Eating behaviours describe how people eat rather than what they eat. We believe that some current, common eating behaviours are part of the problem causing an increase in obesity levels in the UK and elsewhere. We put some questions in to the ALSPAC questionnaire for participants aged 25 years that asked about how fast they ate their meals, with whom and in front of what items if any of technology (such as computers, TV etc.). We will examine this information to see if any such behaviours tend towards increased body mass index in the cohort. This information may add to our clinical advice when counselling people with excess weight how to lose or maintain weight loss.

Gastrointestinal infections are common, with 1 in 4 people in the UK population experiencing an episode each year, which causes an estimated annual cost to the individuals, the National Health Service and the wider economy of £1.5 billion. This research will take a life-course approach to the assessment of the causes and consequences of gastrointestinal infections in the community, from early childhood into early adulthood – continuing into the next generation (ALSPAC-G2 study: Children of the Children of the 90s). This will allow us to provide important insights into changes in causes and consequences of gastrointestinal infections across the individual life-course but also over time at the population level. The findings can then inform public health interventions to reduce the burden of gastrointestinal infections, especially among the most vulnerable groups.

Autism is a chronic condition, arising early in childhood and characterized by two main symptoms: difficulties in social communication/interactions and repetitive behaviours. Sometimes, people with autism also have psychotic illness (e.g. hearing voices or feeling paranoid). The reasons this happens is still unknown. There are several possible explanations:
a. Specific autism-related symptoms, such as repetitive behaviours and restricted interests, might be risk factors for developing psychosis later in life,
b. Genetics of autism might predispose the affected individuals to psychosis later in life,
c. Adverse life events, frequently occurring in people with autism, such as stigmatisation or bullying, might lead to psychosis.
We will investigate these explanations using genetic, clinic and questionnaire data from the ALSPAC cohort. Understanding the reasons why some people with autism develop psychosis is an important step towards developing appropriate prevention strategies and offer adequate psychosocial support to the affected individuals and their families.

Despite the common belief that teachers can impact various aspects of students' lives, the empirical evidence on the breadth and strength of their influence is relatively unclear. This project aims to examine the relative strength of the influence of teachers' characteristics and behaviours as perceived by multiple raters (i.e., teachers themselves, students, and parents) on multiple experiences and outcomes associated with the teacher (e.g., job satisfaction) and their students (e.g., academic achievement).

Metabolites are the ultimate end-point of a biological process and are therefore seen as a link between genotype and phenotype. Assigning individual metabolite changes to diseases is difficult because of the complexity of their interrelationships. Prior to analysis quality control of metabolomics data is required. We have developed a package that automates these quality control steps. We will use the raw metabolomic data as a use case for our package.

Body composition is known to affect metabolite concentrations. These changes may be implicated in disease development. Following quality control we will use the metabolomic data to investigate the relationship between metabolites and different body composition traits.

using same principle of pediatric asthma risk scores to predict asthma in childhood I have created risk factors to predict asthma at age 18 and 26 years old

There has been remarkably little research on women's experience of menstruation from a population health perspective, despite menstruation and pre-menstrual symptoms having wide-reaching consequences for women's physical and mental health. We need a better understanding of the biological (e.g. hormone levels, epigenetics) and lifestyle factors (e.g. smoking, alcohol, diet) that might predict and/or causally affect menstrual experiences (e.g. cycle length, heaviness, regularity, pain and premenstrual mood). This better understanding could inform ways to predict who is at risk of poor experiences, and develop strategies to prevent or improve those experiences. We also need a better understanding of the impact of different menstrual experiences on women's physical and mental health (e.g. fatigue, depression, life satisfaction). Again, this could inform strategies to predict which women are at risk of poor outcomes and help develop preventative interventions.

Social withdrawal (SocW) – defined as reduced social interaction – is a key feature of psychotic disorders and multiple other psychiatric outcomes. Despite growing recognition of its negative consequences, SocW remains one of the least studied human traits, and its underlying mechanisms remain subject of wide speculation. The overall goal of this project is to examine elucidate the role of SocW in the development of psychosis.

By combining clinical data with increasingly powerful ‘genetic risk scores’ (i.e. the sum of risk genes that have shown to be associated with a behavioral trait), we are now able to test whether SocW is a cause or merely a consequence of symptoms in psychosis development. Using the UK Biobank we will create a powerful genetic risk score for SocW, and use this score to examine the role of SocW in psychosis in two large developmental cohorts: The Avon Longitudinal Study of Parents and Children (ALSPAC) and Philadelphia Neurodevelopmental Cohort (PNC). Jointly, these studies followed nearly 16,000 young individuals from childhood to young adulthood, through ages encompassing typical onset of and peak onset age of psychosis. In ALSPAC, we will also test the association between changes in psychotic symptoms and changes in SocW behaviorally, and explore the effects of SocW and established environmental risk in the path to psychosis.

Overall, we aspire to better understand the well-established association between SocW and psychosis, determine critical windows during which individuals may be more or less prone to the influence of SocW, and facilitate much-needed preventive targeted therapies.

Cannabis is widely used for recreational and medical purposes with usage increasing rapidly following its legalization in parts of the world[1]. While there are well-documented effects of cannabis on the users themselves, the impact of its consumption during pregnancy on offspring is much less clear. Previous studies have reported that maternal cannabis usage during pregnancy is associated with lower birth weight and there is the suggestion of impaired neurodevelopment in both observational cohorts in humans and experimental studies in animal models[2-7]. However, how maternal cannabis exposure leads to these adverse health outcomes in offspring remains unclear.
Epigenetic mechanisms play an important role in regulating gene expression and cell homeostasis. Previous experimental studies showed that DNA methylation in offspring could be modified by maternal cannabis exposure[8-10]. In some cases this leads to dysregulation of the immune system of the fetus[11-13]. However, no human studies have yet been conducted, and no specific epigenetic signatures have been identified related to cannabis exposures. We hypothesize that maternal cannabis exposure during pregnancy alters the epigenetic profiles and leads to a specific epigenetic signature of the fetus through in utero exposure, and the epigenetic alterations can then lead to impaired neurodevelopment in the offspring. Therefore, we propose to investigate the association of maternal cannabis exposure around the time of pregnancy with DNA methylation profiles in offspring at birth in the ALSPC cohort.