Non-clinical individuals with subsyndromal hypomanic experiences have been shown to be at a heightened risk for developing BD and have been linked to similar severity and impairment experienced by people with BD. A better understanding of the characterisation of hypomania in young people may help improve accurate and timely diagnosis of BD. Despite its potential importance, limited research is available concerning the structure of hypomania among non-clinical young people, particularly in the UK. Therefore, the current study will explore the structure and characterisation of hypomania in a British nonclinical cohort. We propose to examine the distribution and underlying structure of components of hypomania in ALSPAC, along with measure of different psychological and psychopathological dimensions and investigate hypomania symptoms’ association with other psychopathological variables (e.g., substance abuse). Using confirmatory factor analysis and latent class analysis, this study may help explore the structure and characterisation of hypomania in young people. Better understanding of hypomania could provide opportunities for targeted intervention and prevention.

The central idea of the proposed research is to use metabolic biomarkers to predict the severity of COVID-19 and the likelihood of long COVID for individuals that have not necessarily been diagnosed with a pre-existing health condition. To this end, we will use pre-pandemic data from several cohort studies which, in addition to basic information on age, sex, ethnicity, etc, contain hundreds of metabolic biomarkers for thousands of individuals. To understand the link between these characteristics and the impact of COVID-19, we will use symptoms data for those individuals in the cohort studies that had COVID-19. The data will be analysed with statistical methods to identify associations between the characteristics of individuals before the pandemic and the severity of the disease. This analysis will be complemented with computer programs developed to predict if the infection of an individual will have serious effects based on his/her characteristics before the pandemic. Machine learning techniques will be used to train computer programs to automatically recognise metabolic features that represent a risk for severe COVID-19.

Anxiety and depression are common mental health conditions, and represent a major cause of distress and disability in young people. We do not yet understand a) which factors predict vulnerability in young people, b) what predicts who seeks treatment, or c) what characterises young people who respond to treatments compared to those who do not. We need to understand risk factors to allow us to target preventative efforts more effectively. Furthermore, understanding what determines who seeks treatment might allow greater outreach and support to be given to underserved populations, and understanding the factors determining treatment response may allow future research into novel treatments to be targeted, and greater clinical monitoring of those at risk of non-response. Performing this research in young people specifically is important: not only are young people at a critical point in life where they are forming relationships and making decisions about education and careers, but successful treatment access and response might also determine their future mental health. We propose to analyse data from the ALSPAC study, among others, to understand the factors affecting all these parts of young people’s mental health pathways. We also aim to produce an online, interactive, browser-based application that a) researchers, educators, clinicians and policy-makers can use to understand who to target prevention efforts towards, and b) so that young people and their families can have access to the same knowledge as those involved in treating them.

AvonCAP is an ongoing surveillance study, which aims to record detailed information on every adult patient admitted to Bristol’s two large NHS Trusts with symptoms, signs and/or X-ray evidence of acute disease in the lungs. This includes patients with pneumonia, non-pneumonic respiratory infection, exacerbation of chronic respiratory disease (eg asthma, COPD, pulmonary fibrosis) and heart failure. Additionally, we include patients hospitalised with a positive SARS-CoV-2 test. The study is designed to provide comprehensive surveillance of all adults hospitalised with acute respiratory disease in a defined geographic area, thereby providing an accurate estimate of disease incidence. AvonCAP further aims to investigate how lung diseases may be changing during the COVID-19 pandemic, particularly those which may be preventable in the future by new vaccines. This will enable better implementation and design of public health measures, and may be used to determine national vaccination implementation policy.

Health related data is collected for study eligible adults hospitalised at NBT or UHBW NHS Trust, either via consent or under COPI regulations (the study holds CAG approval to use non-consented data). Some study patients also give their consent to provide samples e.g. saliva, nasopharyngeal swabs, etc.

This proposal will identify patients who are in both the AvonCAP and ALSPAC datasets, and allow sharing of specified data fields between the two studies for these patients. Due to the age range of AvonCAP participants, this is likely to include the parents of the Children of The 90s.

Only relevant ALSPAC data fields will be shared with the AvonCAP study team, and will include potential risk factors for lung disease (e.g. occupation and environment factors, pets), details of GP visits and COVID-19 test results. The AvonCAP study will in turn provide data fields of interest to the ALSPAC project.

This proposal allows data collected on participants in these two studies to have added value and greater contribution to the scientific aims of each project.

Adverse childhood experiences (ACEs), such as abuse, threaten individuals’ life-long
well-being. A growing body of research has supported ACEs’ negative influence on long-term
mental health; however, many existing studies measured ACEs by retrospective self-report, that
is, by adults recalling their childhood experiences. However, there is a need to study
prospectively followed cohorts in order to minimise biases in participant selection and
measurement of ACEs. Examining the impact of ACEs on symptom outcomes conceptualised as
stages could help improve our understanding of the staging model in psychiatry. Therefore, this project proposes to explore the prospective impact of ACEs on the progressive stages of mental disorders in adulthood,

Parental depression is associated with various mental health conditions and other difficulties in offspring. Nevertheless, some individuals do not develop mental health difficulties or do so only temporarily. It indicates that certain protective factors may buffer risks associated with being raised by a depressed parent. Individual, family, social, and lifestyle protective factors were identified in previous research to be relevant for mental health resilience in adolescence. However, as people mature, different protective factors may be relevant in young adulthood - a peak period for the emergence of mental health problems.

Therefore, this study will aim to understand if various protective factors could explain why some individuals do not develop mental health problems or recover from them despite being at higher risk due to genetic and environmental influences. Furthermore, we will aim to test the causal role of the identified protective factors and potential biological, psychosocial and environmental mechanisms that could explain protective factors’ joint contribution to mental health resilience in children of depressed parents.

We expect to identify modifiable protective factors that could be targeted to develop prevention and intervention strategies that could potentially interrupt the transmission of mental health problems from parents to offspring. In this way, the research could improve the lives of both depressed parents and their offspring.

Recent empirical work suggests the prevalence of eating disorders may be raised in autistic individuals, however, questions remain as to whether the co-occurrence of autism and eating disorders could be due to selective samples and/or difficulties disentangling symptoms of autism as compared to symptoms of eating disorders. An alternative explanation is that autism, or high levels of autistic traits, in childhood, may causally increases risk for eating disorders later in development. In addition, autistic children often experience high level of anxiety, and might use overeating or binge eaitng as a coping strategy to sooth and calm themselves down, which might put them on increased risk for later eating disorders. Further research into the pathways and potential mediators of the link between autism, anxiety,and eating disorders is needed to illuminate underpinning mechanisms, which in turn will highlight targets for prevention/intervention.

Individuals who are raised in urban (versus rural) settings are around twice as likely to develop a psychotic disorder such as schizophrenia. Research also suggests that risk for other mental health problems, in particular depression, anxiety and conduct problems, is elevated in urban settings. Given that 70% of the world’s population will live in urban areas by 2050, it is essential that we uncover the pathways linking cities and psychosis so that we can inform intervention efforts.
Air and noise pollution are among the biggest environmental health risks that the world faces, and are particularly problematic in cities. Growing evidence also suggests that air pollution may contribute to the development of mental health problems. However, it is currently unknown whether air and noise pollution might partly explain the elevated risk for mental health problems found in cities. In addition, there has been a lack of longitudinal research, including that using pollution spanning the early years of development. Studies have also often been inadequately controlled for potential confounders.
This project will examine 1) the longitudinal associations of air pollution exposure from pregnancy to age 15 with psychotic experiences at age 12, 18, and 24; and examine specificity by repeating analyses with anxiety, depression, and conduct problems as outcomes; 2) explore the interplay between neighbourhood social characteristics (crime and social fragmentation) and air pollution in the emergence of psychotic experiences, and 3) examine two potential biopsychological mechanisms linking urban neighbourhood exposures with mental health, namely inflammation and cognition.

Emerging evidence suggests that babies born by C-section (Cesarean section) have different hormonal, physical, bacterial, and medical exposures, and that these exposures can subtly alter neonatal physiology. (Sandall et la, 2018) C-section delivery has been associated with a number of chronic disease outcomes in children, including metabolic risk phenotypes and asthma. One of the potential mechanisms through which C-section delivery may increase risk of adverse health outcomes is via epigenetic alterations. (Dahlen et al, 2013)

Dahlen, HG et al. “The EPIIC hypothesis: intrapartum effects on the neonatal epigenome and consequent health outcomes.” Med Hypotheses. 2013. May; 80(5):656-62.

Sandall, J et al. “Short-term and long-term effects of caesarean section on the health of women and children.” Lancet. 2018. Oct 13; 392(10155):1349-1357.