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5. Young Adult ADHD Symptoms in the General Population and Neurocognitive Impairment.

Author

Agha, Sharifah Shameem, Riglin, Lucy, Carbury, Rhian, Blakey, Rachel, Shakeshaft, Amy, Thapar, Ajay K., Tilling, Kate, Collishaw, Stephan, Stergiakouli, Evie, Thapar, Anita, and Langley, Kate

Subjects
YOUNG adults, ATTENTION-deficit hyperactivity disorder, RESPONSE inhibition, SYMPTOMS, TASK performance
Abstract

Objective: Neurocognitive impairments are associated with child and adult ADHD in clinical settings. However, it is unknown whether adult ADHD symptoms in the general population are associated with the same pattern of cognitive impairment. We examined this using a prospective, population-based cohort spanning birth to age 25 years. Methods: We examined associations between self-reported adult ADHD symptoms and cognitive task performance (attention and response inhibition) in adulthood and childhood. Results: Self-rated ADHD symptoms at age 25 were associated with poorer performance in age 25 cognitive tasks capturing ADHD-related functioning (attention B = −0.03, 95% CI [0.05, −0.01], p =.005; response inhibition B = −0.03, 95% CI [−0.05, −0.01], p =.002). Conclusions: Neurocognitive impairments linked to adult ADHD symptoms in the general population, are similar to those found in people with childhood ADHD symptoms and are consistent with findings in adult ADHD clinical samples. [ABSTRACT FROM AUTHOR]

Published
2024
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7. Childhood attention-deficit hyperactivity disorder problems and mid-life cardiovascular risk: prospective population cohort study.

Author

Thapar, Ajay K., Riglin, Lucy, Blakey, Rachel, Collishaw, Stephan, Davey Smith, George, Stergiakouli, Evie, Tilling, Kate, and Thapar, Anita

Subjects
ATTENTION-deficit hyperactivity disorder, CARDIOVASCULAR diseases risk factors, MIDDLE age, COHORT analysis, BODY mass index
Abstract

Background: It is well-known that childhood attention-deficit hyperactivity disorder (ADHD) is associated with later adverse mental health and social outcomes. Patient-based studies suggest that ADHD may be associated with later cardiovascular disease (CVD) but the focus of preventive interventions is unclear. It is unknown whether ADHD leads to established cardiovascular risk factors because so few cohort studies measure ADHD and also follow up to an age where CVD risk is evident. Aims: To examine associations between childhood ADHD problems and directly measured CVD risk factors at ages 44/45 years in a UK population-based cohort study (National Child Development Study) of individuals born in 1958. Method: Childhood ADHD problems were defined by elevated ratings on both the parent Rutter A scale and a teacher-rated questionnaire at age 7 years. Outcomes were known cardiovascular risk factors (blood pressure, lipid measurements, body mass index and smoking) at the age 44/45 biomedical assessment. Results: Of the 8016 individuals assessed both during childhood and at the biomedical assessment 3.0% were categorised as having childhood ADHD problems. ADHD problems were associated with higher body mass index (B = 0.92 kg/m2, s.d. = 0.27–1.56), systolic (3.5 mmHg, s.d. = 1.4–5.6) and diastolic (2.2 mmHg, s.d. = 0.8–3.6) blood pressure, triglyceride levels (0.24 mol/l, s.d. = 0.02–0.46) and being a current smoker (odds ratio OR = 1.6, s.d. = 1.2–2.1) but not with LDL cholesterol. Conclusions: Childhood ADHD problems predicted multiple cardiovascular risk factors by mid-life. These findings, when taken together with previously observed associations with cardiovascular disease in registries, suggest that individuals with ADHD could benefit from cardiovascular risk monitoring, given these risk factors are modifiable with timely intervention. [ABSTRACT FROM AUTHOR]

Published
2023
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11. Validation of the Strengths and Difficulties Questionnaire (SDQ) emotional subscale in assessing depression and anxiety across development.

Author

Armitage, Jessica May, Tseliou, Foteini, Riglin, Lucy, Dennison, Charlotte, Eyre, Olga, Bevan Jones, Rhys, Rice, Frances, Thapar, Ajay K., Thapar, Anita, and Collishaw, Stephan

Subjects
ANXIETY disorders, MENTAL depression, ANXIETY, GENERALIZED anxiety disorder, LONGITUDINAL method
Abstract

Emotional disorders are common in childhood, and their prevalence sharply increases during adolescence. The Strengths and Difficulties Questionnaire (SDQ) is widely used for screening emotional and behavioural difficulties in children and young people, but little is known about the accuracy of the emotional subscale (SDQ-E) in detecting emotional disorders, and whether this changes over development. Such knowledge is important in determining whether symptom changes across age are due to developmental or measurement differences. This study assessed the validity of the SDQ-E and two individual items (low mood and general worry) in differentiating between cases and non-cases of Major Depressive Disorder (MDD), Generalised Anxiety Disorder (GAD), and other anxiety disorders across ages 7, 10, 13, 15, and 25 years in a UK population cohort. Analyses showed moderate accuracy of the subscale in discriminating cases of MDD (AUC = 0.67–0.85), and high accuracy for discriminating cases of GAD (AUC = 0.80–0.93) and any anxiety disorder (AUC = 0.74–0.83) compared to non-cases. The SDQ-E performed well across ages and sex, and generally performed better than the two individual items. Together our findings validate the SDQ-E as a screen for emotional disorders during childhood, adolescence, and early adulthood, and as a tool for longitudinal research on depression and anxiety disorders. [ABSTRACT FROM AUTHOR]

Published
2023
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20. Commentary

Author

Jones, Rhys Bevan, Thapar, Ajay K, and Thapar, Anita

Published
2012

21. Variable Emergence of Autism Spectrum Disorder Symptoms From Childhood to Early Adulthood.

Author

Riglin, Lucy, Wootton, Robyn E., Thapar, Ajay K., Livingston, Lucy A., Langley, Kate, Collishaw, Stephan, Tagg, Jack, Smith, George Davey, Stergiakouli, Evie, Tilling, Kate, and Thapar, Anita

Subjects
AUTISM spectrum disorders, ADULTS, SYMPTOMS, NATURAL history, COMMUNICATION barriers
Abstract

Objective: Autism spectrum disorder (ASD) is currently considered an early-onset neurodevelopmental condition. Follow-up studies of clinic-ascertained autism suggest that autistic symptoms typically decline with age, although symptom improvement is limited for some. To date there have been no population-based prospective studies investigating the natural history of autistic symptoms from childhood to adulthood. The aim of this study was to characterize the development and heterogeneity of autistic symptoms in a population-based cohort from childhood to age 25.Methods: Data were analyzed in a prospective U.K. population-based cohort (ALSPAC). Trajectories were derived using five assessments of the parent-rated Social and Communication Disorders Checklist (SCDC) spanning ages 7-25. Additional measures were used to validate symptom trajectories.Results: Three distinct SCDC symptom trajectory classes were identified: low (88.5%), declining (5.0%), and late-emerging (6.5%). Both the declining and late-emerging trajectory classes were associated with child and adult ASD measures, low IQ, communication problems, peer problems, and worse adult functioning compared with the low trajectory class. Male sex was associated with a higher likelihood of being in the declining trajectory class (odds ratio=2.84, 95% CI=2.19, 3.69). This sex difference was not observed in the late-emerging class (odds ratio=1.00, 95% CI=0.80, 1.24) compared with the low trajectory class.Conclusions: ASD symptom levels that emerged early tended to decline across development, although impairment was still present in adulthood for some. For others, autistic symptoms emerged across adolescence and adulthood. This challenges our current understanding that ASD symptoms inevitably first manifest early in development. [ABSTRACT FROM AUTHOR]

Published
2021
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22. ADHD and depression: investigating a causal explanation.

Author

Riglin, Lucy, Leppert, Beate, Dardani, Christina, Thapar, Ajay K., Rice, Frances, O'Donovan, Michael C., Davey Smith, George, Stergiakouli, Evie, Tilling, Kate, and Thapar, Anita

Subjects
MENTAL depression risk factors, GENETICS, CONFIDENCE intervals, ATTENTION-deficit hyperactivity disorder, RISK assessment, DISEASE relapse, COMPARATIVE studies, ATTRIBUTION (Social psychology), GENOMES, ODDS ratio, CAUSALITY (Physics), LONGITUDINAL method, DISEASE complications, CHILDREN, ADULTS
Abstract

Background: Attention-deficit hyperactivity disorder (ADHD) is associated with later depression and there is considerable genetic overlap between them. This study investigated if ADHD and ADHD genetic liability are causally related to depression using two different methods. Methods: First, a longitudinal population cohort design was used to assess the association between childhood ADHD (age 7 years) and recurrent depression in young-adulthood (age 18–25 years) in N = 8310 individuals in the Avon Longitudinal Study of Parents and Children (ALSPAC). Second, two-sample Mendelian randomization (MR) analyses examined relationships between genetic liability for ADHD and depression utilising published Genome-Wide Association Study (GWAS) data. Results: Childhood ADHD was associated with an increased risk of recurrent depression in young-adulthood (OR 1.35, 95% CI 1.05–1.73). MR analyses suggested a causal effect of ADHD genetic liability on major depression (OR 1.21, 95% CI 1.12–1.31). MR findings using a broader definition of depression differed, showing a weak influence on depression (OR 1.07, 95% CI 1.02–1.13). Conclusions: Our findings suggest that ADHD increases the risk of depression later in life and are consistent with a causal effect of ADHD genetic liability on subsequent major depression. However, findings were different for more broadly defined depression. [ABSTRACT FROM AUTHOR]

Published
2021
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23. Investigating attention‐deficit hyperactivity disorder and autism spectrum disorder traits in the general population: What happens in adult life?

Author

Riglin, Lucy, Leppert, Beate, Langley, Kate, Thapar, Ajay K., O'Donovan, Michael C., Davey Smith, George, Stergiakouli, Evie, Tilling, Kate, and Thapar, Anita

Subjects
COGNITION disorder risk factors, MENTAL illness risk factors, SELF-evaluation, ATTENTION-deficit hyperactivity disorder, COMMUNICATIVE disorders, SEX distribution, AUTISM, LEARNING disabilities, SECONDARY analysis, DISEASE risk factors
Abstract

Background: Attention‐deficit hyperactivity disorder (ADHD) and autism spectrum disorder (ASD) are generally considered early‐onset disorders so most research has therefore tended to focus on children. Differences between ADHD/ASD in adult life and childhood have been noted, but few population‐based studies have examined them in adulthood. Furthermore, the interpretation of findings is hampered by changes in measure and from parent report to self‐report. Method: We examined continuous/trait measures of parent‐ and self‐rated ADHD and ASD in adulthood (age 25 years) in a UK prospective longitudinal sample ALPSAC (the Avon Longitudinal Study of Parents and Children), using many of the same measures that parents reported on in childhood (N = 6,064). Our aim was to investigate these traits in this population for mean‐level sex differences, overlaps with other cognitive, learning and communication problems and their associations with polygenic risk scores (PRS) for neuropsychiatric disorders (ADHD, ASD, schizophrenia, depression and anxiety). Results: ADHD and ASD traits in adulthood, as in childhood, showed associations with childhood cognitive, learning and communication problems and adult communication/language measures, although less so for self‐ratings than parent‐ratings. Males had higher ADHD and ASD trait levels, but this was not as marked as in childhood. In adulthood, ADHD (both parent‐ and self‐rated) and ASD (parent‐rated) symptoms showed associations with ADHD PRS; self‐reported ADHD also showed association with depression PRS, whereas self‐reported ASD did not show strong PRS associations. Conclusions: Our findings suggest that in young adults, ADHD and ASD symptoms have similar characteristics as they do in childhood. Associations with other cognitive, learning and communication problems, and ADHD PRS were somewhat less pronounced for self‐reported adult ADHD and ASD symptoms, suggesting that even at age 25, parent reports, where available, could be clinically useful. [ABSTRACT FROM AUTHOR]

Published
2021
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24. Assessment of age-at-onset criterion for adult attention-deficit hyperactivity disorder.

Author

Riglin, Lucy, Blakey, Rachel, Langley, Kate, Thapar, Ajay K., Agha, Sharifah Shameem, Davey Smith, George, Stergiakouli, Evie, and Thapar, Anita

Subjects
ATTENTION-deficit hyperactivity disorder, RECEIVER operating characteristic curves
Abstract

To investigate the accuracy of the age-at-onset criterion in those who meet other DSM-5 criteria for attention-deficit hyperactivity disorder, using a prospective population cohort we compared four different approaches to asking those aged 25 years (n = 138) when their symptoms started. Receiver operating characteristic curves showed variation between the approaches (χ(3) = 8.99, P = 0.03); all four showed low discrimination against symptoms that had been assessed when they were children (area under the curve: 0.57-0.68). Asking adults to recall specific symptoms may be preferable to recalling at what age symptoms started. However, limitations to retrospective recall add to debate on the validity of ADHD age-at-onset assessment. [ABSTRACT FROM AUTHOR]

Published
2022
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25. General practitioner attitudes to the care of people with epilepsy: an examination of clustering within practices and prediction of patient-rated quality of care

Author

Thapar Ajay K and Roland Martin O

Subjects
Medicine (General), R5-920
Abstract

Abstract Background There is wide variation in the quality of care provided by primary care practices to individuals with chronic illnesses. Individual doctor attitudes and interest have been demonstrated to influence patient outcomes in some instances. Given the trend towards larger practices and part-time working, continuity of care is likely to fall and thus practice-based rather than individual general practitioner attributes and attitudes are likely to become increasingly important. The aim in this paper was to examine the extent to which individual general practitioner (G.P.) attitudes to the care of people with epilepsy cluster within practices and predict patient-rated quality of care. Methods The sample consisted of 1255 people with active epilepsy (a recent seizure or on anti-convulsant medication for epilepsy) and 199 GPs from 82 general practices. Measures of GP attitudes (a 17-item GP attitudes questionnaire) and patient-rated quality of epilepsy care were obtained. 1210 individuals completed initial questionnaires and 975 patients filled in final questionnaires one year later. Responses were achieved from 64 practices (83% of total) and 115 GPs (60% of total). Results 2 main factors were found to underlie GP attitudes to the care of people with epilepsy and these demonstrated clustering within practices "epilepsy viewed as a primary care responsibility" (Eigenvalue 3.98, intra-class correlation coefficient (ICC) 0.40), and "medication skills"(Eigenvalue 2.74, ICC 0.35). GP-rated scores on "epilepsy care being a primary care responsibility" were a significant predictor of patient-rated quality of GP care (p = 0.031). Other contributory factors were seizure frequency (p = 0.044), and patient-rated "shared decision making" (p = 0.022). Conclusion Specific general practitioner attitudes to the care of people with epilepsy cluster within practices and are significantly associated with patient-rated quality of epilepsy care. It is important to take these findings into consideration when planning primary care interventions to ensure people with epilepsy receive the benefits of available medical and surgical expertise.

Published
2005
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26. Childhood neurodevelopmental difficulties and risk of adolescent depression: the role of irritability.

Author

Eyre, Olga, Hughes, Rachael A., Thapar, Ajay K., Leibenluft, Ellen, Stringaris, Argyris, Davey Smith, George, Stergiakouli, Evie, Collishaw, Stephan, and Thapar, Anita

Subjects
MENTAL depression risk factors, AFFECT (Psychology), ATTENTION-deficit hyperactivity disorder, AUTISM, CHILD development deviations, COGNITION, COMMUNICATION, CONFIDENCE intervals, LONGITUDINAL method, MOTOR ability, PATH analysis (Statistics), QUESTIONNAIRES, READING, LOGISTIC regression analysis, ODDS ratio, DISEASE complications, ADOLESCENCE
Abstract

Background: Children with neurodevelopmental disorders are at increased risk of developing depression. Irritability predicts depression in the general population and is common in children with neurodevelopmental disorders. Thus, it is possible that irritability in children with neurodevelopmental disorders contributes to the link with later depression. This study aimed to (a) examine the association between childhood neurodevelopmental difficulties and adolescent depression and (b) test whether irritability explains this association. Methods: Children with any neurodevelopmental difficulty at the age of 7–9 (n = 1,697) and a selected, comparison group without any neurodevelopmental difficulty (n = 3,177) were identified from a prospective, UK population‐based cohort, the Avon Longitudinal Study of Parents and Children. Neurodevelopmental difficulties were defined as a score in the bottom 5% of the sample on at least one measure of cognitive ability, communication, autism spectrum symptoms, attention‐deficit/hyperactivity symptoms, reading or motor coordination. The Development and Well‐Being Assessment measured parent‐reported child irritability at the age of 7, parent‐reported adolescent depression at the age of 10 and 13, and self‐reported depression at the age of 15. Depression measures were combined, deriving an outcome of major depressive disorder (MDD) in adolescence. Logistic regression examined the association between childhood neurodevelopmental difficulties and adolescent MDD, controlling for gender. Path analysis estimated the proportion of this association explained by irritability. Analyses were repeated for individual neurodevelopmental problems. Results: Childhood neurodevelopmental difficulties were associated with adolescent MDD (OR = 2.11, 95% CI = 1.24, 3.60, p = .006). Childhood irritability statistically accounted for 42% of this association. On examining each neurodevelopmental difficulty separately, autistic, communication and ADHD problems were each associated with depression, with irritability explaining 29%–51% of these links. Conclusions: Childhood irritability appears to be a key contributor to the link between childhood neurodevelopmental difficulties and adolescent MDD. High rates of irritability in children with autistic and ADHD difficulties may explain elevated rates of depression in the neurodevelopmental group. [ABSTRACT FROM AUTHOR]

Published
2019
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27. Identifying Novel Types of Irritability Using a Developmental Genetic Approach.

Author

Riglin, Lucy, Eyre, Olga, Thapar, Ajay K., Stringaris, Argyris, Leibenluft, Ellen, Pine, Daniel S., Tilling, Kate, Davey Smith, George, O'Donovan, Michael C., and Thapar, Anita

Subjects
IRRITABILITY (Psychology), MENTAL health services, ATTENTION-deficit hyperactivity disorder, PARENT-child relationships, PSYCHIATRIC diagnosis, THERAPEUTICS
Abstract

Objective: Irritability, which is strongly associated with impairment and negative outcomes, is a common reason for referral to mental health services but is a nosological and treatment challenge. A major issue is how irritability should be conceptualized. The authors used a developmental approach to test the hypothesis that there are several forms of irritability, including a "neurodevelopmental/ADHD-like" type, with onset in childhood, and a "depression/mood" type, with onset in adolescence.Methods: Data were analyzed from the Avon Longitudinal Study of Parents and Children, a prospective U.K. population-based cohort. Irritability trajectory classes were estimated for 7,924 individuals with data at multiple time points across childhood and adolescence (four possible time points from approximately ages 7 to 15). Psychiatric diagnoses were assessed at approximately ages 7 and 15. Psychiatric genetic risk was indexed by polygenic risk scores (PRSs) for attention deficit hyperactivity disorder (ADHD) and depression, derived using large genome-wide association study results.Results: Five irritability trajectory classes were identified: low (81.2%), decreasing (5.6%), increasing (5.5%), late-childhood limited (5.2%), and high-persistent (2.4%). The early-onset high-persistent trajectory was associated with male preponderance, childhood ADHD (odds ratio=108.64, 95% CI=57.45-204.41), and ADHD PRS (odds ratio=1.31, 95% CI=1.09-1.58). The adolescent-onset increasing trajectory was associated with female preponderance, adolescent depression (odds ratio=5.14, 95% CI=2.47-10.73), and depression PRS (odds ratio=1.20, 95% CI=1.05-1.38). Both the early-onset high-persistent and adolescent-onset increasing trajectory classes were associated with adolescent depression diagnosis and ADHD PRS.Conclusions: The developmental context of irritability may be important in its conceptualization: early-onset persistent irritability may be more neurodevelopmental/ADHD-like and later-onset irritability more depression/mood-like. These findings have implications for treatment as well as nosology. [ABSTRACT FROM AUTHOR]

Published
2019
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28. Characterizing Developmental Trajectories and the Role of Neuropsychiatric Genetic Risk Variants in Early-Onset Depression.

Author

Rice, Frances, Riglin, Lucy, Thapar, Ajay K., Heron, Jon, Anney, Richard, O'Donovan, Michael C., and Thapar, Anita

Subjects
MENTAL depression, ATTENTION-deficit hyperactivity disorder, DISEASE risk factors, SCHIZOPHRENIA, GENETICS, AGE of onset, DEPRESSION in adolescence
Abstract

Importance: Depression often first manifests in adolescence. Thereafter, individual trajectories vary substantially, but it is not known what shapes depression trajectories in youth. Adult studies suggest that genetic risk for schizophrenia, a psychiatric disorder with a neurodevelopmental component, may contribute to an earlier onset of depression.Objective: To test the hypothesis that there are distinct trajectories of depressive symptoms and that genetic liability for neurodevelopmental psychiatric disorders (eg, schizophrenia, attention deficit/hyperactivity disorder [ADHD]), as well as for major depressive disorder (MDD), contribute to early-onset depression.Design, Setting, and Participants: The Avon Longitudinal Study of Parents and Children is an ongoing, prospective, longitudinal, population-based cohort that has been collecting data since September 6, 1990, including data on 7543 adolescents with depressive symptoms at multiple time points. The present study was conducted between November 10, 2017, and August 14, 2018.Main Outcomes and Measures: Trajectories based on self-reported depressive symptoms dichotomized by the clinical cutpoint; MDD, schizophrenia, and ADHD polygenic risk score (PRS) were predictors.Results: In 7543 adolescents with depression data on more than 1 assessment point between a mean (SD) age of 10.64 (0.25) years and 18.65 (0.49) years (3568 [47.3%] male; 3975 [52.7%] female), 3 trajectory classes were identified: persistently low (73.7%), later-adolescence onset (17.3%), and early-adolescence onset (9.0%). The later-adolescence-onset class was associated with MDD genetic risk only (MDD PRS: odds ratio [OR], 1.27; 95% CI, 1.09-1.48; P = .003). The early-adolescence-onset class was also associated with MDD genetic risk (MDD PRS: OR, 1.24; 95% CI, 1.06-1.46; P = .007) but additionally with genetic risk for neurodevelopmental disorders (schizophrenia PRS: OR, 1.22; 95% CI, 1.04-1.43; P = .01; ADHD PRS: OR, 1.32; 95% CI, 1.13-1.54; P < .001) and childhood ADHD (χ21 = 6.837; P = .009) and neurodevelopmental traits (pragmatic language difficulties: OR, 1.31; P = .004; social communication difficulties: OR, 0.68; P < .001).Conclusions and Relevance: The findings of this study appear to demonstrate evidence of distinct depressive trajectories, primarily distinguished by age at onset. The more typical depression trajectory with onset of clinically significant symptoms at age 16 years was associated with MDD genetic risk. The less-common depression trajectory, with a very early onset, was particularly associated with ADHD and schizophrenia genetic risk and, phenotypically, with childhood ADHD and neurodevelopmental traits. Findings are consistent with emerging evidence for a neurodevelopmental component in some cases of depression and suggest that the presence of this component may be more likely when the onset of depression is very early. [ABSTRACT FROM AUTHOR]

Published
2019
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29. Developmental Contributions of Schizophrenia Risk Alleles and Childhood Peer Victimization to Early-Onset Mental Health Trajectories.

Author

Riglin, Lucy, Hammerton, Gemma, Heron, Jon, Collishaw, Stephan, Arseneault, Louise, Thapar, Ajay K., Maughan, Barbara, O'Donovan, Michael C., and Thapar, Anita

Subjects
DIAGNOSIS of schizophrenia, AGE factors in disease, COMPARATIVE studies, GENETICS, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, MENTAL health, PSYCHOLOGICAL tests, PSYCHOLOGY, PATHOLOGICAL psychology, RESEARCH, RISK assessment, SCHIZOPHRENIA, PSYCHOLOGY of crime victims, EVALUATION research, CONFOUNDING variables
Abstract

Objective: Twin studies suggest that genetic factors contribute to continuity in mental health problems and that environmental factors are the major contributor to developmental change. The authors investigated the influence of psychiatric risk alleles on early-onset mental health trajectories and whether the trajectories were subsequently modified by exposure to childhood victimization.Methods: The sample was a prospective U.K. population-based cohort, the Avon Longitudinal Study of Parents and Children. The developmental trajectories of emotional problems were estimated in childhood (approximately ages 4-8 years) and adolescence (approximately ages 12-17 years). Psychiatric risk alleles were indexed by polygenic risk scores (PRS) for schizophrenia using genome-wide association study results from the Psychiatric Genomics Consortium. Chronic peer victimization in late childhood (ages 8.5 and 10.5 years) was assessed as an index of environmental exposure. Individuals with sufficient data on emotional problems, the PRS, and victimization were included in the main analyses (N=3,988).Results: Higher schizophrenia PRSs were associated with a trajectory of early-onset increasing emotional problems (odds ratio=1.18, 95% CI=1.02-1.36) compared with a trajectory of low-stable emotional problems. Subsequent exposure to victimization increased the likelihood of transitioning from a trajectory of low-stable emotional problems during childhood (before exposure) to an increasing trajectory in adolescence (after exposure) (odds ratio=2.59, 95% CI=1.48-4.53).Conclusions: While the early development of emotional problems was associated with genetic risk (schizophrenia risk alleles), the subsequent course of emotional problems for those who might otherwise have remained on a more favorable trajectory was altered by exposure to peer victimization, which is a potentially modifiable environmental exposure. [ABSTRACT FROM AUTHOR]

Published
2019
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30. The impact of schizophrenia and mood disorder risk alleles on emotional problems: investigating change from childhood to middle age.

Author

Riglin, Lucy, Collishaw, Stephan, Richards, Alexander, Thapar, Ajay K., Rice, Frances, Maughan, Barbara, O'Donovan, Michael C., and Thapar, Anita

Subjects
AFFECTIVE disorders, AGE distribution, ALLELES, CHILD development, EMOTIONS, GENOMES, LONGITUDINAL method, PSYCHIATRY, REGRESSION analysis, SCHIZOPHRENIA in children, GENOMICS, ODDS ratio, MENTAL illness risk factors
Abstract

Background: Previous studies find that both schizophrenia and mood disorder risk alleles contribute to adult depression and anxiety. Emotional problems (depression or anxiety) begin in childhood and show strong continuities into adult life; this suggests that symptoms are the manifestation of the same underlying liability across different ages. However, other findings suggest that there are developmental differences in the etiology of emotional problems at different ages. To our knowledge, no study has prospectively examined the impact of psychiatric risk alleles on emotional problems at different ages in the same individuals. Methods: Data were analyzed using regression-based analyses in a prospective, population-based UK cohort (the National Child Development Study). Schizophrenia and major depressive disorder (MDD) polygenic risk scores (PRS) were derived from published Psychiatric Genomics Consortium genome-wide association studies. Emotional problems were assessed prospectively at six time points from age 7 to 42 years. Results: Schizophrenia PRS were associated with emotional problems from childhood [age 7, OR 1.09 (1.03–1.15), p = 0.003] to mid-life [age 42, OR 1.10 (1.05–1.17), p < 0.001], while MDD PRS were associated with emotional problems only in adulthood [age 42, OR 1.06 (1.00–1.11), p = 0.034; age 7, OR 1.03 (0.98–1.09), p = 0.228]. Conclusions: Our prospective investigation suggests that early (childhood) emotional problems in the general population share genetic risk with schizophrenia, while later (adult) emotional problems also share genetic risk with MDD. The results suggest that the genetic architecture of depression/anxiety is not static across development. [ABSTRACT FROM AUTHOR]

Published
2018
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31. Brief report: a comparison of child mental health inequalities in three UK population cohorts.

Author

Collishaw, Stephan, Furzer, Emma, Thapar, Ajay K., and Sellers, Ruth

Subjects
COMPETENCY assessment (Law), CHILDREN'S health, CONFIDENCE intervals, INCOME, LONGITUDINAL method, MENTAL health, POVERTY, QUESTIONNAIRES, SURVEYS, ECONOMIC status, HEALTH equity, PARENT attitudes, COLLEGE teacher attitudes
Abstract

There are substantial health disparities between children from low and higher income families. The study aimed to test changes in child mental health inequalities across three large UK population cohorts of 11-year-old children assessed in 1999, 2004 and 2012 as part of the British Child and Adolescent Mental Health Surveys and Millennium Cohort Study. Child mental health was assessed using parent and teacher versions of the Strengths and Difficulties Questionnaire. There were substantial differences in parent and teacher reported symptom scores between children from low and higher income families in each cohort. Differences in parent-reported symptoms increased over time (ES 0.35 [95% CI 0.20, 0.49] in 1999, ES 0.39 [95% CI 0.17, 0.61] in 2004, ES 0.54 [95% CI 0.49, 0.58] in 2012); cohort interaction: p = 0.01). This study found that marked child mental health inequalities exist. The mental health gap between advantaged and disadvantaged children has not reduced over the last 20 years and may be getting worse. [ABSTRACT FROM AUTHOR]

Published
2019
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32. Antecedents of New-Onset Major Depressive Disorder in Children and Adolescents at High Familial Risk.

Author

Rice, Frances, Sellers, Ruth, Hammerton, Gemma, Eyre, Olga, Bevan-Jones, Rhys, Thapar, Ajay K., Collishaw, Stephan, Harold, Gordon T., and Thapar, Anita

Subjects
DEPRESSION in children, DEPRESSION in adolescence, CHILD psychology, MENTAL health, MENTAL health of teenagers, IRRITABILITY (Psychology), PSYCHOSOCIAL factors, DIAGNOSIS of mental depression, POVERTY & psychology, MENTAL depression, DEPRIVATION (Psychology), DISEASE susceptibility, LONGITUDINAL method, CLASSIFICATION of mental disorders, RELATIVE medical risk
Abstract

Importance: Early-onset major depressive disorder (MDD) is common in individuals at high familial risk of depression and is associated with poor long-term mental health, social, and educational outcomes.Objectives: To examine the developmental pathways that lead to first-episode adolescent-onset MDD (incident cases) in those at high familial risk and to postulate a theoretically informed model that enables simultaneous testing of different pathways to incident adolescent-onset MDD composed of contributions from familial/genetic and social risk factors, as well as effects via specific clinical antecedents.Design, Setting, and Participants: This investigation was a 4-year longitudinal study (April 2007 to March 2011) among offspring of depressed parents in the general community. Analyses were conducted between September 1, 2015, and May 27, 2016. Participants were 337 families in whom the index parent (315 mothers and 22 fathers) had experienced at least 2 episodes of MDD (recruited through primary care) and among whom there was a biologically related child in the age range of 9 to 17 years living with the index parent (197 girls and 140 boys with a mean [SD] age of 12.4 [2.0] years) at baseline. Offspring with MDD before the study or at baseline (n = 27), offspring with an episode of MDD that had remitted by follow-up (n = 4), and offspring with missing baseline MDD data (n = 2) were excluded. Ninety-two percent (279 of 304) of families completed the follow-up.Main Outcomes and Measures: The primary outcome was new-onset offspring MDD, and the secondary outcome was the total DSM-IV MDD symptom score.Results: On average, children and adolescents had a mean (SD) of 1.85 (1.74) (range, 0-8.5) DSM-IV symptoms of MDD at follow-up. Twenty (6 males and 14 females) had new-onset MDD, with a mean (SD) age at onset of 14.4 (2.0) years (range, 10-18 years). Irritability (β = 0.12, P = .03) and fear and/or anxiety (β = 0.38, P < .001) were significant independent clinical antecedents of new adolescent-onset MDD, but disruptive behavior (β = -0.08, P = .14) and low mood (β = -0.03, P = .65) were not. The results were similar for the DSM-IV symptom count at follow-up. All the measured familial/genetic and social risk indicators directly influenced risk for new-onset MDD rather than indirectly through acting on dimensional clinical antecedents.Conclusions and Relevance: There are multiple pathways to first-onset adolescent depression in individuals at familial risk. Irritability and fear/anxiety may be additional clinical phenomena to be included as targets in primary preventive interventions focusing on the child. In addition to targeting these phenomena in parents and children, depression prevention methods in high-risk groups may need to take into consideration social risks, such as poverty and psychosocial adversity. [ABSTRACT FROM AUTHOR]

Published
2017
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33. Association of Genetic Risk Variants With Attention-Deficit/Hyperactivity Disorder Trajectories in the General Population.

Author

Riglin, Lucy, Collishaw, Stephan, Thapar, Ajay K., Dalsgaard, Søren, Langley, Kate, Smith, George Davey, Stergiakouli, Evie, Maughan, Barbara, O'Donovan, Michael C., and Thapar, Anita

Subjects
TREATMENT of attention-deficit hyperactivity disorder, NEURODEVELOPMENTAL treatment, MONOGENIC & polygenic inheritance (Genetics), GENOMICS, COMORBIDITY, TRAJECTORY optimization, ATTENTION-deficit hyperactivity disorder, CHILD psychopathology, DISEASE susceptibility, GENETICS, LONGITUDINAL method, PUBLIC health surveillance, RESEARCH funding, CASE-control method
Abstract

Importance: Attention-deficit/hyperactivity disorder (ADHD) is a heritable neurodevelopmental disorder that shows clinical and genetic overlap with other childhood neurodevelopmental disorders. Levels of ADHD symptoms typically decline across childhood and adolescence, although they remain elevated for some individuals. The determinants of symptom persistence and decline are not yet fully understood.Objectives: To test the hypothesis that genetic risk variant load for ADHD (indexed by polygenic risk scores [PRS]), but not for other psychiatric disorders, is associated with population-based ADHD symptom trajectories across childhood and adolescence, and to examine whether higher genetic liability for ADHD is correlated with total number of additional neurodevelopmental disorders (multimorbidity) in childhood.Design, Setting, and Participants: The Avon Longitudinal Study of Parents and Children, an ongoing prospective population-based cohort study, has been collecting data on 14 701 children, including 9757 with data on symptoms of ADHD at multiple time points, since September 6, 1990. The primary exposure variables, PRS, were generated using results of a genome-wide association study from the Psychiatric Genomics Consortium. Childhood multimorbidity scores (ages 7-9 years) were measured by total impairments in 4 domains known to share genetic liability with ADHD: IQ, social communication, pragmatic language, and conduct. Data analysis was conducted from March 1 to September 8, 2016.Main Outcomes and Measures: Attention-deficit/hyperactivity disorder symptom trajectories from ages 4 to 17 years (7 time points).Results: Among 9757 children with data on symptoms of ADHD at multiple time points (age range, 4-17 years; 4968 boys and 4789 girls), 4 ADHD symptom trajectories were identified: low (82.6%), intermediate (7.7%), childhood-limited (5.8%), and persistent (3.9%). Mean (SE) PRS for ADHD were higher in children in the persistent trajectory (0.254 [0.069]) compared with each of the other 3 trajectories (low, -0.018 [0.014], χ21 = 14.67, P < .001, odds ratio, 1.31; intermediate, 0.054 [0.055], χ21 = 4.70, P = .03, odds ratio, 1.22; and childhood-limited, 0.017 [0.060], χ21 = 6.50, P = .01, odds ratio, 1.27). Findings were specific to PRS for ADHD; PRS for other psychiatric conditions did not differ across trajectories. The proportion of children with multimorbidity was also highest in those in the persistent trajectory (42.5%; 95% CI, 33.9%-51.1%; P < .001) and was associated with persistence of ADHD symptoms independent of PRS.Conclusions and Relevance: Persistence of ADHD symptoms across childhood and adolescence in the general population is associated with higher PRS for ADHD. Childhood multimorbidity was also associated with persistence of ADHD symptoms and may help to identify children with ADHD whose symptoms are most likely to continue into adolescence. [ABSTRACT FROM AUTHOR]

Published
2016
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34. Higher cognitive ability buffers stress-related depressive symptoms in adolescent girls.

Author

Riglin, Lucy, Collishaw, Stephan, Shelton, Katherine H., McManus, I. C., Ng-Knight, Terry, Sellers, Ruth, Thapar, Ajay K., Frederickson, Norah, and Rice, Frances

Subjects
COGNITIVE ability, PSYCHOLOGICAL stress, MENTAL depression, SYMPTOMS, PSYCHOLOGY of teenage girls, PSYCHOLOGICAL adaptation, DATA analysis
Abstract

Stress has been shown to have a causal effect on risk for depression. We investigated the role of cognitive ability as a moderator of the effect of stressful life events on depressive symptoms and whether this varied by gender. Data were analyzed in two adolescent data sets: one representative community sample aged 11–12 years (n = 460) and one at increased familial risk of depression aged 9–17 years (n = 335). In both data sets, a three-way interaction was found whereby for girls, but not boys, higher cognitive ability buffered the association between stress and greater depressive symptoms. The interaction was replicated when the outcome was a diagnosis of major depressive disorder. This buffering effect in girls was not attributable to coping efficacy. However, a small proportion of the variance was accounted for by sensitivity to environmental stressors. Results suggest that this moderating effect of cognitive ability in girls is largely attributable to greater available resources for cognitive operations that offer protection against stress-induced reductions in cognitive processing and cognitive control which in turn reduces the likelihood of depressive symptomatology. [ABSTRACT FROM PUBLISHER]

Published
2016
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36. Risk of psychopathology in adolescent offspring of mothers with psychopathology and recurrent depression.

Author

Sellers, Ruth, Collishaw, Stephan, Rice, Frances, Thapar, Ajay K., Potter, Robert, Mars, Becky, Harold, Gordon T., Smith, Daniel J., Owen, Michael J., Craddock, Nick, and Thapar, Anita

Subjects
PATHOLOGICAL psychology, MENTAL illness risk factors, COMORBIDITY, ADOLESCENT psychiatry, CHILD psychiatry, PSYCHIATRIC epidemiology, CHILDREN of people with mental illness, COMPARATIVE studies, MENTAL depression, EPIDEMIOLOGICAL research, RESEARCH methodology, MEDICAL cooperation, MENTAL status examination, PSYCHOLOGY of mothers, PSYCHOLOGICAL tests, RESEARCH, RESEARCH funding, DISEASE relapse, SOCIOECONOMIC factors, EVALUATION research, PSYCHOLOGY
Abstract

Background: Offspring of mothers with depression are at heightened risk of psychiatric disorder. Many mothers with depression have comorbid psychopathology. How these co-occurring problems affect child outcomes has rarely been considered.Aims: To consider whether the overall burden of co-occurring psychopathology in mothers with recurrent depression predicts new-onset psychopathology in offspring.Method: Mothers with recurrent depression and their adolescent offspring (9-17 years at baseline) were assessed in 2007 and on two further occasions up to 2011. Mothers completed questionnaires assessing depression severity, anxiety, alcohol problems and antisocial behaviour. Psychiatric disorder in offspring was assessed using the Child and Adolescent Psychiatric Assessment.Results: The number of co-occurring problems in mothers (0, 1 or 2+) predicted new-onset offspring disorder (odds ratio (OR) = 1.80, 95% CI 1.17-2.77, P = 0.007). Rates varied from 15.7 to 34.8% depending on the number of co-occurring clinical problems. This remained significant after controlling for maternal depression severity (OR = 1.73, 95% CI 1.03-2.89, P = 0.040).Conclusions: The burden of co-occurring psychopathology among mothers with recurrent depression indexes increased risk of future onset of psychiatric disorder for offspring. This knowledge can be used in targeting preventive measures in children at high risk of psychiatric disorder. [ABSTRACT FROM AUTHOR]

Published
2013
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37. Adolescent clinical outcomes for young people with attention-deficit hyperactivity disorder.

Author

Langley, Kate, Fowler, Tom, Ford, Tamsin, Thapar, Ajay K., den Bree, Marianne van, Harold, Gordon, Owen, Michael J., O'Donovan, Michael C., Thapar, Anita, and van den Bree, Marianne

Subjects
ATTENTION-deficit hyperactivity disorder, BEHAVIOR disorders in children, CHILDREN, TEENAGERS, BEHAVIOR disorders
Abstract

Background: Attention-deficit hyperactivity disorder (ADHD) is recognised as a common, disabling condition. Little information is available regarding the long-term outcomes for individuals with ADHD in the UK.Aims: To examine the 5-year outcome for a UK cohort of children with diagnosed, treated ADHD and identify whether maternal and social factors predict key outcomes.Method: One hundred and twenty-six school-aged children (mean age 9.4 years, s.d. = 1.7) diagnosed with ADHD were reassessed 5 years later during adolescence (mean age 14.5 years, s.d. = 1.7) for ADHD, conduct disorder and other antisocial behaviours.Results: Most adolescents (69.8%) continued to meet full criteria for ADHD, were known to specialist services and exhibited high levels of antisocial behaviour, criminal activity and substance use problems. Maternal childhood conduct disorder predicted offspring ADHD continuity; maternal childhood conduct disorder, lower child IQ and social class predicted offspring conduct disorder symptoms.Conclusions: The treatment and monitoring of ADHD need to be intensified as outcomes are poor especially in offspring of mothers with childhood conduct disorder symptoms. [ABSTRACT FROM AUTHOR]

Published
2010
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39. Validation of the short Mood and Feelings Questionnaire in young adulthood.

Author

Eyre, Olga, Bevan Jones, Rhys, Agha, Sharifah Shameem, Wootton, Robyn E, Thapar, Ajay K, Stergiakouli, Evie, Langley, Kate, Collishaw, Stephan, Thapar, Anita, and Riglin, Lucy

Subjects
*YOUNG adults, *DEPRESSION in adolescence, *MENTAL depression, *SENSITIVITY & specificity (Statistics), *QUESTIONNAIRES, *DIAGNOSIS of mental depression, *RESEARCH, *RESEARCH methodology, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *MENTAL health surveys, *RESEARCH funding, *EMOTIONS, *LONGITUDINAL method
Abstract

Background: Depression often onsets in adolescence and is associated with recurrence in adulthood. There is a need to identify and monitor depression symptoms across adolescence and into young adulthood. The short Mood and Feelings Questionnaire (sMFQ) is commonly used to measure depression symptoms in adolescence but has not been validated in young adulthood. This study aimed to (1) examine whether the sMFQ is valid in young adulthood, and (2) identify cut-points best capturing DSM-5 depression diagnosis at age 25 METHODS: The sample included participants in the Avon Longitudinal Study of Parents and Children (ALSPAC) at age 25 (n = 4098). Receiver Operating Characteristic analyses examined how well the self-rated sMFQ discriminates between cases and non-cases of DSM-5 Major Depressive Disorder (MDD) classified using the self-rated Development and Well Being Assessment. Sensitivity and specificity values were used to identify cut-points on the sMFQ RESULTS: The sMFQ had high accuracy for discriminating MDD cases from non-cases at age 25. The commonly used cut-point in adolescence (≥12) performed well at this age, best balancing sensitivity and specificity. However, a lower cut-point (≥10) may be appropriate when favouring sensitivity over specificity e.g., in context of screening. Sensitivity analyses suggested similar results for males and females LIMITATIONS: ALSPAC is a longitudinal population cohort that suffers from non-random attrition CONCLUSIONS: The sMFQ is a valid measure of depression in young adults in the general population. It can be used to screen for and monitor depression across adolescence and early adulthood. [ABSTRACT FROM AUTHOR]

Published
2021
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40. Associations Between Genetic Risk For Psychiatric Disorders and Childhood Neurodevelopment: Investigating Polygenic Risk Scores For Psychiatric Disorders and Traits In General Population Samples.

Author

Riglin, Lucy, Collishaw, Stephan, Thapar, Ajay K., Maughan, Barbara, O'Donovan, Michael C., and Thapar, Anita

Subjects
*22Q11 deletion syndrome, *MENTAL illness, *ATTENTION-deficit hyperactivity disorder, *MENTAL depression, *CHILDREN, *COGNITION disorders, *YOUTH with attention-deficit hyperactivity disorder
Abstract

Most psychiatric disorders are thought to have their origins at least in part in childhood, even if early manifestations of liability are quite different from the later full-blown clinical picture. This work aims to identify traits relevant to risk for psychiatric disorders early in development by investigating which "neurodevelopmental domains" are associated with psychiatric disorder risk alleles during childhood. Findings will be presented testing the hypothesis that psychiatric disorder risk alleles, as measured by polygenic risk scores, affect normative, dimensional childhood characteristics in the general population. Specifically, this work investigates associations between polygenic risk scores for schizophrenia, bipolar disorder, major depressive disorder and Attention Deficit Hyperactivity Disorder and primarily pre-pubertal neurodevelopmental traits using longitudinal general population samples. [ABSTRACT FROM AUTHOR]

Published
2019
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41. SU93THE CONTRIBUTION OF PSYCHIATRIC RISK ALLELES TO A GENERAL LIABILITY TO PSYCHOPATHOLOGY IN EARLY LIFE: INVESTIGATING ONE EXPLANATION FOR PLEIOTROPY.

Author

Riglin, Lucy, Collishaw, Stephan, Thapar, Ajay K., Leppert, Beate, Martin, Joanna, Richards, Alexander, Anney, Richard, Smith, George Davey, Tilling, Kate, Stergiakouli, Evie, O'Donovan, Michael, and Thapar, Anita

Subjects
*22Q11 deletion syndrome, *ALLELES, *AUTISM spectrum disorders, *MENTAL depression
Abstract

Highlights from the article: Su93the contribution of psychiatric risk alleles to a general liability to psychopathology in early life: investigating one explanation for pleiotropy In this study we examine the structure of psychopathology in childhood and early adolescence in a population-based birth cohort, including autistic and ADHD symptoms as well as emotional and behavioral items that have been used in previous studies. PRS were derived from the largest available published genome-wide association studies of schizophrenia, major depressive disorder (MDD), autism spectrum disorder (ASD) and attention-deficit/hyperactivity disorder (ADHD).

Published
2019
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42. SU38EARLY ONSET DEPRESSION: CHARACTERISING DEVELOPMENTAL TRAJECTORIES AND THE ROLE OF NEUROPSYCHIATRIC GENETIC RISK VARIANTS.

Author

Rice, Frances, Riglin, Lucy, Thapar, Ajay K, Heron, Jon, Anney, Richard, O'Donovan, Michael, and Thapar, Anita

Subjects
*ATTENTION-deficit hyperactivity disorder
Abstract

Highlights from the article: Su38early onset depression: characterising developmental trajectories and the role of neuropsychiatric genetic risk variants B Results: b Latent class growth analysis identified three distinct trajectory classes - a persistently low class (73.7%), a late-adolescent-onset class (17.3%), and an early-adolescent-onset class (9.0%). The late-adolescent class, which had features of a "typical" post-pubertal-onset depression trajectory, was associated with an elevated genetic risk for depression as indexed by MDD PRS, but not with liability to neurodevelopmental disorders.

Published
2019
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43. M9 - INVESTIGATING THE IMPACT OF DEPRESSION AND SCHIZOPHRENIA POLYGENIC RISK SCORES ON EMOTIONAL PROBLEMS FROM CHILDHOOD TO MID-LIFE.

Author

Riglin, Lucy, Collishaw, Stephan, Thapar, Ajay K., Maughan, Barbara, O'Donovan, Michael, and Thapar, Anita

Subjects
*ADULT child abuse victims, *SCHIZOPHRENIA, *MENTAL depression, *CHILDREN, *MIDDLE age, *ETIOLOGY of diseases
Abstract

Previous studies find that both schizophrenia and mood disorder risk alleles contribute to adult anxiety and depression. Emotional problems (depression or anxiety) begin in childhood and show strong continuities into adult-life; this suggests that symptoms are the manifestation of the same underlying liability across different ages. However, other findings suggest there are developmental differences in the etiology of emotional problems at different ages. These include (a) differences in treatment responsiveness and gender ratios in child/adolescence compared to adulthood, (b) recent genetic findings that schizophrenia risk alleles were specifically associated with "earlier-onset" (<27 years) rather than "later-onset" depression. To our knowledge, no study has prospectively examined the impact of psychiatric risk alleles on emotional problems at different ages in the same individuals. Data were analyzed using regression-based analyses in two UK, prospective, population-based cohorts (NCDS and ALSPAC). Schizophrenia and Major Depressive Disorder (MDD) Polygenic Risk Scores (PRS), were derived from published Psychiatric Genomics Consortium genome-wide association studies. Emotional problems were assessed prospectively from age 7 to 44 years in NCDS and from age 7 to 18 years in ALSPAC. Schizophrenia PRS were associated with emotional problems from childhood (β=0.044, p=0.005) to mid-life (β=0.033, p=0.023), while MDD PRS were associated with emotional problems only in adulthood (β=0.035, p=0.011; childhood β=0.014, p=0.372). Associations between schizophrenia PRS and early emotional problems appear to be driven by anxiety rather than depression. Our prospective investigations suggests that early (childhood) emotional problems in the general population share more genetic risk with schizophrenia, while later (adult life) emotional problems also shared genetic risk with MDD. This is consistent with findings from cross-sectional clinical studies of MDD. The results suggest that the genetic architecture of depression/anxiety is not static across development. [ABSTRACT FROM AUTHOR]

Published
2019
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