Your search keyword '"Alex S.F. Kwong"' showing total 11 results

1. The role of brain structure in the association between pubertal timing and depression risk in an early adolescent sample (the ABCD Study®): A registered report

Author

Niamh MacSweeney, Judith Allardyce, Amelia Edmondson-Stait, Xueyi Shen, Hannah Casey, Stella W.Y. Chan, Breda Cullen, Rebecca M. Reynolds, Sophia Frangou, Alex S.F. Kwong, Stephen M. Lawrie, Liana Romaniuk, and Heather C. Whalley

Subjects

Pubertal timing, Adolescent depression, Brain structure, ABCD Study, Neurophysiology and neuropsychology, QP351-495

Abstract

Background: Earlier pubertal timing is associated with higher rates of depressive disorders in adolescence. Neuroimaging studies report brain structural associations with both pubertal timing and depression. However, whether brain structure mediates the relationship between pubertal timing and depression remains unclear. Methods: The current registered report examined associations between pubertal timing (indexed via perceived pubertal development), brain structure (cortical and subcortical metrics, and white matter microstructure) and depressive symptoms in a large sample (N = ∼5000) of adolescents (aged 9–13 years) from the Adolescent Brain Cognitive Development (ABCD) Study. We used three waves of follow-up data when the youth were aged 10–11 years, 11–12 years, and 12–13 years, respectively. We used generalised linear-mixed models (H1) and structural equation modelling (H2 & H3) to test our hypotheses. Hypotheses: We hypothesised that earlier pubertal timing at Year 1 would be associated with increased depressive symptoms at Year 3 (H1), and that this relationship would be mediated by global (H2a-b) and regional (H3a-g) brain structural measures at Year 2. Global measures included reduced cortical volume, thickness, surface area and sulcal depth. Regional measures included reduced cortical thickness and volume in temporal and fronto-parietal areas, increased cortical volume in the ventral diencephalon, increased sulcal depth in the pars orbitalis, and reduced fractional anisotropy in the cortico-striatal tract and corpus callosum. These regions of interest were informed by our pilot analyses using baseline ABCD data when the youth were aged 9–10 years. Results: Earlier pubertal timing was associated with increased depressive symptoms two years later. The magnitude of effect was stronger in female youth and the association remained significant when controlling for parental depression, family income, and BMI in females but not in male youth. Our hypothesised brain structural measures did not however mediate the association between earlier pubertal timing and later depressive symptoms. Conclusion: The present results demonstrate that youth, particularly females, who begin puberty ahead of their peers are at an increased risk for adolescent-onset depression. Future work should explore additional biological and socio-environmental factors that may affect this association so that we can identify targets for intervention to help these at-risk youth.

Published

2023

2. Early-life inflammatory markers and subsequent psychotic and depressive episodes between 10 to 28 years of age

Author

Amelia J. Edmondson-Stait, Xueyi Shen, Mark J. Adams, Miruna C. Barbu, Hannah J. Jones, Veronique E. Miron, Judith Allardyce, James P. Boardman, Stephen M. Lawrie, Andrew M. McIntosh, Golam M. Khandaker, Alex S.F. Kwong, and Heather C. Whalley

Subjects

Inflammation, Depression, Psychotic experiences, ALSPAC, Life course, Omics, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Inflammation is implicated in depression and psychosis, including association of childhood inflammatory markers on the subsequent risk of developing symptoms. However, it is unknown whether early-life inflammatory markers are associated with the number of depressive and psychotic symptoms from childhood to adulthood. Using the prospective Avon Longitudinal Study of Children and Parents birth cohort (N = up-to 6401), we have examined longitudinal associations of early-life inflammation [exposures: interleukin-6 (IL-6), C-reactive protein (CRP) levels at age 9y; IL-6 and CRP DNA-methylation (DNAm) scores at birth and age 7y; and IL-6 and CRP polygenic risk scores (PRSs)] with the number of depressive episodes and psychotic experiences (PEs) between ages 10–28 years. Psychiatric outcomes were assessed using the Short Mood and Feelings Questionnaire and Psychotic Like Symptoms Questionnaires, respectively. Exposure-outcome associations were tested using negative binomial models, which were adjusted for metabolic and sociodemographic factors. Serum IL-6 levels at age 9y were associated with the total number of depressive episodes between 10 and 28y in the base model (n = 4835; β = 0.066; 95%CI:0.020–0.113; pFDR = 0.041) which was weaker when adjusting for metabolic and sociodemographic factors. Weak associations were observed between inflammatory markers (serum IL-6 and CRP DNAm scores) and total number of PEs. Other inflammatory markers were not associated with depression or PEs. Early-life inflammatory markers are associated with the burden of depressive episodes and of PEs subsequently from childhood to adulthood. These findings support a potential role of early-life inflammation in the aetiology of depression and psychosis and highlight inflammation as a potential target for treatment and prevention.

Published

2022

3. Maternal postnatal depression and offspring depression at age 24 years in a UK-birth cohort: the mediating role of maternal nurturing behaviours concerning feeding, crying and sleeping [version 2; peer review: 2 approved]

Author

Gemma Hammerton, Iryna Culpin, Jonathan Evans, Marc H. Bornstein, Hannah M. Sallis, Tim Cadman, Alex S.F. Kwong, Alan Stein, Rebecca M. Pearson, Jon Heron, and Kate Tilling

Subjects

ALSPAC, maternal postnatal depression, offspring depression, maternal early nurturing parenting behaviours, population-based study., eng, Medicine, Science

Abstract

Background: Maternal postnatal depression (PND) is a risk factor for offspring depression in adulthood. However, few longitudinal studies have examined the role of maternal nurturing parenting behaviours in the association between maternal PND and offspring depression in adulthood. Methods: We examined pathways from maternal PND measured using self-reported Edinburgh Postnatal Depression Scale at 8 weeks to offspring ICD-10 depression diagnosed using the Clinical Interview Schedule-Revised computerised assessment at 24 years through maternal-reported nurturing behaviours concerning feeding, sleeping and crying measured from pregnancy to age 3 years 6 months in 5,881 members of the UK-based birth cohort study, the Avon Longitudinal Study of Parents and Children. Results: The fully adjusted model revealed an indirect effect from PND to adult offspring depression through the combination of all parenting factors (probit regression coefficient [B]=0.038, 95% confidence interval [CI] 0.005, 0.071); however, there was no evidence of a direct effect from early maternal PND to offspring depression once the indirect effect via parenting factors was accounted for (B=0.009, 95%CI -0.075, 0.093). Specificity analyses revealed indirect effects through maternal worries about feeding (B=0.019, 95%CI 0.003, 0.035, p=0.010) and maternal perceptions and responses to crying (B=0.018, 95%CI 0.004, 0.032, p=0.012). Conclusions: The adverse impact of maternal PND on offspring depression in early adulthood was explained by maternal nurturing behaviours concerning feeding, crying and sleeping in early childhood. Residual confounding and measurement error likely limit reliable conclusions. If found causal, interventions providing support to reduce worries around maternal nurturing behaviours and treating depression could reduce adverse outcomes in adult offspring of depressed mothers.

Published

2022

4. Complex trait methylation scores in the prediction of major depressive disorder

Author

Miruna C. Barbu, Carmen Amador, Alex S.F. Kwong, Xueyi Shen, Mark J. Adams, David M. Howard, Rosie M. Walker, Stewart W. Morris, Josine L. Min, Chunyu Liu, Jenny van Dongen, Mohsen Ghanbari, Caroline Relton, David J. Porteous, Archie Campbell, Kathryn L. Evans, Heather C. Whalley, and Andrew M. McIntosh

Subjects

DNA methylation, Methylation score, Environmental factors, Major depressive disorder, Generation Scotland, Avon longitudinal study of parents and children, Medicine, Medicine (General), R5-920

Abstract

Summary: Background: DNA methylation (DNAm) is associated with time-varying environmental factors that contribute to major depressive disorder (MDD) risk. We sought to test whether DNAm signatures of lifestyle and biochemical factors were associated with MDD to reveal dynamic biomarkers of MDD risk that may be amenable to lifestyle interventions. Methods: Here, we calculated methylation scores (MS) at multiple p-value thresholds for lifestyle (BMI, smoking, alcohol consumption, and educational attainment) and biochemical (high-density lipoprotein (HDL) and total cholesterol) factors in Generation Scotland (GS) (N=9,502) and in a replication cohort (ALSPACadults, N=565), using CpG sites reported in previous well-powered methylome-wide association studies. We also compared their predictive accuracy for MDD to a MDD MS in an independent GS sub-sample (N=4,432). Findings: Each trait MS was significantly associated with its corresponding phenotype in GS (βrange=0.089–1.457) and in ALSPAC (βrange=0.078–2.533). Each MS was also significantly associated with MDD before and after adjustment for its corresponding phenotype in GS (βrange=0.053–0.145). After accounting for relevant lifestyle factors, MS for educational attainment (β=0.094) and alcohol consumption (MSp-value

Published

2022

5. COVID-19 perceived impacts on sleep, fitness, and diet and associations with mental health during pregnancy: A cross-national study

Author

Karmel W. Choi, Hannah H. Kim, Archana Basu, Alex S.F. Kwong, Sonia Hernandez-Diaz, Diego F. Wyszynski, and Karestan C. Koenen

Subjects

Mental healing, RZ400-408

Published

2022

6. Mental-health before and during the COVID-19 pandemic in adults with neurodevelopmental disorders

Author

Amy Shakeshaft, Rachel Blakey, Alex S.F. Kwong, Lucy Riglin, George Davey Smith, Evie Stergiakouli, Kate Tilling, and Anita Thapar

Subjects

Psychiatry and Mental health, Biological Psychiatry

Abstract

The COVID-19 pandemic negatively impacted mental health globally. Individuals with neurodevelopmental disorders (NDDs), including autism spectrum disorder (ASD) and attention deficit hyperactivity disorder (ADHD), are at elevated risk of mental health difficulties. Therefore, we investigated the impact of the pandemic on anxiety, depression and mental wellbeing in adults with NDDs using longitudinal data from the Avon Longitudinal Study of Parents and Children study (n=3,058). Mental health data were collected pre-pandemic (age 21-25) and at three timepoints during the pandemic (ages 27-28) using the Short Mood and Feelings Questionnaire, Generalised Anxiety Disorder Assessment-7, and Warwick Edinburgh Mental Wellbeing Scale. ADHD and ASD were defined using validated cut-points of the Strengths and Difficulties Questionnaire and Autism Spectrum Quotient, self-reported at age 25. We used multi-level mixed-effects models to investigate changes in mental health in those with ADHD and ASD compared to those without. Prevalences of depression, anxiety and poor mental wellbeing were higher at all timepoints (pre-pandemic and during pandemic) in those with ADHD and ASD compared to those without. Anxiety increased to a greater extent in those with ADHD (β=0.8 [0.2,1.4], p=0.01) and ASD (β=1.2 [-0.1,2.5], p=0.07), while depression symptoms decreased, particularly in females with ASD (β=-3.1 [-4.6,-1.5], p=0.0001). On average, mental wellbeing decreased in all, but to a lesser extent in those with ADHD (β=1.3 [0.2,2.5], p=0.03) and females with ASD (β=3.0 [0.2,5.9], p=0.04). To conclude, anxiety disproportionately increased in adults with NDDs during the pandemic, however, the related lockdowns may have provided a protective environment for depressive symptoms in the same individuals.

Published

2023

7. Keeping up with the kids: the value of co-production in the study of irritability in youth depression and its underlying neural circuitry

Author

Niamh MacSweeney, Perrine Louvet, Simal Zafar, Stella Chan, Alex S.F. Kwong, Stehpen Lawrie, Liana Romaniuk, and Heather C Whalley

Abstract

Irritability is a core symptom of adolescent depression, characterised by an increased proneness to anger or frustration. Irritability in youth is associated with future mental health problems and impaired social functioning, suggesting that it may be an early indicator of emotion regulation difficulties. Adolescence is a period during which behaviour is significantly impacted by one’s environment. However, existing research on the neural basis of irritability typically use experimental paradigms that overlook the social context in which irritability occurs. Here, we bring together current findings on irritability in adolescent depression and the associated neurobiology and highlight directions for future research. Specifically, we emphasise the importance of co-produced research with young people as a means to improve the construct and ecological validity of research within the field. Ensuring that our research design and methodology accurately reflect to lives of young people today lays a strong foundation upon which to better understand adolescent depression and identify tractable targets for intervention.

Published

2023

8. Father absence and trajectories of offspring mental health across adolescence and young adulthood: Findings from a UK-birth cohort

Author

Iryna Culpin, Hein Heuvelman, Dheeraj Rai, Rebecca M. Pearson, Carol Joinson, Jon Heron, Jonathan Evans, and Alex S.F. Kwong

Subjects

Adult, Male, Adolescent, Depression, United Kingdom, Psychiatry and Mental health, Clinical Psychology, Fathers, Young Adult, Mental Health, Child, Preschool, Humans, Birth Cohort, Longitudinal Studies, Child

Abstract

BackgroundHigh prevalence of parental separation and resulting biological father absence raises important questions regarding its impact on offspring mental health across the life course. We specifically examined whether these relationships vary by sex and the timing of exposure to father absence (early or middle childhood).MethodsThis study is based on up to 8409 children from the Avon Longitudinal Study of Parents and Children (ALSPAC). Participants provided self-reports of depression (Clinical Interview Schedule-Revised) at age 24 years and depressive symptoms (Short Mood and Feelings Questionnaire) between the ages of 10 and 24 years. Biological father absence in childhood was assessed through maternal questionnaires at regular intervals from birth to 10 years. We estimated the association between biological father absence and trajectories of depressive symptoms using multilevel growth-curve modelling.ResultsEarly but not middle childhood father absence was strongly associated with increased odds of offspring depression and greater depressive symptoms at age 24 years. Early childhood father absence was associated with higher trajectories of depressive symptoms during adolescence and early adulthood compared with father presence. Differences in the level of depressive symptoms between middle childhood father absent and father present groups narrowed into adulthood.LimitationsThis study could be biased by attrition and residual confounding.ConclusionsWe found evidence that father absence in childhood is persistently associated with offspring depression in adolescence and early adulthood. This relationship varies by sex and timing of father's departure, with early childhood father absence emerging as the strongest risk factor for adverse offspring mental health trajectories Further research is needed to identify mechanisms that could inform preventative interventions to reduce the risk of depression in children who experience father absence.

Published

2022

9. T48. DIRECT AND INDIRECT GENETIC EFFECTS IN THE ASSOCIATION BETWEEN PARENT AND CHILD MENTAL HEALTH: A GENETICALLY INFORMED APPROACH IN 7 INTERNATIONAL TRIO COHORTS

Author

Hannah Sallis, Melisa Chuong, Katri Kantojärvi, Lea Sirignano, Robyn Wootton, Hannah J. Jones, Ilaria Costantini, Josef Frank, Fabian Streit, Stephanie Witt, Lea Zillich, Alex S.F. Kwong, Mark Adams, Andrew McIntosh, and Rebecca Pearson

Subjects

Pharmacology, Psychiatry and Mental health, Neurology, Pharmacology (medical), Neurology (clinical), Biological Psychiatry

Published

2022

10. T79. ASSOCIATIONS BETWEEN MARKERS OF INFLAMMATION AND LATER EPISODES OF DEPRESSION AND PSYCHOTIC LIKE EXPERIENCES FROM 10 TO 28 YEARS OLD

Author

Amelia Edmondson-Stait, Xueyi Shen, Mark J. Adams, Miruna C. Barbu, Hannah J. Jones, Veronique E. Miron, Judith Allardyce, Stephen M. Lawrie, Golam M. Khandaker, Andrew M. McIntosh, Alex S.F. Kwong, and Heather C. Whalley

Subjects

Pharmacology, Psychiatry and Mental health, Neurology, Pharmacology (medical), Neurology (clinical), Biological Psychiatry

Published

2022

11. Gene–environment correlations and causal effects of childhood maltreatment on physical and mental health

Author

Varun Warrier, Alex S.F. Kwong, M. (Mannan) Luo, Shareefa Dalvie, Jazz Croft, Hannah M. Sallis, Jessie Baldwin, Marcus R. Munafò, Caroline M. Nievergelt, Andrew J. Grant, Stephen Burgess, Tyler M. Moore, Ran Barzilay, Andrew McIntosh, Marinus H. van IJzendoorn, C.A.M. (Charlotte) Cecil, Varun Warrier, Alex S.F. Kwong, M. (Mannan) Luo, Shareefa Dalvie, Jazz Croft, Hannah M. Sallis, Jessie Baldwin, Marcus R. Munafò, Caroline M. Nievergelt, Andrew J. Grant, Stephen Burgess, Tyler M. Moore, Ran Barzilay, Andrew McIntosh, Marinus H. van IJzendoorn, and C.A.M. (Charlotte) Cecil

Abstract

Background: Childhood maltreatment is associated with poor mental and physical health. However, the mechanisms of gene–environment correlations and the potential causal effects of childhood maltreatment on health are unknown. Using genetics, we aimed to delineate the sources of gene–environment correlation for childhood maltreatment and the causal relationship between childhood maltreatment and health. Methods: We did a genome-wide association study meta-analysis of childhood maltreatment using data from the UK Biobank (n=143 473), Psychiatric Genomics Consortium (n=26 290), Avon Longitudinal Study of Parents and Children (n=8346), Adolescent Brain Cognitive Development Study (n=5400), and Generation R (n=1905). We included individuals who had phenotypic and genetic data available. We investigated single nucleotide polymorphism heritability and genetic correlations among different subtypes, operationalisations, and reports of childhood maltreatment. Family-based and population-based polygenic score analyses were done to elucidate gene–environment correlation mechanisms. We used genetic correlation and Mendelian randomisation analyses to identify shared genetics and test causal relationships between childhood maltreatment and mental and physical health conditions. Findings: Our meta-analysis of genome-wide association studies (N=185 414) identified 14 independent loci associated with childhood maltreatment (13 novel). We identified high genetic overlap (genetic correlations 0·24–1·00) among different maltreatment operationalisations, subtypes, and reporting methods. Within-family analyses provided some support for active and reactive gene–environment correlation but did not show the absence of passive gene–environment correlation. Robust Mendelian randomisation suggested a potential causal role of childhood maltreatment in depression (unidirectional), as well as both schizophrenia and ADHD (bidirectional), but not in physical health conditions (coronary artery dis

Published

2021