This project aims to provide training to our PHD students in Division of Biostatistics and Health Data Science. Several projects are proposed, with a focus on developing statistical methods, ranging from gene-by-environment interaction, mediation analysis, and methods to appropriately account for family structure. Ultimately, our goal is to use this information to train the next generation of PHD students who study statistical genetics and genomics.

Breast density, the proportion of fibroglandular tissue as detected by mammography or magnetic resonance imaging (MRI), is strongly associated with breast cancer risk. However, the mechanisms through which increased breast density leads to increased cancer risk are not well understood. This project aims to map the contribution of common genetic variation to breast density as detected by MRI in a subset of nulliparous women.

We have discovered that autoantibodies to a C-type lectin MICL promote uncontrolled formation of neutrophil extracellular traps (NETs) that exacerbate autoimmune disease (PMID: 19025564). We have also identified the presence of these autoantibodies in a proportion of our healthy control cohorts and we wish to study this longitudinal cohort to see if the presence of these antibodies early in life predispose to the development of autoimmunity.

ALSPAC did not collect DXA measures of body composition at 7 or 8 years of age but did collect impedance. An equation has previously been derived to estimate body fat from impednace in adults and it has been shown that this also correlates well in chidlren but this has never been written up. We plan to examine associations between body fat estimated from impedance and boda fat estimated using DXA at all timepoints where both are available.

The goal of this project application is to enable a PhD student to use data requested in previous applications.
We and others have identified numerous risk factors that influence mental health in young adults and early adulthood. These include adversity, cannabis use, population density, immigrant status (PMID: 29352556, 31563981), exposure to infections such as COVID (PMID: 35987197), obstetric and delivery complications (PMID: 12091183), and maternal characteristics and behaviours during pregnancy. Evidence for example suggests that offspring of mothers who smoked during pregnancy have an increased risk (38%) of developing schizophrenia (PMID: 27216261). Furthermore, infection during pregnancy is associated with an increased the risk of psychosis in offspring (PMID: 26303935). Additionally, in the ALSPAC cohort, we recently identified that suicidal ideation at age 17 is associated with 7-fold increased odds of psychotic disorder, and with depressive disorder and generalised anxiety disorder at age 24. Indeed, over 40% of those with psychotic disorder in early adulthood had experienced this symptom in late adolescence (Mongan et al, 2022).
We and others have also identified evidence for inflammatory marker dysregulation both preceding and in association with psychiatric disorders including psychosis, depression and recently, long COVID (PMID: 36085284, 35472304). Dysregulation of acute inflammatory markers [such as Interleukin (IL)-6 and C-Reactive Protein] and complement proteins has been reported prior to and in association with these outcomes (PMID: 25133871, PMID: 32857162).

Using ALSPAC data we identified for the first time the cross-sectional association of suPAR (soluble urokinase plasminogen activator receptor- an established marker of chronic inflammation) and IL-6 (an established marker of primarily acute inflammation) with psychotic disorder in young adults (PMID: 37004760). We previously found an inverse association between the anti-inflammatory marker n-3 fatty acid docosahexaenoic acid (DHA) at age 17 and psychotic disorder at age 24 in the ALSPAC cohort (PMID 34059620). Using ALSPAC data, we have also shown for the first time that elevated suPAR is associated cross-sectionally with cannabis exposure, itself a marker for mental ill health (Power et al., 2022 (under review)).
We now seek to expand our knowledge to mental health outcomes in early adulthood (using data collected at age 24 and age 30). We wish to examine cross-sectional and longitudinal associations between early life, childhood and later life risk factors with inflammation in relation to clinical thresholds of psychiatric disorders, as well as in relation to specific symptoms and symptom severity. In light of recent findings, (PMID: 34390805; PMID: 26033244), we are particularly interested in the relationship between adverse childhood events including physical, sexual and emotional abuse, bullying or victimisation, and inflammatory dysregulation in the development of psychiatric disorders. Elevated inflammatory levels (supar) for example have been reported in adolescents that have experienced persistent parent-child separation in childhood (PMID: 34454061).

Additionally, sexual minority groups can experience increased exposure to victimization and discrimination, as well as higher rates of anxiety, depression, suicidal thoughts and antisocial behaviour (PMID: 35572280). Recent evidence suggests the presence of increased inflammatory marker levels in such groups (PMID: 32930919).
Additionally, emerging evidence also suggests that exposure to adversity such as high stress across lifetime (PMID: 26673150) or exposure to sexual abuse (PMID: 29365106) influences epigenetic aging in adulthood. One recent meta-analysis quantified this age acceleration, showing that any exposure to childhood trauma was associated with an epigenetic “outpace” of as much as 6 months (PMID: 29452766).
We hypothesise that exposure to environmental risk factors and early-life adversity is associated with chronic inflammatory dysregulation, in line with recent evidence (PMID: 31682707, 26033244, 34990745). We also hypothesise that inflammatory dysregulation will be more common in those who go on to report mental disorders in adulthood (PMID: 25133871, PMID: 32857162). Crucially, we hypothesise that inflammatory dysregulation mediates the relationship between environmental exposures and adult mental disorders, which could provide evidence for a biological mechanism by which environmental exposures influences the risk of adult mental disorder. Alternatively, environmental exposures and biological risk factors may operate independently, but have a cumulative effect on the risk of mental disorders. We propose to investigate this using a combination of existing ALSPAC data, and new data derived from assays undertaken by us which assessed levels of the robust marker of chronic inflammation, suPAR, in age 24 plasma samples donated by ALSPAC participants.

Additionally, we would like to request data relating to general medical conditions and previous infections as accounting for these factors will be important to avoid potential confounding of our findings. For example, there are reports of associations between childhood infection, in particular viral CNS infections and increased risk for psychosis in adulthood (PMID: 29450471; PMID: 22704639). Regarding suPAR itself, there is also evidence of associations between elevated suPAR levels with the development of cancer, CVD, T2D and mortality in the general and psychiatric populations (PMID: 20561148).

We are interested in investigating the longitudinal associations between biological and environmental risk factors with subsequent mental ill-health at age 24 and age 30 (when available). In order to explain any potential relationships appropriately, we will need to include particular demographic variables (such as ethnicity) as co-varying factors.
Previous research has shown that the incidence of psychotic disorders is elevated in various ethnic groups (PMID: 28642258). Evidence has also indicated an association between ethnicity and inflammation, with Caucasian populations often having lower CRP or IL-6 levels compared to other ethnic groups (PMID: 15205215; PMID: 16123316). Based on such findings, we feel that it is important to determine the extent of the relationship between ethnicity, inflammation and later psychiatric outcomes.
Evidence has also shown that lifestyle factors including low physical activity can contribute to a higher suPAR levels (PMID: 30679937), as well as altered levels of acute inflammatory biomarkers (CRP) in healthy populations (PMID: 12038947). Physical activity was also shown to act as a potential protective mechanism against oxidative stress in first-episode psychosis patients (PMID: 32709912). Based on such findings, we would like to investigate how physical activity might influence the relationship between inflammation (as measured by suPAR, and/or CRP & IL-6) and later psychiatric outcome.

An earlier project, B4168 aims to investigate longitudinal associations between environmental risk factors and subsequent mental ill-health, and then if possible, to investigate whether inflammation mediates the relationship between these environmental risk factors and mental health outcomes. One such risk factor is childhood trauma.
There is some evidence that trauma exposure is associated with elevated inflammatory levels (PMID: 29741788) and with poor mental health outcomes (PMID: 23592532).
We aim to explore if these relationships exist in relation to age 24 chronic inflammatory marker - suPAR - and if inflammation (as measured by suPAR) mediates the relationship between trauma and poor mental health.
Recently, emerging evidence suggests that while trauma might be related to elevated inflammation levels, certain positive experiences in childhood are associated with lower levels of inflammation (PMID: 36420372). Therefore, we feel that in order to fully understand the relationship between trauma exposure, inflammation and later mental health outcomes, we must investigate and account for positive childhood experiences as an important confounder/contributor in the relationship.

No new data is requested - Only data from B4168 will be used.

Pubertal timing refers to the pace at which individuals reach certain stages of puberty relative to their same-age and same-sex peers. The global trend towards earlier pubertal timing is of concern due to its associated adverse health implications including cardiovascular diseases, type Ⅱ diabetes and sex steroid-sensitive cancers(2). In addition, earlier pubertal timing may also lead to increased risky behaviours during adolescence including depression, early sexual activity and substance abuse(2). Therefore, identifying modifiable factors that influence pubertal timing is important to mitigate these adverse outcomes. Studies suggest that passive tobacco smoke exposure is associated with puberty timing, e.g., several birth cohorts have shown that maternal smoking during their third trimester associates with an earlier age of menarche. Life course epidemiology theory may help us understand how passive tobacco smoke exposure relate to pubertal timing. Under this theory, we proposed three life course models to explain the association between passive tobacco smoke exposure and pubertal timing: the critical period model, the risk accumulation model and a compound model of risk accumulation with a sensitive period. The critical period model assumes that exposure during a limited time window has an adverse impact on development, contributing to disease onset in later life, and this impact cannot be modified by subsequent exposures. In contrast, the risk accumulation model posits that as the number and/or duration of exposure increases, there is cumulative damage to biological systems. Additionally, a compound model of risk accumulation with a sensitive period suggests that within the risk accumulation model, there is stronger association between exposure and outcome during a specific developmental period relative to other periods. To our knowledge, no previous study has examined the contribution of passive tobacco smoke exposure during different early life periods (prenatal, infancy and childhood) to pubertal timing.

The @30 clinic which has collected data on the original parents of ALSPAC has some gaps in the vision and hearing data as these measures were not ready to be collected from the start. We would also like to collect cognition data which was not collected in the original clinic (although was funded and originally proposed). These data will be used in a wide variety of studies, focussed on aging in the parent cohort and used as baseline for future funding proposals

The first years of life have a profound impact on later behavioural, emotional and social development. An intriguing and modifiable risk factor for later psychopathology is the early regulation of bodily functions, such as the sleep-wake cycle, self-soothing and food ingestion, which goes awry in about 20% of infants leading to regulatory problems (RPs) with crying, sleeping and/or feeding. About 2-8% of infants and toddlers experience multiple or prolonged RPs. Mounting evidence shows that RPs can have adverse long-term effects on behavioural, emotional and/or social outcomes. The proposed project will investigate the impact of early RPs on mental health outcomes from childhood to adulthood, examining multimodal neurobiological markers as possible underlying mechanisms. We will go beyond the state of-the-art in three ways. Firstly, we will analyse rich phenotypic and neuroimaging data of three population-based studies from three countries (Generation R, ALSPAC and BLS). To enable cross-timepoint and cross-dataset brain surface analysis, we will develop novel robust vertex-wise mixed modelling, meta-analysis and federated mega-analysis tools as part of an existing open-source R package. Secondly, we will examine neurobiological pathways of the RP-mental health association, via brain structure (i.e., cortex morphology) and function (i.e., intrinsic functional connectivity). Thirdly, we will employ the hierarchical dimensional HiTOP framework to characterize adverse outcomes of early RPs with better precision and generalizability. This may result in new findings on neurobiology and effects of RPs on dimensional mental health phenotypes, and crosswalk models for the research community.

Obsessive Compulsive disorder (OCD) is a chronic and debilitating condition characterised by the presence of obsessions (i.e., recurrent, or intrusive thoughts or images) and/or compulsions (repetitive and ritualised behaviours carried out in an attempt to alleviate anxiety) (American Psychiatric Association, 2022). OCD is thought to affect 1-4% of adults in the general population (NICE, 2018). In contrast, psychotic disorders are classified as eight distinct diagnoses in the DSM-5-TR, each featuring a combination of hallucinations, delusions, disorganised speech, abnormal psychomotor behaviour and negative symptoms (American Psychiatric Association, 2022). It is estimated that psychotic disorders have a lifetime prevalence of 3% (Perälä et al, 2007).

OCD, when present in psychotic disorders, has been linked to complications in treatment of either condition (Cederlof et al, 2015). Additionally, this comorbidity is associated with increased symptom severity, decreased quality of life, more depressive symptoms and higher rates of suicidaility and overall poorer prognosis (Cunill et al., 2008; Lieuwe de Haan et al., 2012; Niendam et al, 2009; Sharma & Reddy, 2019). Some research has explored the cross-sectional relationship between OCD and psychosis. One study conducted in Sweden found that individuals diagnosed with OCD were 12 times likelier to have a diagnosis of psychosis (Cederlof et al, 2015). Similarly, within a population of individuals diagnosed with psychosis, 25% also presented with obsessive compulsive symptoms (OCS) and 15% met diagnostic criteria for OCD (Scotti-Muzzi & Saide, 2017). Whilst current literature documents cross-sectional links between the two disorders, there is a dearth of literature exploring whether OCD is prospectively associated with psychosis, or whether psychosis is prospectively associated with OCD. Additionally, whether this association is true for OCS and psychotic-like experiences. There is also very little known about the mechanisms which may explain this association. One research study found significant associations between the presence of delusions and obsessions as well as auditory hallucinations and compulsions, suggesting that they could share common mechanisms (Guillem et al, 2009). Through developing a better understanding of the association between OCD/OCS and psychosis/ psychotic experiences at a symptom level, psychological interventions may be adapted or developed for individuals who present with both.

This project proposes to re-use the dataset B2172 in order to explore the research question, whilst also requesting additional variables (please see exposures, outcomes and confounders for a list of the data to re-use request and new variables to request).

References:

American Psychiatric Association. (2022) Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition, Text Revision, DSM-5-TR. American Psychiatric Association

Cederlöf, M., Lichtenstein, P., Larsson, H., Boman, M., Rück, C., Mikael Landén, & Mataix-Cols, D. (2014). Obsessive-Compulsive Disorder, Psychosis, and Bipolarity: A Longitudinal Cohort and Multigenerational Family Study. Schizophrenia Bulletin, 41(5), 1076–1083. https://doi.org/10.1093/schbul/sbu169

Cunill, R., Castells, X., & Simeon, D. (2008). Relationships Between Obsessive-Compulsive Symptomatology and Severity of Psychosis in Schizophrenia. The Journal of Clinical Psychiatry, 70(1), 70–82. https://doi.org/10.4088/jcp.07r03618

Guillem, F., Satterthwaite, J., Pampoulova, T., & Stip, E. (2009). Relationship between psychotic and obsessive compulsive symptoms in schizophrenia. Schizophrenia Research, 115(2-3), 358–362. https://doi.org/10.1016/j.schres.2009.06.004

Lieuwe de Haan, Sterk, B., & Renate. (2012). Presence of obsessive compulsive symptoms in first‐episode schizophrenia or related disorders is associated with subjective well‐being and quality of life. Early Intervention in Psychiatry, 7(3), 285–290. https://doi.org/10.1111/j.1751-7893.2012.00377.x

NICE. (2018) Obsessive-compulsive disorder: How common is it?

Niendam, T. A., Berzak, J., Cannon, T. D., & Bearden, C. E. (2009). Obsessive compulsive symptoms in the psychosis prodrome: Correlates of clinical and functional outcome. Schizophrenia Research, 108(1-3), 170–175. https://doi.org/10.1016/j.schres.2008.11.023

Perälä, J., Jaana Suvisaari, Saarni, S. I., Kimmo Kuoppasalmi, Erkki Isometsä, Pirkola, S., Timo Partonen, Annamari Tuulio-Henriksson, Jukka Hintikka, Tuula Kieseppä, Tommi Härkänen, Koskinen, S., & Jouko Lönnqvist. (2007). Lifetime Prevalence of Psychotic and Bipolar I Disorders in a General Population. Archives of General Psychiatry, 64(1), 19–19. https://doi.org/10.1001/archpsyc.64.1.19

Scotti-Muzzi, E., & Saide. O. L, (2016). Schizo-obsessive spectrum disorders: an update. CNS Spectrums, 22(3), 258–272. https://doi.org/10.1017/s1092852916000390

Sharma, L. P., & Reddy, J. (2019). Obsessive–compulsive disorder comorbid with schizophrenia and bipolar disorder. Indian Journal of Psychiatry, 61(7), 140–140. https://doi.org/10.4103/psychiatry.indianjpsychiatry_527_18