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Published Online: 1 October 2012

Psychiatric Disorders After Pediatric Traumatic Brain Injury: A Prospective, Longitudinal, Controlled Study

Publication: The Journal of Neuropsychiatry and Clinical Neurosciences

Abstract

The authors compared a group of patients ages 7-17, who were hospitalized with either traumatic brain injury (TBI) or orthopedic injury (OI), regarding the risk of psychiatric disorder developing prospectively within the following 3 months. Patients were assessed within 1 month of injury for pre-injury functioning by means of psychiatric, family-history, and family-adversity interviews, and scales of socioeconomic and adaptive-functioning measures. After 3 months, incidence of novel psychiatric disorder was significantly more frequent in the group of TBI patients, and the difference was not accounted for by any of the baseline measures: pre-injury adaptive functioning, family adversity, psychiatric history, socioeconomic status, severity of injury, or age at injury.

Abstract

The objective was to examine the effects of traumatic brain injury (TBI), as compared with orthopedic injury (OI), relative to the risk for psychiatric disorder. There has only been one previous prospective study of this nature. Participants were age 7–17 years at the time of hospitalization for either TBI (complicated mild-to-severe) or OI. The study used a prospective, longitudinal, controlled design, with standardized psychiatric assessments conducted at baseline (reflecting pre-injury functioning) and 3 months post-injury. Assessments of pre-injury psychiatric, adaptive functioning, family adversity, and family psychiatric history status were conducted. Severity of injury was assessed by standard clinical scales. The outcome measure was the presence of a psychiatric disorder not present before the injury (“novel”), during the first 3 months after TBI. Enrolled participants (N=141) included children with TBI (N=75) and with OI (N=66). The analyses focused on 118 children (84%) (TBI: N=65; OI: N=53) who returned for follow-up assessment at 3 months. Novel psychiatric disorder (NPD) occurred significantly more frequently in the TBI (32/65; 49%) than the OI (7/53; 13%) group. This difference was not accounted for by pre-injury lifetime psychiatric status; pre-injury adaptive functioning; pre-injury family adversity, family psychiatric history, socioeconomic status, injury severity, or age at injury. Furthermore, none of these variables significantly discriminated between children with TBI who developed, versus those who did not develop, NPD. These findings suggest that children with complicated mild-to-severe TBI are at significantly higher risk than OI-controls for the development of NPD in the first 3 months after injury.
Traumatic brain injury (TBI) in children and adolescents is a major public health problem.1 Accumulated knowledge of psychiatric complications after pediatric TBI derives from over 20 cohorts, including 7 from our group,226 studied over the past 80 years. Other pediatric TBI studies that include behavioral outcomes, but not specifically psychiatric outcomes, complement the psychiatric literature.2731 However, there has only been one published study of pediatric TBI that used a standardized psychiatric interview, a prospective longitudinal design, and had an injured control group.3 That study included 60 children with TBI (31 with severe TBI, 29 with “mild” TBI) and 28 orthopedic injury (OI) controls studied at baseline (soon after injury), at 4 months, 12 months, and 27 months after injury. New psychiatric disorder developed in 48% of children (10/21) with “severe” TBI, in 15% of children (3/20) with “mild” TBI, and 5% of children (1/22) with OI in the first 4 months after injury. The onset of psychiatric disorders within the first 4 months after injury in the severe TBI group was associated with the child’s concurrent intellectual level. In children with severe TBI, pre-injury behavior predicted new psychiatric disorder at 12 months, and psychosocial adversity predicted new psychiatric disorder that persisted over two assessments. This seminal study has weaknesses, by contemporary standards, related to the use of one of the earliest versions of a standardized psychiatric interview for parents of children, direct children’s psychiatric assessment by a brief mental status exam only, and in the classification of TBI severity before common use of the Glasgow Coma Scale.32 Our attempts to estimate the reported severity of TBI in the 1981-published study by modern criteria suggest that individuals in the severe-TBI group would retain such classification, and that about ⅔ of the “mild-TBI” group (defined clinically by posttraumatic amnesia greater than 1 hour but less than 1 week) would retain such classification, whereas about ⅓ of the “mild-TBI” would be classified as complicated mild-or-moderate TBI.33 Another limitation of the older study was that children who were judged to have a psychiatric disorder before the injury were not considered eligible for the development of a “new psychiatric disorder.” In our psychiatric studies, which began in 1992, we coined the term “novel psychiatric disorder (NPD)” so that the outcome of interest would not be confused with “new psychiatric disorder” used in the landmark study. The new term was necessary to understand the development of psychopathology in children who have a pre-injury psychiatric disorder because this is very common in children with TBI.2 Novel psychiatric disorder (NPD) is therefore diagnosed in one of two conditions. The first condition coincides with the definition of new psychiatric disorder, and this could occur in a participant with no lifetime pre-injury psychiatric disorder who then develops a psychiatric disorder after injury. The second condition could occur in the case of a participant with a lifetime psychiatric disorder who then develops a post-injury psychiatric disorder that was never before present (e.g., a subject with a lifetime history of major depressive disorder who develops oppositional defiant disorder after the injury would receive the classification, but would not if only a new episode of major depression occurred).
We reported on NPD in an uncontrolled study involving 50 consecutively hospitalized children with uncomplicated mild-to-severe TBI who were recruited soon after injury and studied prospectively for 2 years.2,3436 NPD occurred in 45% of children (17/38) followed at 3 months post-injury, including 82% of children (9/11) with severe TBI and 30% of children (8/27) with mild-to-moderate TBI. Five of six models to account for NPD at 3 months were significantly predictive: severity of injury, lifetime psychiatric disorder, family psychiatric history, pre-injury family functioning, and socioeconomic status/pre-injury intellectual functioning.
We reported on NPD in a study of 24 consecutively hospitalized children with severe TBI, individually matched to 24 children hospitalized for mild TBI, and individually matched to 24 children hospitalized for OI.10 The children were studied retrospectively an average of 2 years after injury. Severe TBI was associated with a significantly higher rate of NPD (15/24; 63%), compared with children with mild TBI (5/24; 21%) and orthopedic injury (1/24; 4%). These findings could not be attributed to age at injury or assessment, gender, race, social class, pre-injury psychiatric disorders, family psychiatric history, family stress, or injury-to-assessment duration.
In accordance with previous findings, we hypothesized that: 1) NPD 3 months post-injury would be significantly increased in the TBI versus the OI group; 2) pre-injury psychiatric disorder, pre-injury psychosocial adversity, and greater-intensity family psychiatric history would be significantly associated with NPD; and 3) severity of TBI would be related to NPD.

Methods

Study procedures were approved by the institutional review boards of the participating organizations and complied with the NIH policies on human subjects. Participants with TBI or OI were recruited from consecutive admissions to medical centers in Dallas, Houston, and Miami. Inclusion of the OI group was intended to control for factors predisposing children to injury and for stress resulting from hospitalization. Children were age 7–17 years at the time of injury. Participants with TBI were included if they had a complicated mild-to-severe TBI. Severity of TBI classification was based on the lowest post-resuscitation score on the Glasgow Coma Scale (GCS),32 which was recorded from clinical notes. The GCS is the standard measure of severity of acute brain injury associated with TBI. The scale measures motor, eye-opening, and verbal responsiveness. Scores range from 3 (unresponsive) to 15 (normal). Severe TBI was defined by GCS scores of 3–8, moderate TBI by GCS scores of 9–12, and complicated mild TBI by GCS scores of 13–15, with brain lesions (contusions, hematomas) indicated by computed tomographic scans. The OI patients had mild-to-moderate orthopedic injuries as defined by the Abbreviated Injury Scale.37 The current investigation examined participants at baseline within 1 month after injury, and 3 months post-injury. All participants were English-speaking. Children were excluded if they had a previous head injury, penetrating gunshot wound to the brain, history of child abuse, preexisting neurologic disorders (e.g., mental retardation and epilepsy), pervasive developmental disorder, prematurity or low birth weight, hypoxia, or hypotension.

Psychiatric Measures

DSM-IV psychiatric diagnoses38 were derived by utilizing a semistructured interview, the Schedule for Affective Disorders and Schizophrenia for school-aged children, Present and Lifetime Version (K-SADS-PL).39 The K-SADS-PL is an integrated parent–child interview that generates diagnoses based on a clinician’s synthesizing data collected from parent and child separately, querying symptoms that were present in the weeks before injury and pre-injury lifetime symptoms (at baseline), and symptoms present or past from injury to 3 months (at 3-month assessment). The entire interview was completed by the parent, including the attention-deficit hyperactivity disorder (ADHD) supplement, regardless of whether the ADHD screen was positive. The interview of the children was shortened to relieve burden on the children, who also completed an extensive neurocognitive battery. All children completed the depression and anxiety disorder sections, and children 13 years and older also answered the conduct disorder, drugs, and alcohol sections.
The Neuropsychiatric Rating Schedule (NPRS)40 is a semistructured interview designed to identify symptoms and subtypes of personality change (PC) due to TBI.24,41,42 Both parents and children served as informants in the interview, which took place at baseline and at 3 months after injury. We specifically waived the 1-year duration of symptomatology criterion to allow us to monitor symptomatology that was clinically significant. The instrument has been shown to provide reliable and valid diagnoses of the common subtypes of PC.40 Previous studies have emphasized that PC is not a personality disorder, and its diagnosis does not require the assessment of personality. Rather, PC38 is diagnosed when the child presents with clinically significant affective lability, aggression, disinhibition, apathy, or paranoia.24,4043
Best-estimate psychiatric diagnoses44 were generated by the interviewer after integrating the reports of the parent and the child from the NPRS and the K-SADS interviews and, when available, from the Behavioral Assessment System for Children, 2nd Edition (BASC-2)45 and the Behavior Rating Inventory of Executive Function (BRIEF),46 completed by the teacher. The methodology of diagnoses generated by the clinician from interview and questionnaire data provided by multiple sources is designed to minimize the risk of over- or under-reporting that may occur with questionnaire-derived data only.47

Predictive Variables

Family Psychiatric History

The Family History Research Diagnostic Criteria48 interview was conducted by trained research assistants at each site. Criteria were modified to conform to DSM-IV criteria. At least one parent acted as the informant and was questioned about psychiatric disorders in each first-degree relative of the index child with TBI. Family ratings were then summarized for first-degree relatives, on a 4-point scale49 of increasing severity — 0: no family psychiatric disorder; 1: at least one family member met criteria for a psychiatric disorder, but no treatment was received; 2: a family member met criteria for a psychiatric disorder and has received outpatient treatment or been arrested for antisocial behavior; 3: a family member met criteria for a psychiatric disorder and has had inpatient psychiatric treatment or has been incarcerated.

Socioeconomic Status (SES)

The Socioeconomic Composite Index (SCI)50 was based on three variables: maternal education, coded on a 7-point scale, with values representing <7 years’ education to attainment of a graduate degree; the Duncan Occupational Status Index;51 and annual family income, based on an 8-point scale, ranging from <$20,000 to >$60,000, as part of the Life Stressors and Resources Scale (LISRES).52 These three variables were transformed into z-scores and then averaged together to yield a composite z-score, which was standardized (mean: 0; standard deviation [SD]: 1).

Psychosocial Adversity Measure

The Life Stressors and Social Resources Inventory–Adult Form (LISRES–A)52 was completed by parents. The Family Stressors score was computed as the mean of the T scores for the Stressors scales (Work, Health, Spouse, Extended Family, and Friends). The Family Resources score was defined as the mean of the T scores for Resource scales (Work, Spouse, Extended Family, and Friends).

Adaptive Functioning Measure

Pre-injury adaptive functioning was retrospectively assessed shortly after the injury by use of the Vineland Adaptive Behavior Scale interview.53 This assessment involved a semistructured interview with the primary caretaker, conducted by a trained research assistant. The Adaptive Behavior composite standard score was the predictive variable of interest.

Data Analysis

The analyses conducted included comparisons between the TBI versus OI groups, NPD versus no-NPD groups, and participants versus nonparticipants at 3 months. Fisher’s exact test and independent-sample t-tests were used to compare the groups for dependent variables that were categorical or continuous, respectively. To control for potentially confounding dependent variables, logistic regression was used when needed in analyses of NPD.

Results

A group of 141 subjects were recruited and participated in the “baseline” psychiatric assessment to record pre-injury psychiatric diagnoses. These included 75 children with TBI and 66 children with OI. Table 1 shows pre-injury characteristics of the participants. The TBI group was significantly older than the OI group (mean age [SD]: 13.4 [2.8] versus 12.0 [2.5]; t[139]=2.99; p=0.003). The groups differed significantly by race, with the OI having a higher representation of Black/Biracial children versus Caucasian/Asian children and Hispanic/American Indian children (χ2[2]=8.68; p=0.013). The groups were not significantly different in gender, socioeconomic composite index, pre-injury adaptive functioning, pre-injury family stressors, pre-injury family resources, and family psychiatric history. Table 2 shows that the groups were not significantly different in rates of the general category of pre-injury psychiatric disorder or specific pre-injury psychiatric disorders.
TABLE 1. Demographics and Injury Characteristics, Mean (standard deviation)
 TBI (N=75)OI (N=66)tdf
Age at injury, mean (SD)13.4 (2.8)12.0 (2.5)2.99139
Male (%)50 (67)47 (71)  
Race    
 Black1123  
 White3220  
 Hispanic3020  
 American Indian10  
 Asian01  
 Biracial12  
Socioeconomic Composite Index−0.0443 (0.833) N=740.0967 (0.834) N=63−0.99135
Pre-injury Adaptive Functioning95.3 (14.4) N=6399.0 (11.1) N=58−1.58119
Pre-injury Family Stressors46.7 (9.6) N=5748.5 (10.7) N=57−0.93112
Pre-injury Family Resources53.8 (10.3) N=5854.8 (10.7) N=57−0.51113
Pre-injury Family Psychiatric History1.24 (1.0) N=501.27 (1.1) N=59−0.15107
Mechanism of injury    
 Auto, truck, bus (driver/passenger)262  
 Motorcycle/moped75  
 RV/off-road71  
 Bicycle55  
 Fall1213  
 Falling object01  
 Sports/play432  
 Hit by motor vehicle (pedestrian)133  
 Other14  
All comparisons were nonsignificant except age at injury (p=0.003).
The OI group had a higher representation of Black/Biracial children versus Caucasian/Asian children and Hispanic/American Indian children (p=0.013)
TBI: traumatic brain injury; OI: orthopedic injury; SD: standard deviation.
TABLE 2. Pre-Injury Psychiatric Disorders in Children With TBI and OI, N (%)
 TBI (N=75)OI (N=66)
Pre-injury psychiatric disorder (current)35 (47%)28 (42%)
Lifetime psychiatric disorder (current + resolved)39 (52%)28 (42%)
Specific psychiatric disorders  
 Pre-injury ADHD (current)24 (32%)22 (33%)
 Lifetime pre-injury ADHD25 (33%)22 (33%)
 Pre-injury oppositional-defiant disorder (current)7 (9%)4 (6%)
 Lifetime pre-injury oppositional-defiant disorder8 (11%)5 (8%)
 Pre-injury externalizing disorder (current)28 (37%)22 (33%)
 Lifetime pre-injury externalizing disorder29 (39%)22 (33%)
 Pre-injury depressive disorder (current)5 (7%)3 (5%)
 Lifetime pre-injury depressive disorder8 (11%)3 (5%)
 Pre-injury anxiety disorder (current)13 (17%)12 (18%)
 Lifetime pre-injury anxiety disorder16 (21%)13 (20%)
 Pre-injury internalizing disorder (current)17 (23%)13 (15%)
 Lifetime pre-injury internalizing disorder22 (29%)14 (21%)
 Pre-injury drug abuse (current)2 (3%)0 (0%)
 Lifetime pre-injury drug abuse2 (3%)1 (2%)
All comparisons (Fisher’s exact test) were nonsignificant.
TBI: traumatic brain injury; OI: orthopedic injury; ADHD: attention-deficit/hyperactivity disorder.
Externalizing disorder consists of attention-deficit/hyperactivity disorder, oppositional-defiant disorder, or conduct disorder; internalizing disorder consists of any depressive disorder (e.g., major depression; dysthymic disorder; depressive disorder, not otherwise specified), or any anxiety disorder.

Occurrence

In all, 118 of the original 141 eligible children (84%) returned for the 3-month psychiatric assessment. The returning group was not significantly different from the children who did not return in age, gender, socioeconomic composite index, pre-injury adaptive functioning, and pre-injury psychiatric disorder status. However, Black/Biracial participants were less likely to return for follow-up (11/37 Black/Biracial, 3/53 Caucasian/Asian, and 9/51 Hispanic/American Indian children did not return; χ2[2]=9.35; p=0.009).
The distribution of NPD that occurred in the TBI and OI groups is shown in Table 3. NPD at any point within the first 3 months post-injury occurred significantly more in the TBI group (32/65; 49%) than the OI group (7/53, 13%; Fisher’s exact test: p<0.0005). Because age at injury was significantly different between the TBI and OI groups, we conducted a logistic-regression analysis, with NPD as the independent variable and group (TBI versus OI) and age at injury as the dependent variables. The regression was significant (−2 log likelihood χ2[2]=18.93;p=0.0001), although, of the dependent variables, only Group (TBI versus OI) was significant (Wald χ2[1]=15.51; p=0.0001), whereas age at injury was not significant. Similarly, NPD that was unresolved at the 3-month assessment occurred significantly more in the TBI group (32/65; 49%) than the OI group (5/53; 9%; Fisher’s exact test: p<0.0005). A corresponding logistic regression controlling for age at injury was significant (−2 log likelihood χ2[2]=24.09; p=0.0001), although, of the dependent variables, only Group (TBI versus OI) was significant (Wald χ2[1]=17.84; p=0.0000), whereas age at injury was not significant. The specific NPDs that occurred significantly more in the TBI versus the OI group were Personality Change disorder (22/65, 34% versus 0/53; Fisher’s exact test: p<0.0005) and Externalizing disorder (11/60, 18% versus 2/49, 4%; Fisher’s exact test: p=0.035). The subtypes of personality change occurred as follows: affective lability (N=21); disinhibited (N=15), aggressive (N=8), apathetic (N=1). Subtypes of novel ADHD in the TBI cohort included Inattentive (N=2), Combined (N=1), and Not otherwise specified (N=3). Novel ADHD in the OI group was Inattentive (N=1).
TABLE 3. Psychiatric Disorders in the First 3 Months After TBI and OI, N (%)
 TBI (N=65)OI (N=53)p
Novel psychiatric disorder (current)32 (49%)5 (9%)0.000
Novel psychiatric disorder (current + resolved)32 (49%)7 (13%)0.000
Novel psychiatric disorders   
 Personality change disorder (resolved)22/65 (0)0 (0)0.000
 ADHD (resolved)6/46 (0)1/32 (0)NS
 Oppositional-defiant disorder (resolved)5/57 (0)1/49 (0)NS
 Externalizing disorder (resolved)11/60 (0)2/49 (0)0.035
 Anxiety disorder (resolved)10/65 (0)4/53 (1)NS
 Depressive disorder (resolved)5/59 (1)1/51 (1)NS
 Internalizing disorder (resolved)12/65 (0)5/53 (2)NS
 Drug abuse (resolved)1/64 (0)1/52 (0)NS
TBI: traumatic brain injury; OI: orthopedic injury; ADHD: attention-deficit/hyperactivity disorder.
The denominators fluctuate depending on eligibility to develop a specific NPD (e.g., a child with only pre-injury ADHD can develop oppositional-defiant disorder and therefore count as a novel externalizing disorder, but a child with pre-injury ADHD and ODD would not be eligible to develop a novel externalizing disorder. The drug abuse in the child with TBI consisted of both alcohol and cannabis abuse, and cannabis abuse alone in the child with OI.
The hypothesized predictors of NPD were first examined with the combined TBI and OI cohort (Table 4). Socioeconomic composite index, lifetime pre-injury psychiatric disorder, pre-injury adaptive functioning, pre-injury family stressors, and pre-injury family psychiatric history were not significantly related to NPD in the first 3 months after injury. Pre-injury family resources were nonsignificantly higher in the NPD group (p=0.096 [NS]); neither was age at injury associated with NPD. There was a trend for girls to have a higher rate of NPD (18/40 [45%] versus 21/78 [27%]; Fisher’s exact test: p=0.063 [NS]). Also, there was a trend for Blacks/Biracial versus Caucasian/Asian and Hispanic/American Indian children to have a lesser rate of NPD (Fisher’s exact test: p=0.087 [NS]). This was most likely due to the overrepresentation of this group in the OI group, which had a significantly lower incidence of NPD.
TABLE 4. Predictors of Novel Psychiatric Disorder 3 Months After TBI and OI
All ParticipantsNovel Psychiatric Disorder (N=39)No Novel Psychiatric Disorder (N=79)tdfp
Age at injury12.9 (3.2)12.7 (2.6)−0.35116NS
Gender    0.063
 Male (%)21/78 (27%)57/78 (73%)
 Female (%)18/40 (45%)22/40 (55%)
Race   20.087
 Black4 (15%)22 (85%)   
 White/Asian20 (40%)30 (60%)   
 Hispanic/American Indian15 (36%)27 (64%)   
Socioeconomic Composite Index0.023 (0.86)0.092 (0.86)0.41116NS
Lifetime pre-injury psychiatric disorder21/39 (54%)38/79 (48%)  NS
Pre-injury Adaptive Functioning96.9 (11.5) N=3595.9 (11.6) N=68−0.38101NS
Pre-injury Family Stressors47.6 (10.7) N=2947.7 (9.9) N=700.0697NS
Pre-injury Family Resources56.7 (9.4) N=3052.8 (11.0) N=70−1.68980.096
Pre-injury Family Psychiatric History1.4 (1.1) N=261.3 (1.0) N=65 89NS
TBI Participants OnlyNovel Psychiatric Disorder (N=32)No Novel Psychiatric Disorder (N=33)tdfp
Glasgow Coma Scale score, mean (SD)7.2 (4.9)8.3 (4.2)1.0263NS
Age at injury, mean (SD)13.1 (3.2)13.7 (2.6)0.9263NS
Gender (%)    0.072
 Male17/42 (40%)25/42 (60%)
 Female15/23 (65%)8/23 (35%)
Race   2NS
 Black4 (50%)4 (50%)   
 White/Asian16 (53%)14 (47%)   
 Hispanic/American Indian12 (44%)15 (56%)   
Socioeconomic Composite Index0.003 (0.87)−0.090 (0.87)−0.4363NS
Lifetime pre-injury psychiatric disorder18/32 (56%)15/33 (45%)  NS
Pre-injury Adaptive Functioning95.9 (16.9) N=2892.1 (10.3) N=27−1.0253NS
Pre-injury Family Stressors48.8 (11.2) N=2244.9 (8.0) N=28−1.4248NS
Pre-injury Family Resources55.8 (10.3) N=2352.9 (11.0) N=28−0.9849NS
Pre-injury Family Psychiatric History1.53 (1.02) N=191.04 (0.98) N=25−1.6042NS
Values are mean (standard deviation), unless otherwise indicated.
TBI: traumatic brain injury; OI: orthopedic injury; SD: standard deviation.
The analyses were repeated with the TBI group alone because of the relatively low frequency of NPD in the OI group. A very similar pattern was evident, in that socioeconomic composite index, lifetime pre-injury psychiatric disorder, pre-injury adaptive functioning, pre-injury family stressors, pre-injury family resources, pre-injury family psychiatric history, and age were not significantly related to NPD in the first 3 months after injury. In these analyses, race was not associated with NPD, but girls again showed a trend toward a higher rate of NPD (15/23 [65%] versus 17/42 [40%]; Fisher’s exact test: p=0.072 [NS]).
Severity of injury, as measured by the Glasgow Coma Scale, did not predict NPD (Table 4). The incidence of NPD by severity of injury categories was as follows: severe TBI 22/39 (56%), moderate TBI 2/11 (18%), and complicated mild TBI 8/15 (53%).

Discussion

This study is only the second prospective, controlled psychiatric study of pediatric TBI in which a standardized psychiatric interview assessment was conducted. The first study of its kind was published three decades ago, when assessment and treatment protocols were very different. Despite the passage of time, the findings of the two studies are remarkably similar. The major finding in the current study is that the development of NPD within the first 3 months after TBI (49%) occurs significantly more commonly than after OI (13%). As in most studies of pediatric TBI, NPD consisted of a heterogeneous set of specific disorders.3,35 The most frequent NPD was personality change due to a general-medical condition,24,4143 characterized most commonly by affective lability, then disinhibition, aggression, rarely apathy, and no paranoia subtypes. The next most frequent disorders were internalizing disorder, externalizing disorder, anxiety disorder, ADHD, oppositional-defiant disorder, and depressive disorder. Only personality change and externalizing disorders occurred significantly more commonly in the TBI group. The TBI and OI groups were well matched and were not significantly different in socioeconomic status, gender, pre-injury adaptive functioning, pre-injury family stressors, pre-injury family resources, pre-injury family psychiatric history, a general category of pre-injury psychiatric disorder, and specific pre-injury psychiatric disorders. The OI group was significantly younger, but when age was controlled in regression analyses, Group (TBI versus OI) and not age at injury was significantly related to NPD. Race was significantly different between the TBI and OI groups, with an overrepresentation of Black/Biracial children in the OI group. Furthermore, Black/Biracial children had a significantly lower rate of follow-up at 3 months, such that participants at 3 months were not significantly different with regard to race.
Surprisingly, none of the other hypothesized predictive variables, including lifetime pre-injury psychiatric disorder, SES, pre-injury adaptive functioning, pre-injury family stressors, pre-injury family resources, pre-injury family psychiatric history, and severity of TBI were significantly related to NPD. Neither were age, gender, or race related to NPD. Larger studies may shed light on whether the trend for higher rates of NPD among girls holds true, and, if so, additional research on a possible hormonal influence on NPD may prove fruitful.
The principal data that guided our hypotheses regarding predictors of NPD were the 3-month follow-up results from our first prospective, uncontrolled psychiatric interview study of pediatric TBI.2 These results demonstrated a significant relationship of NPD with severity of injury, lifetime psychiatric disorder, family psychiatric history, pre-injury family functioning, and socioeconomic status/pre-injury intellectual functioning. The main difference in the current study and our earlier study was that patients with uncomplicated mild TBI were excluded from the current study, but constituted 50% of the sample in the earlier study. The expansion of the range of injury severity would have the tendency to elicit a relationship of severity of injury to NPD because of expected lower rates in children with uncomplicated mild TBI. It is unclear why psychosocial variables were not significant predictors of NPD. One possible explanation is that over two-thirds of the cases classified as NPD were accounted for by personality change, which is significantly related to injury variables, rather than psychosocial variables, especially in the first year after TBI.24,41,43 Different sets of predictors of NPD are significant, depending on time elapsed since injury.2,3436 It has been postulated that injury-related variables have a greater influence on outcome relative to psychosocial variables the shorter the elapsed time since injury.3 The opposite was found related to the specific outcome of oppositional-defiant symptoms, where the symptoms proved to be transient in less-severely injured participants and persistent in more-severely injured participants.54
There is the presumption that the reason that NPD was more frequent in the TBI versus the OI group is because brain damage combined with the emotional trauma inherent in children who suffer TBI is more potent in generating new-onset psychopathology than emotional trauma without brain damage in children with OI. Yet the relatively crude measure of severity of brain injury, the GCS, did not predict which children with TBI would develop NPD. A follow-up manuscript focuses on the association of NPD and structural neuroimaging modalities, including diffusion tensor imaging, volumetric analysis of regions of interest and lesions, and cortical thickness.55
The findings of this study must be considered within its limitations. Interrater reliability assessments for the diagnosis of NPD were not directly tested based on videotaped interviews. However, the child psychologists at each site closely supervised the assessments; and, furthermore, fidelity in diagnosis was maintained across sites by frequent telephone conferences and transmission of written summaries of psychiatric assessments that were critiqued by the first author and other interviewers, resulting in a consensus diagnosis. The psychiatric interviewers were not blind to the group status of participants (TBI or OI). However, in previous studies of pediatric TBI by our own group10 and others,3 unblinded and blinded ratings were very similar and did not influence the findings. As in many long-term follow-up studies, attrition was an issue, at 16%. However, participants versus nonparticipants at 3 months were not significantly different in multiple demographic and psychosocial variables, except that Black/Biracial children had a higher nonparticipation rate.
The study had a number of strengths. Three decades after the first, this was only the second, and now, largest, prospective, longitudinal, controlled psychiatric study of pediatric TBI using standardized interviews. The study used updated and in-depth psychosocial and injury-related variables to document pre-injury, injury, and post-injury status. The depth and breadth of measures were extensive and included interview measures of psychopathology, family psychiatric history, and adaptive functioning, as well as rating scales of injury and other psychosocial risk factors for NPD.

Conclusions And Implications

Psychiatric disorders frequently follow brain injury in children and occur at significantly higher rates than after orthopedic injury without brain injury. TBI is common and is a major public health problem. Dealing with this problem requires intervention at the level of prevention of injury, early recognition, and treatment of post-injury psychiatric disorders. Understanding the biological basis of NPD and the functional impairments they induce will be important in the development and delivery of effective biopsychosocial treatments. Future manuscripts will examine the association of NPD with neurocognitive variables and also examine injury, neuroimaging, and psychosocial correlates of specific NPDs, such as personality change. The understanding of brain–behavior relationships will also be enhanced with the examination of the post-injury course of pre-injury psychiatric disorders, which are quite common.

Acknowledgments

This work was completed at the Department of Psychiatry, University of California, San Diego, and Rady Children’s Hospital, San Diego.

Footnote

Disclosures: Drs. Max and Bigler independently provide expert testimony in cases of traumatic brain injury on an ad-hoc basis for plaintiffs and defendants in a more-or-less equal ratio. This activity constitutes approximately 5% of their respective professional activities. The other authors have no disclosures.

References

1.
Langlois JA, Rutland-Brown W, Thomas KE: The incidence of traumatic brain injury among children in the United States: differences by race. J Head Trauma Rehabil 2005; 20:229–238
2.
Max JE, Smith WL, Sato Y, et al.: Traumatic brain injury in children and adolescents: psychiatric disorders in the first three months. J Am Acad Child Adolesc Psychiatry 1997; 36:94–102
3.
Brown G, Chadwick O, Shaffer D, et al.: A prospective study of children with head injuries, III: psychiatric sequelae. Psychol Med 1981; 11:63–78
4.
Massagli TL, Fann JR, Burington BE, et al.: Psychiatric illness after mild traumatic brain injury in children. Arch Phys Med Rehabil 2004; 85:1428–1434
5.
Black P, Jeffries JJ, Blumer D, et al: The posttraumatic syndrome in children: characteristics and incidence, in The Late Effects of Head Injury. Edited by Walker AE, Caveness WF, Critchley M, and the Research Group on Head Injuries. Springfield, IL, C.C. Thomas, 1969, pp 142–149 (chapter 114)
6.
Hjern B, Nylander I: Acute head injuries in children: traumatology, therapy, and prognosis. Acta Paediatr 1964; 152; Stockholm, Sweden: Almqvist & Wiksells Boktryckeri AB. 36
7.
Luis CA, Mittenberg W: Mood and anxiety disorders following pediatric traumatic brain injury: a prospective study. J Clin Exp Neuropsychol 2002; 24:270–279
8.
Bloom DR, Levin HS, Ewing-Cobbs L, et al.: Lifetime and novel psychiatric disorders after pediatric traumatic brain injury. J Am Acad Child Adolesc Psychiatry 2001; 40:572–579
9.
Lehmkuhl G, Thoma W: Development in children after severe head injury, in Brain and Behavior in Child Psychiatry. Edited by, Rothenberger A. Berlin, New York, Springer-Verlag, 1990, pp 267–282
10.
Max JE, Koele SL, Smith WL, et al.: Psychiatric disorders in children and adolescents after severe traumatic brain injury: a controlled study. J Am Acad Child Adolesc Psychiatry 1998; 37:832–840
11.
Shaffer D, Chadwick O, Rutter M: Psyciatric outcome of localized head injury in children, in Outcome of Severe Damage to the Central Nervous System. Edited by, Ciba F. Amsterdam, New York, Elsevier, 1975, pp 191–213
12.
Rune V: Acute head injuries in children: a retrospective epidemiologic, child psychiatric, and electroencephalographic study on primary school children in Umea. Acta Paediatr Scand Suppl 1970; 209(Suppl):209-, 3–12
13.
Max JE, Lindgren SD, Knutson C, et al.: Child and adolescent traumatic brain injury: psychiatric findings from a paediatric outpatient specialty clinic. Brain Inj 1997; 11:699–711
14.
Bender L (ed): Personality problems of the child with a head injury, in Psychopathology of Children With Organic Brain Disorders. Springfield, IL, C.C. Thomas, 1956, pp 66–96
15.
Blau A: Mental changes following head trauma in children. Arch Neurol Psychiatry (Chicago) 1936; 35:723–769
16.
Strecker EA, Ebaugh FG: Neuropsychiatric sequelae of cerebral trauma in children. Arch Neurol Psychiatry 1924; 12:443–453
17.
Max JE, Sharma A, Qurashi MI: Traumatic brain injury in a child psychiatry inpatient population: a controlled study. J Am Acad Child Adolesc Psychiatry 1997; 36:1595–1601
18.
Harrington JA and Letemendia FJJ: Persistent psychiatric disorders after head injuries in children. J Ment Sci 1958; (Oct.):1205–1218
19.
Kasanin J: Personality changes in children following cerebral trauma. J Nerv Ment Dis 1929; 69:385–406
20.
Max JE, Dunisch DL: Traumatic brain injury in a child psychiatry outpatient clinic: a controlled study. J Am Acad Child Adolesc Psychiatry 1997; 36:404–411
21.
Otto U: [The postconcussion syndrome in children]. Acta Paedopsychiatr 1960; 27:6–20
22.
Dillon H, Leopold RL: Children and the post-concussion syndrome. JAMA 1961; 175:86–92
23.
Max JE, Bowers WA, Baldus D, et al.: Pediatric traumatic brain injury and burn patients in the civil justice system: the prevalence and impact of psychiatric symptomatology. J Am Acad Psychiatry Law 1998; 26:247–258
24.
Max JE, Levin HS, Schachar RJ, et al.: Predictors of personality change due to traumatic brain injury in children and adolescents six to twenty-four months after injury. J Neuropsychiatry Clin Neurosci 2006; 18:21–32
25.
Keenan HT, Hall GC and Marshall SW: Early head injury and attention deficit hyperactivity disorder: retrospective cohort study. BMJ 2008; 337:a1984
26.
Vasa RA, Grados M, Slomine B, et al.: Neuroimaging correlates of anxiety after pediatric traumatic brain injury. Biol Psychiatry 2004; 55:208–216
27.
Anderson V, Le Brocque R, Iselin G, et al.: Adaptive ability, behavior, and quality of life pre- and posttraumatic brain injury in childhood. Disabil Rehabil 2012; 34:1639–1647
28.
Babikian T, Satz P, Zaucha K, et al.: The UCLA Longitudinal Study of Neurocognitive Outcomes Following Mild Pediatric Traumatic Brain Injury. J Int Neuropsychol Soc 2011; 17:886–895
29.
Taylor HG, Yeates KO, Wade SL, et al.: Influences on first-year recovery from traumatic brain injury in children. Neuropsychology 1999; 13:76–89
30.
Yeates KO, Kaizar E, Rusin J, et al.: Reliable change in postconcussive symptoms and its functional consequences among children with mild traumatic brain injury. Arch Pediatr Adolesc Med 2012
31.
Fay GC, Jaffe KM, Polissar NL, et al.: Outcome of pediatric traumatic brain injury at three years: a cohort study. Arch Phys Med Rehabil 1994; 75:733–741
32.
Teasdale G, Jennett B: Assessment of coma and impaired consciousness: a practical scale. Lancet 1974; 2:81–84
33.
Rutter M, Chadwick O, Shaffer D, et al.: A prospective study of children with head injuries, I: design and methods. Psychol Med 1980; 10:633–645
34.
Max JE, Lindgren SD, Robin DA, et al.: Traumatic brain injury in children and adolescents: psychiatric disorders in the second three months. J Nerv Ment Dis 1997; 185:394–401
35.
Max JE, Robin DA, Lindgren SD, et al.: Traumatic brain injury in children and adolescents: psychiatric disorders at two years. J Am Acad Child Adolesc Psychiatry 1997; 36:1278–1285
36.
Max JE, Robin DA, Lindgren SD, et al.: Traumatic brain injury in children and adolescents: psychiatric disorders at one year. J Neuropsychiatry Clin Neurosci 1998; 10:290–297
37.
Association for the Advancement of Automotive Medicine: Abbreviated Injury Scale, 1990 Revision. Des Plaines, IL, Association for the Advancement of Automotive Medicine, 1990
38.
American Psychiatric Association: Diagnostic and Statistical Manual of Mental Disorders, 4th Ed., TR. Washington, DC, American Psychiatric Press, 2000
39.
Kaufman J, Birmaher B, Brent D, et al.: Schedule for Affective Disorders and Schizophrenia for School-Age Children-Present and Lifetime Version (K-SADS-PL): initial reliability and validity data. J Am Acad Child Adolesc Psychiatry 1997; 36:980–988
40.
Max JE, Castillo CS, Lindgren SD, et al.: The Neuropsychiatric Rating Schedule: reliability and validity. J Am Acad Child Adolesc Psychiatry 1998; 37:297–304
41.
Max JE, Levin HS, Landis J, et al.: Predictors of personality change due to traumatic brain injury in children and adolescents in the first six months after injury. J Am Acad Child Adolesc Psychiatry 2005; 44:434–442
42.
Max JE, Robertson BAM, Lansing AE: The phenomenology of personality change due to traumatic brain injury in children and adolescents. J Neuropsychiatry Clin Neurosci 2001; 13:161–170
43.
Max JE, Koele SL, Castillo CC, et al.: Personality change disorder in children and adolescents following traumatic brain injury. J Int Neuropsychol Soc 2000; 6:279–289
44.
Leckman JF, Sholomskas D, Thompson WD, et al.: Best estimate of lifetime psychiatric diagnosis: a methodological study. Arch Gen Psychiatry 1982; 39:879–883
45.
Reynolds CR, Kamphaus RW: Behavioral Assessment System for Children, 2nd Edition (BASC-2). Circle Pines, MN, AGS Publishing, 2004
46.
Gioia GA, Isquith PK, Guy SC, et al.: Behavior Rating Inventory of Executive Function. Child Neuropsychol 2000; 6:235–238
47.
Fletcher JM, Ewing-Cobbs L, Miner ME, et al.: Behavioral changes after closed head injury in children. J Consult Clin Psychol 1990; 58:93–98
48.
Andreasen NC, Endicott J, Spitzer RL, et al.: The family history method using diagnostic criteria: reliability and validity. Arch Gen Psychiatry 1977; 34:1229–1235
49.
Max JE, Arndt S, Castillo CS, et al.: Attention-deficit hyperactivity symptomatology after traumatic brain injury: a prospective study. J Am Acad Child Adolesc Psychiatry 1998; 37:841–847
50.
Yeates KO, Taylor HG, Drotar D, et al.: Pre-injury family environment as a determinant of recovery from traumatic brain injuries in school-age children. J Int Neuropsychol Soc 1997; 3:617–630
51.
Stevens G, Featherman DL: A revised socioeconomic index of occupational status. Soc Sci Res 1981; 10:364–395
52.
Moos R, Moos B: Life Stressors and Social Resources InventoryAdult Form: Professional Manual. Odessa, FL, Psychological Assessment Resources, Inc., 1994
53.
Sparrow SS, Cicchetti DV, Balla DA: Vineland Adaptive Behavior Scales, 2nd Edition. Circle Pines, MN, American Guidance Services, 2005
54.
Max JE, Castillo CS, Bokura H, et al.: Oppositional defiant disorder symptomatology after traumatic brain injury: a prospective study. J Nerv Ment Dis 1998; 186:325–332
55.
Max JE, Wilde EA, Bigler ED, et al.: Neuroimaging correlates of novel psychiatric disorders after pediatric traumatic brain injury. J Am Acad Child Adolesc Psychiatry (in press)

Information & Authors

Information

Published In

Go to The Journal of Neuropsychiatry and Clinical Neurosciences
Go to The Journal of Neuropsychiatry and Clinical Neurosciences
The Journal of Neuropsychiatry and Clinical Neurosciences
Pages: 427 - 436
PubMed: 23224448

History

Received: 20 June 2012
Accepted: 31 August 2012
Published online: 1 October 2012
Published in print: Fall 2012

Authors

Details

Jeffrey E. Max, M.B.B.Ch.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Elisabeth A. Wilde, Ph.D.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Erin D. Bigler, Ph.D.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Marianne MacLeod, M.A.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Ana C. Vasquez, B.S.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Adam T. Schmidt, Ph.D.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Sandra B. Chapman, Ph.D.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Gillian Hotz, Ph.D.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Tony T. Yang, M.D., Ph.D.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).
Harvey S. Levin, Ph.D.
From the Dept. of Psychiatry, Univ. of California San Diego, Rady Children's Hospital (JEM); Dept. of Physical Medicine & Rehabilitation, Baylor College of Medicine, Houston, TX (EAW, MM, ACV, ATS, HSL); Dept. of Psychology & Neuroscience, Brigham Young Univ., Provo, UT (EDB); Center for BrainHealth, Univ. of Texas, Dallas, TX (SC); Dept. of Neurosurgery, Univ. of Miami, Miller School of Medicine, Miami, FL (GH); Dept. of Psychiatry, Univ. of California San Francisco, San Francisco, CA (TTY).

Notes

Send correspondence to: Jeffrey E. Max, M.B.B.Ch., Rady Children's Hospital, 3020 Children’s Way, MC 5018, San Diego, CA 92123; e-mail: [email protected]

Funding Information

This study was supported by National Institute of Mental Health (NIMH) Grant K-08 MH01800 (Dr. Max) and National Institute of Neurological Disorders and Stroke (NINDS) Grant NS-21889 (Dr. Levin).

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