Childhood Maltreatment Predicts Unfavorable Course of Illness and Treatment Outcome in Depression: A Meta-Analysis
Abstract
Objectives:
Evidence suggests that childhood maltreatment may negatively affect not only the lifetime risk of depression but also clinically relevant measures of depression, such as course of illness and treatment outcome. The authors conducted the first meta-analysis to examine the relationship between childhood maltreatment and these clinically relevant measures of depression.
Method:
The authors conducted searches in MEDLINE, PsycINFO, and Embase for articles examining the association of childhood maltreatment with course of illness (i.e., recurrence or persistence) and with treatment outcome in depression that appeared in the literature before December 31, 2010. Recurrence was defined in terms of number of depressive episodes. Persistence was defined in terms of duration of current depressive episode. Treatment outcome was defined in terms of either a response (a 50% reduction in depression severity rating from baseline) or remission (a decrease in depression severity below a predefined clinical significance level).
Results:
A meta-analysis of 16 epidemiological studies (23,544 participants) suggested that childhood maltreatment was associated with an elevated risk of developing recurrent and persistent depressive episodes (odds ratio=2.27, 95% confidence interval [CI]=1.80–2.87). A meta-analysis of 10 clinical trials (3,098 participants) revealed that childhood maltreatment was associated with lack of response or remission during treatment for depression (odds ratio=1.43, 95% CI=1.11–1.83). Meta-regression analyses suggested that the results were not significantly affected by publication bias, choice of outcome measure, inclusion of prevalence or incidence samples, study quality, age of the sample, or lifetime prevalence of depression.
Conclusions:
Childhood maltreatment predicts unfavorable course of illness and treatment outcome in depression.
Major depression is a common and impairing illness, often exhibiting a recurrent and progressive course. Depression ranks among the most common psychiatric disorders worldwide, with a 12-month prevalence between 10% and 17% and a lifetime prevalence between 17% and 40% (1, 2). Because the lifetime prevalence of depression is at most four times its 12-month prevalence, depressive episodes are not independent events uniformly distributed in the population but rather tend to cluster in the same individuals. Consistent with this evidence, 60% of individuals who have recovered from a depressive episode will have a recurrence within 5 years (3). The rate of recurrence may be even higher in individuals who experience more persistent depressive episodes and in those who have a poor treatment outcome with residual subthreshold symptoms (3, 4). Because of the large health impact and economic burden associated with a poor longitudinal course of depressive illness, it is important to identify factors that predict risk of developing recurrent and persistent depressive episodes and lack of remission or response during treatment for depression.
Childhood maltreatment may predict an unfavorable course of illness and treatment outcome. Compared with individuals who have not been maltreated, those with a history of childhood maltreatment are at greater risk of meeting criteria for a depressive episode at any point in life (5). Maltreated individuals are also at greater risk of enduring cognitive (6) and biological (7) vulnerabilities associated with heightened stress sensitivity (8), which might predispose them to an unfavorable course of illness and treatment outcome. For example, maltreated individuals tend to have elevated inflammation levels (7, 9), which have been associated with recurrent depressive episodes (10) and poor treatment response (11).
To test whether individuals with a history of childhood maltreatment are at elevated risk of an unfavorable depression course and treatment outcome, we performed meta-analyses of epidemiological studies investigating the association between childhood maltreatment and depression recurrence or persistence and of clinical trials investigating the association between childhood maltreatment and outcome of psychological, pharmacological, or combined treatment. We also explored the effects of various possible sources of artifact or bias on the results of the meta-analyses.
Method
Inclusion Criteria
We identified studies satisfying the following criteria: definition of childhood adversities consistent with childhood maltreatment (physical abuse, sexual abuse, neglect, or family conflict or violence); diagnosis of depressive disorder, ascertained either in population-based or in clinical samples; and evaluation of relevant depression measures (12). Depression recurrence was defined in terms of number of depressive episodes over the period of observation or as risk of a new depressive episode in individuals with prior history of depression. Depression persistence was defined as prolonged duration of uninterrupted illness, including dysthymia, over the period of observation. Treatment outcome was defined as a change in depression scores between the beginning and the end of treatment, either as a continuous measure (i.e., improvement, defined as percentage improvement on a depression rating scale) or as a categorical outcome (i.e., response, defined as a reduction of depression rating scale score by 50% or more; or remission, defined as a decrease of depressive symptoms below a predetermined clinical significance level).
Identification of Studies
We searched MEDLINE, PsycINFO, and Embase databases for articles describing the relationship between childhood maltreatment (search terms: child* maltreatment, child* abuse, child* neglect, early experience) and relevant depression measures (search terms: depress*, mood disorder, MDD, recurrence, persistence, chronic, duration, length, improvement, response, remission, treatment, psychotherapy, CBT, pharmacotherapy, antidepressant, SSRI) using human subjects, written in English, and published by December 31, 2010.
Data Extraction
Two authors independently extracted data from eligible articles. Inconsistencies were resolved in consensus meetings and confirmed with the authors of the primary studies when necessary.
Statistical Analysis
Extracted data were converted to odds ratio effect sizes (13) reflecting the probability of unfavorable outcomes, with odds ratios above 1 reflecting a greater likelihood of recurrence, persistence, or poor treatment outcome in individuals with a history of childhood maltreatment compared to those without. The meta-analysis of clinical trials examined the difference in outcome between depressed patients with a history of childhood maltreatment and those without in the same active treatment arm. Where only continuous outcomes were reported, the risk of unfavorable outcomes was derived using validated methods (14). Heterogeneity between studies was tested with Cochran's Q test (15). In the presence of a homogeneous distribution, we carried out meta-analyses using fixed-effects models weighting each study by a measure of sampling error, such as the inverse variance. If the dispersion of effect sizes was greater than expected from sampling error alone (i.e., heterogeneity), we carried out meta-analyses using random-effects models, which include both sampling and study-level errors. Fixed- and random-effects meta-analyses were performed using the meta and metan programs applied in the Stata software package (StataCorp, College Station, Tex.). Additional analyses explored the effects of various possible sources of artifact or bias on the results.
First, we assessed the presence of publication bias visually by funnel plot (16) and formally by its direct statistical analogue, Begg's adjusted-rank correlation test (17), using the metabias program applied in Stata. In the presence of significant rank correlation tests, we adopted a nonparametric trim-and-fill method (18) using the metatrim program applied in Stata.
Second, we assessed the sensitivity of meta-analysis results to different outcome measures through subgroup analyses.
Third, we assessed the sensitivity of the results to different sampling strategies through subgroup analyses. Studies in clinical (or prevalence) samples and those in population (or incidence) samples could lead to different results because of ascertainment bias (19). The potential ascertainment bias could not have affected the results of clinical trials, which were restricted to clinical samples.
Fourth, we assessed the impact of study quality on the meta-analysis results through meta-regression using the metareg program applied in Stata. The quality of epidemiological studies was assessed with the Newcastle-Ottawa Scale (20), which has been recommended by the Cochrane collaboration (21) and has been used in previous studies (22). The quality of clinical trials was assessed by an adapted version of the Jadad scale (23) based on randomization, consideration of dropouts, and blinding. Because the contrast of interest was between individuals with a history of maltreatment and those without in the same active treatment arm, we considered blinding to maltreatment status rather than to treatment allocation.
Fifth, we assessed the presence of age effects through meta-regression analyses. Age effects could have influenced the meta-analysis results in two ways. With regard to the epidemiological studies, it was possible that because maltreated individuals are younger at the onset of depression than individuals without a history of maltreatment (24), they could spend more time at risk of recurrence and show greater depression recurrence and persistence for this reason. It was not possible to extract information on age at illness onset from the studies examined. However, we reasoned that the relative contribution of earlier age at onset to the total time that maltreated individuals spend at risk decays as the age of the sample increases. Therefore, if age at onset explained the association between childhood maltreatment and depression recurrence and persistence, we should have observed a significant negative correlation between mean age of the samples and effect sizes. With regard to the clinical trials, previous research has suggested that individuals at different ages could have a different response to the same antidepressant treatment (25). Therefore, it was possible that the age of the sample could have explained between-study differences in the association between childhood maltreatment and treatment outcomes in depression.
Finally, we assessed the presence of recall bias through meta-regression analyses. Most of the studies we examined were based on retrospective recall of childhood maltreatment. The reliability of retrospective recall of childhood maltreatment may be limited in individuals with a lifetime history of depression (26, 27) because of biases in autobiographical memory (28, 29). Therefore, to the extent that lifetime history of depression was different between the studies, it was possible that recall bias could have explained between-study differences in the association between childhood maltreatment and depression course. Recall bias was not an issue for the meta-analysis of the clinical trials, because all participants were depressed at the time the assessment of maltreatment history was carried out.
Results
The study selection procedure is summarized in Figure 1.
Epidemiological Studies
The association between childhood maltreatment and poor longitudinal course of depressive disorder (i.e., recurrence or persistence) was tested in 16 studies with a total of 23,544 participants (Table 1) (7, 30–44). We identified significant heterogeneity across studies (Q=46.1, df=15, p<0.001) and therefore performed an analysis using a random-effects model. A meta-analysis of these studies showed that compared to those without a history of childhood maltreatment, maltreated individuals were twice as likely to have an unfavorable longitudinal course of depression (odds ratio=2.27, 95% confidence interval [CI]=1.80–2.87) (Figure 2). We performed additional analyses to explore the effects of possible sources of artifact or bias on these results.
Authors (Reference) | Study N | Mean Age or Range (Years) | % Female | Sample Type | Depression Measure | Maltreatment Measure | Outcome Definition | Length of Observation (Years) | Results |
---|---|---|---|---|---|---|---|---|---|
Kessler and Magee (30) | 1,024 | 33 | 50 | Population | DIS, FHRDC | Own questionnaire | Recurrence: new depressive episode(s) in individuals with history of depression | 16 | Family violence associated with greater recurrence (odds ratio=2.04, 95% CI=1.42–2.93) |
Brown and Moran (31) | 404 | 18–50 | 100 | Population | PSE | CECA | Persistence: depressive episode lasting 12 months or more | 3 | Childhood adversity associated with greater persistence (odds ratio=4.02, 95% CI=1.59–10.15) |
Brown et al. (32) | 125 | 18–60 | 100 | Clinical | PSE | CECA | Persistence: nonrecovery from depression over 12 months | 2 | Childhood adversity associated with greater persistence (odds ratio=1.93, 95% CI=1.05–3.54) |
Zlotnick et al. (33) | 37 | 100 | Clinical | Semi-structured interview | Own questionnaire | Persistence: non-recovery (HAM-D <7 for 3 consecutive months after hospital discharge) | 1 | Childhood adversity not associated with persistence (odds ratio=2.29, 95% CI=0.49–10.61) | |
Kessler et al. (34) | 5,877 | 15–54 | 50 | Population | CIDI | Own questionnaire | Persistence: risk of dysthymia | 40 | Childhood adversity associated with greater persistence (odds ratio=2.81, p<0.05) |
Bernet and Stein (35) | 88 | 42 | 50 | Clinical | SCID | CTQ | Recurrence: number of depressive episodes | 25 | Childhood trauma associated with greater recurrence (t=4.78, p<0.0005) |
Hayden and Klein (36) | 86 | 31.1 | 75.6 | Clinical | SCID, longitudinal interval follow-up evaluation | EHEI | Persistence: nonrecovery from dysthymic disorder (<8 consecutive weeks with minimal or no symptoms) | 5 | Physical abuse associated with greater persistence (smaller recovery: hazard ratio=0.83, 95% CI=0.60–1.15) |
Wainwright and Surtees (37) | 3,353 | 62.3 | 55.2 | Population | Structured self-assessment | Own questionnaire | Recurrence: number of depressive episodes | 46 | Physical abuse not associated with greater recurrence (relative risk=1.27; 95% CI=0.77–1.99) |
Brown et al. (38) | 198 | 34 | 100 | Population | SCAN | CECA | Persistence: depressive episode lasting ≥12 months | 17 | Childhood adversity associated with greater recurrence (odds ratio=14.9, 95% CI=6.0–37.0) |
Collishaw et al. (39) | 3,624 | 44.2 | 50 | Population | SADS-L | CECA | Recurrence: ≥3 lifetime depressive episodes | 28 | Childhood adversity associated with greater recurrence (odds ratio=7.80, 95% CI=1.7–35.5) |
Danese et al. (7) | 1,037 | 32 | 48 | Population | DIS | Prospective observation + retrospective reports | Recurrence: ≥2 lifetime depressive episodes | 21 | Childhood adversity associated with greater recurrence (odds ratio=2.60, 95% CI=1.60–4.24) |
Ritchie et al. (40) | 942 | 72 | 58 | Population | MINI diagnosis or CES-D >16 or current antidepressant treatment | Own questionnaire | Recurrence: ≥2 depressive episodes | 4 | Childhood adversity associated with greater recurrence (odds ratio=2.89, 95% CI=1.83–4.57) |
Wiersma et al. (41) | 1,230 | 40.7 | 67.3 | Clinical | CIDI | CTI | Persistence: depressive episode lasting ≥24 months | 4 | Physical abuse associated with greater persistence (odds ratio=1.99, 95% CI=1.37–2.88) |
Angst et al. (42) | 110 | 27–41 | 60 | Clinical | SPIKE | Own questionnaire | Persistence: depressive symptoms for most days over 2 years or daily for 12 months | 13 | Childhood adversity associated with greater persistence (p=0.05) |
McLaughlin et al. (43) | 5,692 | 36.7 | 42 | Population | CIDI | Own questionnaire | Persistence: time since more recent episode, controlling for age at onset and time since onset | 20 | Physical abuse associated with greater persistence (odds ratio=1.9, 95% CI=1.5–2.4) |
Suija et al. (44) | 123 | 39 | 85 | Clinical | CIDI | CTI | Recurrence: new depressive episode in individuals with history of depression | 1 | Childhood trauma associated with greater recurrence (odds ratio=1.58, 95% CI=1.05–2.38) |
Publication bias.
The funnel plot showed asymmetrical distribution of the studies, and results of Begg's adjusted-rank correlation test were significant (p=0.027), suggesting the possibility of publication bias. However, the trim-and-fill procedure achieved a similar combined effect size (odds ratio=1.78, 95% CI=1.38–2.31) to the nonfilled analysis, suggesting that potential publication bias did not significantly affect the results.
Sensitivity analyses.
First, we performed sensitivity analyses to examine whether the association between childhood maltreatment and course of illness was comparable across different measures of depression course (Figure 2). The association between childhood maltreatment and depression recurrence was tested in seven studies. We identified significant heterogeneity across studies (Q=15.1, df=6, p=0.020) and therefore performed an analysis using a random-effects model. A meta-analysis of these studies showed that maltreated individuals were twice as likely as those without a history of childhood maltreatment to develop recurrent depressive episodes (odds ratio=2.24, 95% CI=1.62–3.10). The association between childhood maltreatment and depression persistence was tested in nine studies. We identified significant heterogeneity across the studies (Q=30.60, df=8, p<0.001) and therefore performed an analysis using a random-effects model. A meta-analysis of these studies showed that maltreated individuals were twice as likely as those without a history of childhood maltreatment to develop persistent depressive episodes (odds ratio=2.34, 95% CI=1.65–3.32).
Second, we performed sensitivity analyses to examine whether the association between childhood maltreatment and course of illness was comparable across clinical and population samples. The association between childhood maltreatment and depression course was tested in seven clinical (prevalence) samples. Heterogeneity approached significance across studies (Q=10.69, df=6, p=0.098), so we performed an analysis using a random-effects model. A meta-analysis of the studies with clinical samples showed that maltreated individuals were nearly twice as likely as those without a history of childhood maltreatment to develop recurrent or persistant depressive episodes (odds ratio=1.78, 95% CI=1.36–2.34). The association between childhood maltreatment and depression course was tested in nine population (incidence) samples. We identified significant heterogeneity across the studies (Q=30.12, df=8, p<0.001) and therefore performed an analysis using a random-effects model. A meta-analysis of the studies with population samples showed that maltreated individuals were more than twice as likely as those without a history of childhood maltreatment to develop recurrent or persistent depressive episodes (odds ratio=2.75, 95% CI=1.94–3.91).
Bias owing to study quality.
Meta-regression analysis showed that between-study differences in quality ratings based on the Newcastle-Ottawa Scale did not explain the between-study variability in the association of childhood maltreatment with depression course (p=0.611), suggesting that bias due to study quality was unlikely. (The study quality assessment is reported in the data supplement that accompanies the online edition of this article.)
Effect of age at illness onset.
This analysis was based on proxy measures of mean age of the samples. We extracted data on mean age from 15 studies. We did not observe the negative correlation between age of the samples and effect sizes that was expected in the presence of an age-at-onset effect (r=–0.075, 95% CI=–0.541 to 0.392). In addition, meta-regression analysis showed that between-study differences in age of the sample did not explain the between-study variability in the association of childhood maltreatment with depression course (p=0.819), suggesting that confounding by age at onset was unlikely.
Recall bias.
This analysis was based on proxy measures of lifetime history of depression. We extracted data on lifetime prevalence of depression from 14 studies. Meta-regression analysis showed that between-study differences in lifetime prevalence of depression did not explain the between-study variability in the association of childhood maltreatment with depression course (p=0.878), suggesting that recall bias was unlikely.
Clinical Trials
The association between childhood maltreatment and the outcome of treatment with psychological therapy, antidepressant medication, or combined treatment was tested in 10 studies (15 active treatment arms) with a total of 3,098 participants (Table 2) (45–54). We identified significant heterogeneity across studies (Q=24.77, df=14, p=0.037) and therefore performed an analysis using a random-effects model. A meta-analysis of these studies revealed that maltreated individuals were more likely than those without a history of childhood maltreatment to show poor treatment outcome (odds ratio=1.43, 95% CI=1.11–1.83) (Figure 3). We performed additional analyses to explore the effect of possible sources of artifact or bias on these results.
Authors (Reference) | Study N | Mean Age (Years) | % Female | Depression Measure | Maltreatment Measure | Treatment Description | Length of Treatment (Weeks) | Outcome Definition | Results |
---|---|---|---|---|---|---|---|---|---|
Sakado et al. (45) | 60 | 43 | 50 | SCID | PBI | Tricyclic antidepressant | 16 | Remission: HAM-D-17 <8 | Low paternal care associated with lack of remission (odds ratio=1.9, 95% CI=1.7–2.2) |
Nemeroff et al. (46) | 681 | 43 | 65.3 | SCID | CTS | CBASP, nefazodone, combination | 12 | Improvement: HAM-D-24 score reduction | Childhood abuse associated with poor outcome within the pharmacological treatment arm and good outcome within the psychotherapy treatment arm (trauma-by-treatment interaction F=3.13, df=1, 495, p=0.045) |
Barbe et al. (47) | 107 | 15.8 | 75.7 | K-SADS; BDI ≥ 13 | CBQ | CBT, SBFT, NST | 12–16 | Remission: free from major depressive disorder diagnosis for ≥2 months | Family conflict associated with lack of remission (relative risk=0.95, 95% CI=0.91–0.998) |
Enns and Cox (48) | 171 | 41.8 | 64.3 | Unstructured interview | DMQ, PBI | Various antidepressants and psychological treatments | 52 | Response: 50% decrease in BDI scoreRemission: BDI <10 | Sexual abuse associated with lack of response (χ2=4.32, p=0.038) and lack of remission (χ2=4.38, p=0.036); low parental care or overprotection were unrelated to outcome (p=0.58) |
Asarnow et al. (49) | 287 | 15.9 | 69.8 | CDRS-R ≥40; CGI ≥4; resistance to SSRIs | CBQ, clinical interview | Medication switch alone (SSRI or venlafaxine), medication switch plus CBT | 12 | Response: CDRS-R score reduction ≥50% | Childhood abuse associated with lack of response to CBT but not to pharmacotherapy or combination (abuse-by-treatment interaction β=0.15, p<0.001) |
Johnstone et al. (50) | 195 | 32 | 57 | Not specified | PBI, own questionnaire | Fluoxetine, nortriptyline | 6 | Improvement: MADRS score percentage reduction | Maternal overprotection was associated with less improvement (odds ratio=0.93, 95% CI=0.89–0.97). Parental care and childhood abuse were unrelated to outcome |
Klein et al. (51) | 808 | 43.6 | 55 | SCID, HAM-D-17 ≥20 | MOPS, CTQ | Texas Medication Algorithm | 12 | Remission: HAM-D-17 <8 | Childhood abuse associated with lack of remission (odds ratio=0.52, p<0.01) |
Shirk et al. (52) | 50 | 15.9 | 68 | C-DISC-IV | LEQ | CBT | 12 | Remission: free from major depressive disorder diagnosis at the end of treatment Improvement: BDI score reduction | Childhood trauma associated with lack of remission (ρ=–0.31 to –0.35, p<0.05) |
Lewis et al. (53) | 427 | 14.6 | 54 | K-SADS-PL, CDRS-R >45 | PTSD section of K-SADS-PL | Fluoxetine, CBT, combination, placebo | 12 | Improvement: reduction in CDRS-R score | Childhood trauma associated with poor response to CBT but not with response to fluoxetine or combination treatment (trauma-by-treatment-by-time interaction F=2.02, p<0.05) |
Miniati et al. (54) | 312 | 39 | 73 | SCID | Clinical interview | Medication (citalopram or escitalopram), IPT, combination | 12 | Time to remission (Remission: HAM-D-17 <8) | Childhood abuse associated with longer time to remission across treatments (hazard ratio=1.68, 95% CI=1.09–2.59) |
Publication bias.
The funnel plot showed symmetrical distribution of the studies and Begg's adjusted rank correlation test was nonsignificant (p=0.553), suggesting that publication bias was unlikely.
Sensitivity analyses.
We performed sensitivity analyses to examine whether the association between childhood maltreatment and treatment outcome was comparable across different treatment modalities (Figure 3). The association between childhood maltreatment and the outcome of psychotherapy was tested in four studies. We did not identify significant heterogeneity across studies (Q=6.03, df=3, p=0.110) and therefore performed an analysis using a fixed-effects model. A meta-analysis of these studies revealed that compared to those without a history of childhood maltreatment, maltreated individuals showed a nonsignificantly higher risk for poor outcome of psychotherapy (odds ratio=1.12, 95% CI=0.68–1.85). The association between childhood maltreatment and the outcome of pharmacological treatment was tested in six studies. We did not identify significant heterogeneity across studies (Q=8.41, df=5, p=0.135) and therefore performed an analysis using a fixed-effects model. A meta-analysis of these studies revealed that maltreated individuals showed a poorer outcome of pharmacological treatment compared to those without a history of childhood maltreatment (odds ratio=1.26, 95% CI=1.01–1.56). The association between childhood maltreatment and the outcome of combined treatment (psychotherapy and antidepressant medications) was tested in five studies. We did not identify significant heterogeneity across studies (Q=4.84, df=4, p=0.304) and therefore performed an analysis using a fixed-effects model. A meta-analysis of these studies revealed that maltreated individuals showed poorer outcome of combined treatment compared to those without a history of childhood maltreatment (odds ratio=1.90, 95% CI=1.40–2.58).
Bias owing to study quality.
Meta-regression analysis showed that between-study differences in quality ratings based on the adapted Jadad scale did not explain the between-study variability in the association of childhood maltreatment with treatment outcome (p=0.383), suggesting that bias due to study quality was unlikely. (The study quality assessment is reported in the online data supplement.)
Age effect.
Meta-regression analysis showed that between-study differences in mean age of the sample did not explain the between-study variability in the association between childhood maltreatment and poor response to antidepressant treatment (p=0.644). Furthermore, a meta-regression analysis showed that classification into pediatric (<18 years) compared with adult samples did not explain the variability in the association between childhood maltreatment and poor response to antidepressant treatment (p=0.498).
Discussion
This meta-analysis addressed the possible developmental origins of heterogeneity in clinically relevant measures of depression such as course of illness and treatment outcome. The epidemiological studies suggested that maltreated individuals were twice as likely as those without a history of childhood maltreatment to develop both recurrent and persistent depressive episodes. Findings from clinical trials were consistent with the epidemiological observations. Compared with depressed individuals without a history of childhood maltreatment, depressed and maltreated individuals appeared to benefit less from treatment (and particularly from combined treatment), thereby incurring greater risk of recurrent and persistent depressive episodes (4).
Limitations
These results should be evaluated in the context of several potential limitations. First, selective publication of studies reporting significant associations between childhood maltreatment and clinically relevant depression measures may influence results. We identified evidence of publication bias in epidemiological studies, but the trim-and-fill procedure suggested that publication bias was unlikely to significantly change the meta-analysis results. In contrast, both graphical and statistical methods suggested that the presence of significant publication bias was unlikely in clinical trials. Second, the results could also be limited to particular outcome measures. However, subgroup analyses appeared to be insensitive to the outcome measures examined. Third, results from epidemiological studies could be limited to clinical or population samples. However, subgroup analyses appeared to be overall insensitive to the sample type examined. Fourth, study quality could have influenced the results. However, differences in study quality could not explain between-study heterogeneity in the association between childhood maltreatment and depression course or treatment outcome. Fifth, the earlier age at onset for depression in maltreated individuals could influence epidemiological study results, leading to spurious findings of greater depression recurrence in maltreated individuals compared with individuals with no history of maltreatment by increasing the amount of time that maltreated individuals spent at risk. However, we could not observe the negative correlation between effect sizes and mean age of the samples that was expected in the presence of age-at-onset effect. In addition, the differences in mean age could not explain between-study heterogeneity in the association between childhood maltreatment and depression course. Sixth, results from epidemiological studies could also be influenced by recall bias owing to between-study differences in lifetime history of depression. However, differences in lifetime history of depression could not explain between-study heterogeneity in the association between childhood maltreatment and depression course. Finally, the available data did not enable us to examine the relative contribution of different maltreatment subtypes or the effect of other potential confounders.
Implications
Despite the potential limitations, the study results have important implications in several areas.
Future research.
Childhood maltreatment may be conceptualized as a developmental risk factor triggering a chain of risks (55) such as subsequent depressive episodes that might progressively potentiate the vulnerability to poor course of illness (56, 57). In order to understand the origins of this chain of risks, studies should explore the cognitive and biological correlates of maltreatment in childhood before the accumulation of multiple depressive episodes (58). Furthermore, it will be important to characterize the gene-environment interplay underlying the effects of childhood maltreatment on depression outcomes (59–61). Childhood maltreatment may be conceptualized as an environmental risk factor for poor depression course and a moderator of treatment outcome (62), complementing the emerging genetic markers of vulnerability to recurrent depression (63) and poor treatment response (64, 65).
Clinical care.
Information about a history of childhood maltreatment helps identify individuals who are at high risk of developing a recurrent and persistent subtype of depression and those who will respond poorly to treatment. Because of the lack of placebo-controlled studies, we were unable to test whether depressed and maltreated individuals benefit more or less from treatment (versus placebo) than depressed individuals who were not maltreated. In contrast, we observed that depressed and maltreated individuals have a poorer outcome compared with depressed individuals who were not maltreated (i.e., a poor prognosis) within treatment groups. Clinicians may consider that the routine inquiry about childhood maltreatment is not harmful (66) and could add important prognostic information to their assessment. Clinicians may also consider more intensive and alternative treatment options for depressed individuals with a history of childhood maltreatment. The meta-analytical evidence that maltreated and depressed individuals have a poor response to combined treatment with structured psychological therapy and antidepressant medications indicates that simply combining these two common options is not sufficient. It will be important to explore the response of maltreated and depressed individuals to new treatments targeting the biological vulnerabilities described in this subgroup (7, 60), including elevated inflammation levels (67, 68).
Public health.
Interventions aimed at reducing childhood maltreatment could help prevent the large health and economic burden linked to poor depression course. Childhood years are thought to be a sensitive developmental window for the maturation of emotion regulation (69). Therefore, in the same way that childhood educational interventions have greater returns in human capital formation than interventions at later ages (70), early preventive and therapeutic interventions may be more effective (and cost-effective) in preventing a poor longitudinal course of depression than interventions at later ages, when harmful developmental trajectories have already been established.
1. : The epidemiology of major depressive disorder. JAMA 2003; 289:3095–3105Crossref, Medline, Google Scholar
2. : How common are common mental disorders? evidence that lifetime prevalence rates are doubled by prospective versus retrospective ascertainment. Psychol Med 2010; 40:899–909Crossref, Medline, Google Scholar
3. : Multiple recurrences of major depressive disorder. Am J Psychiatry 2000; 157:229–233Link, Google Scholar
4. : Past, present, and future directions for defining optimal treatment outcome in depression. JAMA 2003; 289:3152–3160Crossref, Medline, Google Scholar
5. : The effects of stressful life events on depression. Annu Rev Psychol 1997; 48:191–214Crossref, Medline, Google Scholar
6. : The evolution of the cognitive model of depression and its neurobiological correlates. Am J Psychiatry 2008; 165:969–977Link, Google Scholar
7. : Elevated inflammation levels in depressed adults with a history of childhood maltreatment. Arch Gen Psychiatry 2008; 65:409–415Crossref, Medline, Google Scholar
8. : Depression and sensitization to stressors among young women as a function of childhood adversity. J Consult Clin Psychol 2000; 68:782–787Crossref, Medline, Google Scholar
9. : Childhood maltreatment predicts adult inflammation in a life-course study. Proc Natl Acad Sci USA 2007; 104:1319–1324Crossref, Medline, Google Scholar
10. : Depression and c-reactive protein in US adults: data from the third national health and nutrition examination survey. Arch Intern Med 2004; 164:1010–1014Crossref, Medline, Google Scholar
11. : Cytokine production and treatment response in major depressive disorder. Neuropsychopharmacology 2000; 22:370–379Crossref, Medline, Google Scholar
12. : Conceptualization and rationale for consensus definitions of terms in major depressive disorder: remission, recovery, relapse, and recurrence. Arch Gen Psychiatry 1991; 48:851–855Crossref, Medline, Google Scholar
13. : Practical Meta-Analysis. Thousand Oaks, Calif, SAGE Publications, 2000Google Scholar
14. : Meta-analysis of screening and diagnostic tests. Psychol Bull 1995; 117:167–178Crossref, Medline, Google Scholar
15. : The comparison of percentages in matched samples. Biometrika 1950; 37:256–266Crossref, Medline, Google Scholar
16. : Bias in meta-analysis detected by a simple, graphical test. BMJ 1997; 315:629–634Crossref, Medline, Google Scholar
17. : Operating characteristics of a rank correlation test for publication bias. Biometrics 1994; 50:1088–1101Crossref, Medline, Google Scholar
18. : A nonparametric “trim and fill” method of accounting for publication bias in meta-analysis. J Am Stat Assoc 2000; 95:89–98Google Scholar
19. : The clinician's illusion. Arch Gen Psychiatry 1984; 41:1178–1182Crossref, Medline, Google Scholar
20. : The Newcastle-Ottawa Scale (NOS) for assessing the quality of nonrandomised studies in meta-analyses. 2011. http://www.ohri.ca/programs/clinical_epidemiology/oxford.htm.Google Scholar
21. Higgins JPTGreen S (eds): Cochrane Handbook for Systematic Reviews of Interventions, Version 5.1.0. 2011. www.cochrane-handbook.orgGoogle Scholar
22. : Sexual abuse and lifetime diagnosis of somatic disorders: a systematic review and meta-analysis. JAMA 2009; 302:550–561Crossref, Medline, Google Scholar
23. : Assessing the quality of reports of randomized clinical trials: is blinding necessary? Control Clin Trials 1996; 17:1–12Crossref, Medline, Google Scholar
24. : A prospective investigation of major depressive disorder and comorbidity in abused and neglected children grown up. Arch Gen Psychiatry 2007; 64:49–56Crossref, Medline, Google Scholar
25. : Differential efficacy of escitalopram and nortriptyline on dimensional measures of depression. Br J Psychiatry 2009; 194:252–259Crossref, Medline, Google Scholar
26. : Psychopathology and early experience: a reappraisal of retrospective reports. Psychol Bull 1993; 113:82–98Crossref, Medline, Google Scholar
27. : Validity of adult retrospective reports of adverse childhood experiences: review of the evidence. J Child Psychol Psychiatry 2004; 45:260–273Crossref, Medline, Google Scholar
28. : Autobiographical memory processes and the course of depression. J Abnorm Psychol 1999; 108:511–517Crossref, Medline, Google Scholar
29. : Autobiographical memories in women remitted from major depression. J Abnorm Psychol 2000; 109:331–334Crossref, Medline, Google Scholar
30. : Childhood adversities and adult depression: basic patterns of association in a US national survey. Psychol Med 1993; 23:679–690Crossref, Medline, Google Scholar
31. : Clinical and psychosocial origins of chronic depressive episodes, I: a community survey. Br J Psychiatry 1994; 165:447–456Crossref, Medline, Google Scholar
32. : Clinical and psychosocial origins of chronic depressive episodes, II: a patient enquiry. Br J Psychiatry 1994; 165:457–465Crossref, Medline, Google Scholar
33. : Childhood abuse and recovery from major depression. Child Abuse Negl 1995; 19:1513–1516Crossref, Medline, Google Scholar
34. : Childhood adversity and adult psychiatric disorder in the US National Comorbidity Survey. Psychol Med 1997; 27:1101–1119Crossref, Medline, Google Scholar
35. : Relationship of childhood maltreatment to the onset and course of major depression in adulthood. Depress Anxiety 1999; 9:169–174Crossref, Medline, Google Scholar
36. : Outcome of dysthymic disorder at 5-year follow-up: the effect of familial psychopathology, early adversity, personality, comorbidity, and chronic stress. Am J Psychiatry 2001; 158:1864–1870Link, Google Scholar
37. : Childhood adversity, gender and depression over the life-course. J Affect Disord 2002; 72:33–44Crossref, Medline, Google Scholar
38. : Development of a retrospective interview measure of parental maltreatment using the Childhood Experience of Care and Abuse (CECA) instrument: a life-course study of adult chronic depression, 1. J Affect Disord 2007; 103:205–215Crossref, Medline, Google Scholar
39. : Resilience to adult psychopathology following childhood maltreatment: evidence from a community sample. Child Abuse Negl 2007; 31:211–229Crossref, Medline, Google Scholar
40. : Association of adverse childhood environment and 5-HTTLPR genotype with late-life depression. J Clin Psychiatry 2009; 70:1281–1288Crossref, Medline, Google Scholar
41. : The importance of childhood trauma and childhood life events for chronicity of depression in adults. J Clin Psychiatry 2009; 70:983–989Crossref, Medline, Google Scholar
42. : Childhood adversity and chronicity of mood disorders. Eur Arch Psychiatry Clin Neurosci 2010; 261:21–27Crossref, Medline, Google Scholar
43. : Childhood adversities and adult psychiatric disorders in the national comorbidity survey replication, II: associations with persistence of DSM-IV disorders. Arch Gen Psychiatry 2010; 67:124–132Crossref, Medline, Google Scholar
44. : I: factors associated with recurrent depression: a prospective study in family practice. Fam Prac 2011; 28:22–28Crossref, Medline, Google Scholar
45. : Perceived parenting pattern and response to antidepressants in patients with major depression. J Affect Disord 1999; 52:59–66Crossref, Medline, Google Scholar
46. : Differential responses to psychotherapy versus pharmacotherapy in patients with chronic forms of major depression and childhood trauma. Proc Natl Acad Sci USA 2003; 100:14293–14296Crossref, Medline, Google Scholar
47. : Lifetime history of sexual abuse, clinical presentation, and outcome in a clinical trial for adolescent depression. J Clin Psychiatry 2004; 65:77–83Crossref, Medline, Google Scholar
48. : Psychosocial and clinical predictors of symptom persistence vs remission in major depressive disorder. Can J Psychiatry 2005; 50:769–777Crossref, Medline, Google Scholar
49. : Treatment of selective serotonin reuptake inhibitor-resistant depression in adolescents: predictors and moderators of treatment response. J Am Acad Child Adolesc Psychiatry 2009; 48:330–339Medline, Google Scholar
50. : Childhood neglect and abuse as predictors of antidepressant response in adult depression. Depress Anxiety 2009; 26:711–717Crossref, Medline, Google Scholar
51. : Early adversity in chronic depression: clinical correlates and response to pharmacotherapy. Depress Anxiety 2009; 26:701–710Crossref, Medline, Google Scholar
52. : School-based cognitive-behavioural therapy for adolescent depression. J Emot Behav Disord 2009; 17:106–117Crossref, Google Scholar
53. : Impact of childhood trauma on treatment outcome in the Treatment for Adolescents With Depression Study (TADS). J Am Acad Child Adolesc Psychiatry 2010; 49:132–140Medline, Google Scholar
54. : Clinical characteristics and treatment outcome of depression in patients with and without a history of emotional and physical abuse. J Psychiatr Res 2010; 44:302–309Crossref, Medline, Google Scholar
55. : Pathways from childhood to adult life. J Child Psychol Psychiatry 1989; 30:23–51Crossref, Medline, Google Scholar
56. : Transduction of psychosocial stress into the neurobiology of recurrent affective disorder. Am J Psychiatry 1992; 149:999–1010Link, Google Scholar
57. : Stressful life events and previous episodes in the etiology of major depression in women: an evaluation of the “kindling” hypothesis. Am J Psychiatry 2000; 157:1243–1251Link, Google Scholar
58. : Biological embedding of stress through inflammation processes in childhood. Mol Psychiatry 2011; 16:244–246Crossref, Medline, Google Scholar
59. : Genetic opportunities for psychiatric epidemiology: on life stress and depression. Epidemiol Psichiatr Soc 2008; 17:201–210Crossref, Medline, Google Scholar
60. : The implications of gene-environment interactions in depression: will cause inform cure? Mol Psychiatry 2008; 13:1070–1078Crossref, Medline, Google Scholar
61. : Genes, environments, and individual differences in response to treatment. Harv Rev Psychiatry 2011; 19:109–124Crossref, Medline, Google Scholar
62. : How do risk factors work together? mediators, moderators, and independent, overlapping, and proxy risk factors. Am J Psychiatry 2001; 158:848–856Link, Google Scholar
63. : Genome-wide association study of major recurrent depression in the U.K. population. Am J Psychiatry 2010; 167:949–957Link, Google Scholar
64. : Personalized medicine for depression: can we match patients with treatments? Am J Psychiatry 2010; 167:1445–1455Link, Google Scholar
65. : Genome-wide pharmacogenetics of antidepressant response in the GENDEP project. Am J Psychiatry 2010; 167:555–564Link, Google Scholar
66. : Research participants telling the truth about their lives: the ethics of asking and not asking about abuse. Am Psychol 2006; 61:218–226Crossref, Medline, Google Scholar
67. : Inflammation and its discontents: the role of cytokines in the pathophysiology of major depression. Biol Psychiatry 2009; 65:732–741Crossref, Medline, Google Scholar
68. : The cyclooxygenase-2 inhibitor celecoxib has therapeutic effects in major depression: results of a double-blind, randomized, placebo controlled, add-on pilot study to reboxetine. Mol Psychiatry 2006; 11:680–684Crossref, Medline, Google Scholar
69. : Neuroscience, molecular biology, and the childhood roots of health disparities. JAMA 2009; 301:2252–2259Crossref, Medline, Google Scholar
70. : Skill formation and the economics of investing in disadvantaged children. Science 2006; 312:1900–1902Crossref, Medline, Google Scholar