant associations. A study of 1054 Canadian children with ASD (Boukhris et al. Reference Boukhris, Sheehy, Mottron and Bérard2016) reported an unadjusted RR of ASD following SSRI treatment (RR = 2.27; 95% CI 1.48–3.46) that were partially attenuated after adjustments for factors, including maternal history of depression (RR = 1.75; 95% CI 1.03–2.97). Similarly sized RRs have also been reported in a Californian sample of 298 children with ASD (RR = 2.2; 95% CI 1.2–4.3) (Croen et al. Reference Croen, Grether, Yoshida, Odouli and Hendrick2011), in a Danish sample of 5215 children with ASD (adjusted RR = 1.8; 95% CI 1.4–2.3) (Gidaya et al. Reference Gidaya, Lee, Burstyn, Yudell, Mortensen and Newschaffer2014), in a US study of 421 male cases with ASD (adjusted RR = 2.91; 95% CI 1.07–7.93) (Harrington et al. Reference Harrington, Lee, Crum, Zimmerman and Hertz-Picciotto2014), and in a Swedish study of 4429 cases with ASD (RR = 3.34; 95% CI 1.50–7.47) (Rai et al. Reference Rai, Lee, Dalman, Golding, Lewis and Magnusson2013).

The discrepancies between the results of previous studies and the present study could be due to several factors. If the present findings of different psychiatric disorder profiles in mothers treated with specific antidepressants (online Supplementary Figs. S11 and S12) was comparable in previous studies, the proportion of these specific antidepressant drugs could explain the mixed results in previous studies. However, the limited adjustment for the parents’ mental illnesses in previous studies may also explain the discrepancies.

Strengths of the study include a large prospective population-based sample of children and their parents with close to complete healthcare data coverage. Any estimate of prevalence of ASD is highly dependent on the birth year, follow-up time, and sex distribution in the sample, still our estimates agree well with other studies in the Nordic countries and in the USA (Idring et al. Reference Idring, Rai, Dal, Dalman, Sturm, Zander, Lee, Serlachius and Magnusson2012; Sandin et al. Reference Sandin, Schendel, Magnusson, Hultman, Suren, Susser, Gronborg, Gissler, Gunnes, Gross, Henning, Bresnahan, Sourander, Hornig, Carter, Francis, Parner, Leonard, Rosanoff, Stoltenberg and Reichenberg2016). Data from a healthcare system with equal access limit the risk of selection biases. Inclusion of children born during a limited period reduces potential confounding by factors that may vary over time. Examination of any diagnosis of mental illness in the parents’ lifetime allowed detailed adjustment for confounding due to, e.g., genetic liability. The requirement of at least two dispensations overlapping the pregnancy further increased the specificity of the exposure. Furthermore, supplementary analyses of antidepressants divided into specifically SSRI antidepressants and non-SSRI antidepressants, and non-antidepressant psychotropic drugs all revealed similar findings, lending further support to the interpretation that the mental illness confounds the association between maternal antidepressant medication during pregnancy and increased risk of ASD in offspring.

However, the findings should also be interpreted in light of some limitations. Overall, our study summarizes the results of a multitude of statistical tests, which always increase the risk of erroneous rejection of a specific hypothesis. When applying the Bonferroni–Holm procedure in the comparison of specific drugs compared with ‘no treatment of antidepressants’, no drugs were at a statistically significantly higher risk. Although drugs recorded in the Prescribed Drug Register have been prescribed and collected, we cannot be entirely sure to what extent the medication was actually consumed. To address this limitation, we divided the exposed children into those born to a mother with only a single dispensation, and those with at least two dispensations overlapping the pregnancy. The study focused on those with at least two dispensations, as a continuous dispensation pattern was assumed to better reflect an ongoing treatment. Although we adjusted for both parents’ education level at childbirth, we could not adjust for the income of the family. While education level had no effect on the association in our Swedish sample, this may not be the case in cohorts from other countries. Moreover, the Patient Register does not provide information from the primary care, and as such, any diagnoses confined to a primary care setting will go undetected. Still, this will not affect the study's ability to detect children with an ASD, as they are referred to a specialist that is covered by the Patient Register. The lack of primary care data may, however, affect the study's ability to capture psychiatric diagnoses as measure of mental illness among the parents, and consequently the ability to adjust for potential confounding due to underlying mental illness diagnosed in a primary care setting only. Antidepressant prescriptions are accompanied with a diagnosis in Sweden, yet supplemental analyses show that about 25% of mothers treated with an antidepressant during pregnancy lack a psychiatric diagnosis in the Patient Register (online Supplementary Fig. S13), which could indicate residual confounding. Moreover, the severity of the psychiatric disorders investigated was not known, nor if the mothers experienced ongoing episodes of the lifetime diagnosed disorders. It is likely that mothers treated with antidepressants during pregnancy experienced a more severe disorder than unmedicated mothers with a lifetime diagnosis of depression or anxiety. Finally, the current study cohort was restricted to children born in 2006 and 2007, and therefore is underpowered to perform family-control analyses, which can be valuable to address potential residual confounding due to shared familial and genetic factors.

Conclusion

Medication with antidepressants during pregnancy does not appear to be causally associated with an increased risk of ASD in the offspring. Instead, the results suggest that the association is explained by factors related to the underlying susceptibility to psychiatric disorders. Based on these findings, the risk of ASD in the offspring should not be a consideration to withhold treatment with commonly used antidepressant from pregnant women.

Supplementary material

The supplementary material for this article can be found at https://doi.org/10.1017/S0033291717001301.

Acknowledgment

This study was supported by grants from the National Institutes of Health; grant HD073978 from the Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institute of Environmental Health Sciences, and National Institute of Neurological Disorders and Stroke; grant MH097849 from the National Institute of Mental Health; by the Beatrice and Samuel A. Seaver Foundation; by the Fredrik and Ingrid Thuring Foundation; and by the Swedish Society of Medicine. The sponsors of the study had no role in study design, data collection, data analysis, data interpretation, writing of the report, or in the decision to submit the paper for publication. The corresponding author had full access to all data in the study and had final responsibility for the decision to submit for publication.

Declaration of Interest

None.

References

Andrade, SE, Raebel, MA, Brown, J, Lane, K, Livingston, J, Boudreau, D, Rolnick, SJ, Roblin, D, Smith, DH, Willy, ME, Staffa, JA, Platt, R (2008). Use of antidepressant medications during pregnancy: a multisite study. American Journal of Obstetrics & Gynecology 198, 194e1194e5.Google Scholar
Bakker, MK, Kolling, P, van den Berg, PB, de Walle, HE, de Jong van den Berg, LT (2008). Increase in use of selective serotonin reuptake inhibitors in pregnancy during the last decade, a population-based cohort study from the Netherlands. British Journal of Clinical Pharmacology 65, 600606.CrossRefGoogle ScholarPubMed
Boukhris, T, Sheehy, O, Mottron, L, Bérard, A (2016). Antidepressant use during pregnancy and the risk of autism spectrum disorder in children. JAMA Pediatrics 170, 117124.CrossRefGoogle ScholarPubMed
Castro, V, Kong, S, Clements, C, Brady, R, Kaimal, A, Doyle, A, Robinson, E, Churchill, S, Kohane, I, Perlis, R (2016). Absence of evidence for increase in risk for autism or attention-deficit hyperactivity disorder following antidepressant exposure during pregnancy: a replication study. Translational Psychiatry 6, e708.Google Scholar
Cipriani, A, Furukawa, TA, Salanti, G, Geddes, JR, Higgins, JP, Churchill, R, Watanabe, N, Nakagawa, A, Omori, IM, McGuire, H, Tansella, M, Barbui, C (2009). Comparative efficacy and acceptability of 12 new-generation antidepressants: a multiple-treatments meta-analysis. Lancet 373, 746758.CrossRefGoogle ScholarPubMed
Clements, CC, Castro, VM, Blumenthal, SR, Rosenfield, HR, Murphy, SN, Fava, M, Erb, JL, Churchill, SE, Kaimal, AJ, Doyle, AE (2015). Prenatal antidepressant exposure is associated with risk for attention-deficit hyperactivity disorder but not autism spectrum disorder in a large health system. Molecular Psychiatry 20, 727734.CrossRefGoogle ScholarPubMed
Cnattingius, S, Ericson, A, Gunnarskog, J, Kallen, B (1990). A quality study of a medical birth registry. Scandinavian Journal of Social Medicine 18, 143148.Google Scholar
Croen, LA, Grether, JK, Yoshida, CK, Odouli, R, Hendrick, V (2011). Antidepressant use during pregnancy and childhood autism spectrum disorders. Archives of General Psychiatry 68, 11041112.Google Scholar
Efron, B, Tibshirani, RJ (1994). An Introduction to the Bootstrap. Chapman and Hall/CRC Press: London.Google Scholar
Ekbom, A (2011). The Swedish multi-generation register. Methods in Molecular Biology 675, 215220.Google Scholar
Gidaya, NB, Lee, BK, Burstyn, I, Yudell, M, Mortensen, EL, Newschaffer, CJ (2014). In utero exposure to selective serotonin reuptake inhibitors and risk for autism spectrum disorder. Journal of Autism and Developmental Disorders 44, 25582567.Google Scholar
Grambsch, PM, Therneau, TM (1994). Proportional hazards tests and diagnostics based on weighted residuals. Biometrika 81, 515526.CrossRefGoogle Scholar
Harrington, RA, Lee, L-C, Crum, RM, Zimmerman, AW, Hertz-Picciotto, I (2014). Prenatal SSRI use and offspring with autism spectrum disorder or developmental delay. Pediatrics 133, e1241e1248.Google Scholar
Hogberg, U, Larsson, N (1997). Early dating by ultrasound and perinatal outcome. A cohort study. Acta Obstetricia et Gynecologica Scandinavica 76, 907912.CrossRefGoogle ScholarPubMed
Holm, S (1979). A simple sequentially rejective multiple test procedure. Scandinavian Journal of Statistics 6, 6570.Google Scholar
Hviid, A, Melbye, M, Pasternak, B (2013). Use of selective serotonin reuptake inhibitors during pregnancy and risk of autism. New England Journal of Medicine 369, 24062415.CrossRefGoogle ScholarPubMed
Idring, S, Rai, D, Dal, H, Dalman, C, Sturm, H, Zander, E, Lee, BK, Serlachius, E, Magnusson, C (2012). Autism spectrum disorders in the Stockholm Youth Cohort: design, prevalence and validity. PLoS ONE 7, e41280.Google Scholar
International Schizophrenia Consortium, Purcell, SM, Wray, NR, Stone, JL, Visscher, PM, O'Donovan, MC, Sullivan, PF, Sklar, P (2009). Common polygenic variation contributes to risk of schizophrenia and bipolar disorder. Nature 460, 748752.Google Scholar
Jokiranta, E, Brown, AS, Heinimaa, M, Cheslack-Postava, K, Suominen, A, Sourander, A (2013). Parental psychiatric disorders and autism spectrum disorders. Psychiatry Research 207, 203211.Google Scholar
Lecrubier, Y (2001). The burden of depression and anxiety in general medicine. Journal of Clinical Psychiatry 62(Suppl. 8), 49; discussion 10-1.Google Scholar
Lichtenstein, P, Yip, BH, Bjork, C, Pawitan, Y, Cannon, TD, Sullivan, PF, Hultman, CM (2009). Common genetic determinants of schizophrenia and bipolar disorder in Swedish families: a population-based study. Lancet 373, 234239.Google Scholar
Ludvigsson, JF, Andersson, E, Ekbom, A, Feychting, M, Kim, JL, Reuterwall, C, Heurgren, M, Olausson, PO (2011). External review and validation of the Swedish national inpatient register. BMC Public Health 11, 450.Google Scholar
Ludvigsson, JF, Otterblad-Olausson, P, Pettersson, BU, Ekbom, A (2009). The Swedish personal identity number: possibilities and pitfalls in healthcare and medical research. European Journal of Epidemiology 24, 659667.Google Scholar
Malm, H, Brown, AS, Gissler, M, Gyllenberg, D, Hinkka-Yli-Salomaki, S, McKeague, IW, Weissman, M, Wickramaratne, P, Artama, M, Gingrich, JA, Sourander, A (2016). Gestational exposure to selective serotonin reuptake inhibitors and offspring psychiatric disorders: a national register-based study. Journal of the American Academy of Child and Adolescent Psychiatry 55, 359366.Google Scholar
Marmorstein, NR, Malone, SM, Iacono, WG (2004). Psychiatric disorders among offspring of depressed mothers: associations with paternal psychopathology. American Journal of Psychiatry 161, 15881594.Google Scholar
Meltzer-Brody, S, Stuebe, A (2014). The long-term psychiatric and medical prognosis of perinatal mental illness. Best Practice & Research Clinical Obstetrics & Gynaecology 28, 4960.CrossRefGoogle ScholarPubMed
O'Hara, MW, McCabe, JE (2013). Postpartum depression: current status and future directions. Annual Review of Clinical Psychology 9, 379407.Google Scholar
Olfson, M, Marcus, SC (2009). National patterns in antidepressant medication treatment. Archives of General Psychiatry 66, 848856.Google Scholar
Rai, D, Lee, BK, Dalman, C, Golding, J, Lewis, G, Magnusson, C (2013). Parental depression, maternal antidepressant use during pregnancy, and risk of autism spectrum disorders: population based case-control study. BMJ 346, f2059.CrossRefGoogle ScholarPubMed
Sandin, S, Schendel, D, Magnusson, P, Hultman, C, Suren, P, Susser, E, Gronborg, T, Gissler, M, Gunnes, N, Gross, R, Henning, M, Bresnahan, M, Sourander, A, Hornig, M, Carter, K, Francis, R, Parner, E, Leonard, H, Rosanoff, M, Stoltenberg, C, Reichenberg, A (2016). Autism risk associated with parental age and with increasing difference in age between the parents. Molecular Psychiatry 21, 693700.Google Scholar
Sorensen, MJ, Gronborg, TK, Christensen, J, Parner, ET, Vestergaard, M, Schendel, D, Pedersen, LH (2013). Antidepressant exposure in pregnancy and risk of autism spectrum disorders. Clinical Epidemiology 5, 449459.Google Scholar
Sullivan, PF, Daly, MJ, O'Donovan, M (2012). Genetic architectures of psychiatric disorders: the emerging picture and its implications. Nature Reviews Genetics 13, 537551.Google Scholar
Wettermark, B, Hammar, N, Fored, CM, Leimanis, A, Otterblad Olausson, P, Bergman, U, Persson, I, Sundstrom, A, Westerholm, B, Rosen, M (2007). The new Swedish Prescribed Drug Register – opportunities for pharmacoepidemiological research and experience from the first six months. Pharmacoepidemiology and Drug Safety 16, 726735.Google Scholar
WHO (2006). The Anatomical Therapeutic Chemical Classification System with Defined Daily Doses (ATC/DDD). WHO: Oslo.Google Scholar
Figure 0

Table 1. Cohort subject characteristics

Figure 1

Table 2. Relative risks of autism spectrum disorder due to exposure to any type of antidepressantsa

Figure 2

Table 3. Relative risks of autism spectrum disorder due to exposure to specific antidepressantsa

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