We propose to address the problem of handling large-scale genome-wide DNA methylation data. To this end, we will develop a novel technique for clustering DNA methylation (DNAm) sites which will aid reducing the complexity of the subsequent EWAS. For example, a DNAm site that is hypo-methylated in the smoker cohort but hyper-methylated in non-smoker one merits further analysis for significant association with smoking, while those sites exhibiting no difference in the two cohorts does not.
We will investigate the use of algorithms for large matrix factorisation under constraints to provide a natural clustering of DNAm sites, and study what statistical guarantee is achievable under which conditions. To verify the suitability of the proposed method, we propose to use the DNA methylation data available from ARIES.

A subgroup of people in the population have a change in their genetic make-up that greatly increases their risk of physical disorder and psychiatric disorder. The medical consequences of these genetic changes are however still very poorly understood. Particularly, we don't really know how these changes lead to increased risk of combinations of physical and mental health problems over time. As presence of a physical or mental health problem increases risk of other ones developing, it is important to understand how and why this happens in this high-risk group. Because these genetic changes are rare, it is important to bring together large samples to study their role in medical outcomes properly. This is particularly important if we want to understand how these changes influence the combined risk of physical and mental health problems in different groups within the population, for example young people versus adults, different ethnic groups and groups from different socio-economic backgrounds. To study these important questions, we propose to work together across four large UK studies in which these genetic changes have been established and which have collected rich information on physical and mental health as well as relevant risk factors. The data sets we will work with differ in the age and ethnic and socio-economic background of the participants. We will be able to follow over time how risk of physical and mental health problems influence each other and how this may be different in these different age. ethnic and socioeconomic groups. The findings will have important implications for developing better interventions for this group, for understanding complex medical risks in the population more generally and for insights into the biology of complex medical risks.

Alcohol use during adolescence is a major public health concern, in particular because the brain is still developing and undergoing considerable structural and functional changes. Identifying risk factors that influence adolescent alcohol use is important to appropriately target prevention programs. One area of research that has received considerable attention is the role cognitive functioning (e.g., working memory and inhibition) play as risk for involvement in adolescent alcohol use. There is also a large literature showing a relationship between substance use and self-harm. It is possible that alcohol may increase the risk of self-harm by lowering inhibitions and impairing working memory, which is central to decision making. There is also evidence to suggest that there may be a bi-directional relationship, as several longitudinal studies have reported an association between adolescent self-harm and alcohol problems in adulthood. Although previous prospective studies have examined this association, they are often limited by the use of small sample size, different alcohol use phenotype (i.e. bingeing vs frequency), different follow-up periods, or lack of control for relevant confounders.

Socioeconomic differences in cardiovascular health are evident in adulthood. When these inequalities emerge and how they change through the life course is not well understood. Understanding when inequalities in cardiovascular health emerge may inform early life prevention opportunities.

Maternal education, a predictor of social-economic status, has been associated with several offspring health outcomes during the life course (e.g. obesity, type 2 diabetes, cognitive function...). The biological mechanisms regulating this association are yet to be understood. Possible mediation in the maternal education-offspring health outcome relationship might be played by DNA-methylation epigenetics markers. We therefore aim to investigate how epigenetics changes are associated to maternal educational attainment.

Between 2015 and 2016, obesity affected approximately 13.7 million children and adolescents in the United States. Children with obesity are more likely to have high blood pressure, abnormal lipids and insulin resistance even though overt cardiovascular disease may not develop for decades.Additionally, children with obesity are at increased risk for musculoskeletal and mental health disorders, as well as certain cancers. This project aims to to better understand the development and progression of the metabolic derangement seen with obesity in children as well as the associations with development of comorbidities. Inflammation is considered to be the common link between obesity and its progression to various comorbidities. If we are able to identify an early signal in children with obesity who are more likely to develop diseases such as asthma, cardiovascular disease and cancers we will be able to address the problem in a timely fashion and offer focused intervention and treatment to these high risk children

Mental illness accounts globally for one third of years lived with disability, leading to tremendous loss of human, societal and economic potential. Most symptoms (e.g., depression, anxiety, conduct problems) emerge before adulthood, highlighting the first two decades of life as an important period of heightened vulnerability. Epigenetics has emerged as a biological system that captures the underlying genetic and environmental risk factors, but we do not yet understand the developmental dynamics in this system over time. Such knowledge, however, is critical if we are to understand how mental health disorders develop, and thus how they may be prevented.

Sleep disturbances during childhood are common and often resolve spontaneously without intervention (Touchette et al., 2005; Galland et al., 2012). However, those that are persistent and frequent have been shown to be associated with the development of later psychopathology including psychotic like experiences (Jeppesen et al., 2014). Previous research exploring data from the Avon Longitudinal Study of Parents and Children has shown that children, aged 2.5 and 9 years old, experiencing frequent nightmares were more likely to report psychotic experiences at age 12 (Fisher et al., 2014). Similarly, nightmares at 12 years old was also found to be associated with an increased risk of psychotic experiences at aged 18 (Thompson et al., 2015). Such findings suggest that nightmares during childhood may represent an important and clinically significant indicator for risk of psychotic experiences in adolescence.

The relationship between childhood sleep disturbances and the presence of psychotic experiences beyond the age of 18 is still yet to be understood. Research has shown that the incidence of psychotic experiences often peaks during adolescence to early adulthood (McGrath et al., 2016) and sleep disturbances frequently co-occur with psychotic like experiences during this time (Taylor et al., 2015). Consequently, understanding which early sleep problems present as a risk factor for the development of later psychotic experiences is key. This project will explore the longitudinal associations between childhood and adolescent sleep problems between the ages of 2.5 - 17 years old and self-reported psychotic experiences at 24 years old.

Fisher, H.L., Lereya, S.T., Thompson, A., Lewis, G., Zammit, S. and Wolke, D., 2014. Childhood parasomnias and psychotic experiences at age 12 years in a United Kingdom birth cohort. Sleep, 37(3), pp.475-482.
Galland, B.C., Taylor, B.J., Elder, D.E. and Herbison, P., 2012. Normal sleep patterns in infants and children: a systematic review of observational studies. Sleep medicine reviews, 16(3), pp.213-222.
Jeppesen, P., Clemmensen, L., Munkholm, A., Rimvall, M.K., Rask, C.U., Jørgensen, T., Larsen, J.T., Petersen, L., van Os, J. and Skovgaard, A.M., 2015. Psychotic experiences co‐occur with sleep problems, negative affect and mental disorders in preadolescence. Journal of Child Psychology and Psychiatry, 56(5), pp.558-565.
McGrath, J.J., Saha, S., Al-Hamzawi, A.O., Alonso, J., Andrade, L., Borges, G., Bromet, E.J., Oakley Browne, M., Bruffaerts, R., Caldas de Almeida, J.M. and Fayyad, J., 2016. Age of onset and lifetime projected risk of psychotic experiences: cross-national data from the World Mental Health Survey. Schizophrenia bulletin, 42(4), pp.933-941.
Taylor, M.J., Gregory, A.M., Freeman, D. and Ronald, A., 2015. Do sleep disturbances and psychotic-like experiences in adolescence share genetic and environmental influences?. Journal of Abnormal Psychology, 124(3), p.674.
Thompson, A., Lereya, S.T., Lewis, G., Zammit, S., Fisher, H.L. and Wolke, D., 2015. Childhood sleep disturbance and risk of psychotic experiences at 18: UK birth cohort. The British Journal of Psychiatry, 207(1), pp.23-29.
Touchette, É., Petit, D., Paquet, J., Boivin, M., Japel, C., Tremblay, R.E. and Montplaisir, J.Y., 2005. Factors associated with fragmented sleep at night across early childhood. Archives of pediatrics & adolescent medicine, 159(3), pp.242-249.

Different parts of our brains communicate with one another as we learn new information during the day, then continue to communicate “offline” as we sleep. This overnight brain activity helps file memories for long-term storage, but the process is complex and delicate: lots of genes influence brain activity in ways we do not yet understand. We also need to establish why and how this process is disrupted in disorders like schizophrenia, which are associated with impaired sleep-dependent brain activity and memory. This study will investigate links between a set of schizophrenia-associated genes and brain function during sleep.

Participants will be asked to wear a ‘fitbit’-like device for 2 weeks of normal activity, so we can track when and how much they sleep. We will then use a comfortable sleep cap that contains an array of recording devices to monitor EEG brainwaves while participants sleep at home for 2 nights. By analysing the EEG data using machine learning methods (similar to those used for speech recognition), we will identify patterns of activity that make up their personal “sleep fingerprint”. This will allow us to test whether these fingerprints vary according to genetics in a healthy population, without interference from things like medication that complicate patient studies.

The main outcomes will be (1) development of novel analysis methods allowing us to capture brain activity, (2) a deeper understanding of the mechanisms that determine variation in patterns of brain activity during sleep and (3) a route towards understanding mechanisms of schizophrenia liability.