Observational studies in children and adolescents have found evidence for prospective associations between behaviour/emotional problems and incontinence. Although prospective studies reduce the likelihood of reverse causation, they are limited by residual confounding. 

Depression and anxiety are debilitating conditions that often start in late adolescence and young adulthood.
Understanding who is at the most risk of these conditions is important because it can help to target and tailor preventative approaches.
This project will aim to identify the smallest group associated with the largest amount of new cases of depression and anxiety.

Autistic traits refer to characteristics commonly seen in individuals with autism spectrum disorder (ASD), such as difficulties with social interaction and communication, repetitive behaviours, and restricted interests (1). Some studies have suggested that individuals with ASD may have a higher risk of experiencing constipation and continence problems (2, 3). This may be due in part to sensory processing difficulties that can affect the way individuals with ASD perceive and respond to bodily sensations, including those related to bowel and bladder function (3). In addition, some individuals with ASD may have dietary restrictions or preferences that could contribute to constipation such as avoiding certain textures or types of food (3).

Further research is needed to better understand the relationships between these problems (constipation and continence) and autism and to develop effective interventions for individuals who experience these problems. Although several clinical studies have been conducted in the past to investigate these relationships (4), to the best of our knowledge, no population-based studies have been done. This research will examine relationships between autistic traits and continence and constipation in children and adolescents in the ALSPAC cohort.

Attention-Deficit Hyperactivity Disorder (ADHD) has symptoms of inattention, hyperactivity, or both. However, patients with ADHD often experience symptoms of other disorders such as autism spectrum disorder (ASD), epilepsy, conduct disorder, or anxiety symptoms. Previously, it was reported that there are shared heritability and cognitive process across the conditions, implying that there are common underlying biopsychological factors that have not been identified.Epigenetic biomarkers, especially blood DNA methylation (DNAm) became significantly important in understanding neurodevelopmental disorders such as ADHD. Even though the associations between DNAm and each condition were investigated, there is a limited amount of research on DNAm biomarkers across ADHD-related phenotypes (ADHD and co-occurring symptoms). We hypothesized that the underlying biological factors would be specific to clusters of conditions and could be used as a diagnosis factor for children. Therefore, we propose to investigate the relationships between each of the individual traits linked to ADHD and DNAm to reveal their epigenetic similarities and differences. The epigenetic similarities and differences will give in-depth insight to understand ADHD. We will use a series of computational methods including EWAS and machine learning to investigate the DNAm biomarkers of complex ADHD-related phenotypes from around 1500 participants from the Avon Longitudinal Study of Parents and Children.

Previous research has found partial evidence for a role of personality traits in mental health outcomes. However, many of these studies do not examine all of the big 5 personality traits simultaneously, examine mental health generally, or a small number of mental health symptoms. These studies also tend to examine participants cross-sectionally, without examining the way in which personality traits may influence mental health longitudinally, after controlling for confounders. This study aims to overcome the previous patchwork coverage of this topic by combining a range of exposure and outcome variables in a prospective cohort study.

Individuals with Attention deficit hyperactivity disorder (ADHD) may be more likely to suffer from mental health problems than the general population. We aim to investigate the relationship between ADHD and depression using data from a longitudinal study of over 14000 children born in the early 90s with ongoing data collection. We will investigate whether specific risk factors such as bullying and childhood adversity may influence this relationship and act as modifiable targets for intervention.

X-linked, red-green colour blindness (CVD) is a congenital condition affecting 8% of men (0.4% of women). Depending on type and severity, affected individuals have significant difficulties discriminating a wide range of colours facing wide-ranging challenges on a day-to-day basis (e.g. interpreting colour-coded information at the workplace or recreational environments). A growing impact is expected in educational settings due to an increasing reliance on colour resources in schools. Unfortunately, a study using a birth cohort from 1958 (Cumberland et al, 2004) has reported a lack of impact of colour blindness on Maths and reading ability but fails to account for the increase in colour in classrooms in recent years. Regrettably the publication led to the cessation of CVD school screening in 2009, preventing children from accessing more appropriate resources.
In contrast, a number of authors have argued that CVD can increase difficulties experienced in a range of school subjects including Sciences, Maths, Art, PE and Geography as such subjects may use colour to explain concepts, give instructions and require it in problem solving tasks. Alongside any academic implications, CVD has been found to have an effect on social, psychological and emotional outcomes. For example CVD children may experience teasing from classmates.
We here propose to investigate the potential impacts of CVD on education and emotional outcomes in a more recent cohort.

Studies conducted using animals have been instrumental in describing the brain impairment and physiological processes that cause prenatal alcohol exposure (PAE). Research has shown that similar brain and physiological features are likely to be affected in those displaying
increase criminality and behavioral disorders. Some features affected include inattention, impulsivity, the poor executive functioning, impulse control, memory and cause and effect thinking.

Fetal alcohol spectrum disorder (FASD) is attributed to the effects of PAE, and has been associated with a two to six fold increase in mental disorder diagnosis in offsprings of alcohol binge drinking mothers. Youths with FASD are 19 times more likely to end up incarcerated than those without. Cigarette smoking and illicit drugs used in pregnancy also contribute to adverse pregnancy outcomes and are important risk factors of criminality.

Offspring of mothers who drank during pregnancy especially heavy drinking of greater than 21 units a week, will be at an increased risk for adolescents antisocial activities and conversely criminal activities in adulthood. It is also likely that there is a positive relationship between the quantity of alcohol used and number and intensity of antisocial activities and criminal activities.

Analytical approaches which disentangle heterogeneous effects on trait susceptibility provide important insight on the relationship between complex traits and disease. Lifecourse Mendelian randomization (MR) is a novel statistical approach which has been developed to address lifecourse specific effects on disease susceptibility (1, 2, 3). Additionally, stratifying instrumental variables based on tissue derived gene expression data provides further molecular context to interpret the effect (4, 5).

Evaluation of the relationship between lifecourse and tissue dependent effects on biomarkers measured in early life provides important insight on key etiological and susceptibility windows of disease. The results of a recent analysis have provided evidence of a direct effect for the brain-mediated component of body-size on the adipose tissue secreted hormone leptin measured at age 10 in the lifecourse (Richardson et al, in revision). Through the integration of tissue-specific data, this approach highlights the etiological importance of appetite regulation in the links between adiposity and leptin levels in early life.

Additionally, this study also showed evidence for an effect of adult body-size on circulating leptin measured in childhood (when accounting for the effect of early life body size), which is directionally implausible. This raises the possibility that the adult derived exposure may be a strong predictor for traits in early life which have an effect on childhood leptin levels. In this project we will further characterize the relationship between adult body size and early life adiposity measures and a range of childhood biomarkers to refine the interpretation of this causal relationship.

References:

1. Richardson TG, Sanderson E, Elsworth B, Tilling K, Davey Smith G. Use of genetic variation to separate the effects of early and later life adiposity on disease risk: mendelian randomisation study. BMJ. 2020;369:m1203.
2. Richardson TG, Power GM, Davey Smith G. Adiposity may confound the association between vitamin D and disease risk - a lifecourse Mendelian randomization study. Elife. 2022;11.
3. Sanderson E, Richardson TG, Morris TT, Tilling K, Davey Smith G. Estimation of causal effects of a time-varying exposure at multiple time points through multivariable mendelian randomization. PLoS Genet. 2022;18(7):e1010290.
4. Leyden GM, Shapland CY, Davey Smith G, Sanderson E, Greenwood MP, Murphy D, et al. Harnessing tissue-specific genetic variation to dissect putative causal pathways between body mass index and cardiometabolic phenotypes. Am J Hum Genet. 2022.
5. Leyden GM, Greenwood MP, Gaborieau V, Han Y, Amos CI, Brennan P, et al. Disentangling the aetiological pathways between body mass index and site-specific cancer risk using tissue-partitioned Mendelian randomisation. Br J Cancer. 2022.