Individuals with a mental health condition are more likely to develop metabolic syndrome, which is a collection of risk factors for heart disease like elevated blood sugar, cholesterol, and blood pressure. Conversely, those with metabolic syndrome are also at higher risk of mental illness. This relationship can be partially explained by factors like lifestyle and medication; however, shared biology also influences the cardiovascular system and brain. For example, there is emerging evidence that there are genetic risk factors that are related to both mental health and cardiovascular disease. The impact of this genetic risk for both disorders remains poorly understood in children and adolescents. Given early intervention is important for both mental illness and heart disease, understanding these relationships may assist to identify how best to implement early intervention. This study will investigate individuals with high genetic risk for both mental health conditions and heart disease to establish whether this impacts their psychological and physical development.

Poor mental health affects more than one billion people worldwide but despite this frequent occurrence and the potential personal burden, treatment options are scarce and not always effective. There is a need, therefore, for a better understanding of the environmental and biological causes of mental health problems, so that new treatments can be developed.
It is known that stressful or traumatic situations can increase an individual’s chance of developing a range of mental health problems. In response to a stressful situation, whether psychological or physical, the human body activates processes that aim to increase the chance of survival. These responses are referred to as “fight-flight-freeze” and can result in giving the body energy, making you feel more, and reducing the sensation of pain. One key hormone involved in this response is cortisol. Although the release of cortisol in response to stress is initially beneficial, evidence has shown that experiencing severe or ongoing stressful events can lead to abnormal cortisol levels, which in turn has been linked to harmful outcomes, including obesity, cancer, heart disease, susceptibility to infection, and poor mental health.
Mental health problems that have been linked to cortisol levels include psychosis, depression, anxiety, and post-traumatic stress disorder (PTSD). For example, studies have shown that individuals diagnosed with depression or schizophrenia have higher levels of cortisol in their blood or saliva when compared to individuals without a psychiatric illness, while individuals with PTSD have lower levels. Some studies also show that high cortisol levels in early life associate with developing a mental health problem later in life, indicating that stress response abnormalities may cause mental health problems. However, findings are not always consistent, and results are hard to compare as the time of day the cortisol measure is taken and the material used for measurement (e.g., saliva, blood, urine) vary across studies.
One way in which cortisol may be causally linked to mental health problems is through inflammation. In normal conditions, cortisol reduces inflammation (e.g., it’s commonly used to treat inflammatory diseases such as arthritis and asthma), however, studies have shown that under abnormal conditions (e.g., during ongoing stress), the relationship changes and high levels of cortisol are associated with increased inflammation. An increase in inflammation can be harmful to neurons in the brain by affecting neuron functioning and decreasing neuron repair. As such, studies have linked stress-related inflammation to poor mental health, however, the size of these studies are small and, again, studies are hampered by inadequate measures of cortisol and inflammation.
As can be seen, there is a need for large studies using improved measures of cortisol to investigate the causal link between stress response and mental health. In this project we therefore aim to generate reliable, robust measures of cortisol and inflammation using serum measures, genetic data and hair samples, to investigate whether cortisol levels lie on the pathway between early life trauma and mental health and whether they influence inflammation.
This work will inform whether interventions targeting the stress response system have the potential to prevent or treat psychiatric disorders.

Complex disorders such as psychiatric conditions often arise from varying combinations of genetic and environmental factors. This represents a major problem for drug development, as the cause of the disease is highly variable from person to person, and as such, drug response rates vary significantly. By examining an individual’s unique genetic risk factors, treatment response rates could theoretically be increased by improving subcategorization of individuals and personalising the administration of appropriate medications. Although genetic risk scores have been developed for this purpose, the use of epigenetic information in the form of DNA methylation remains relatively underexplored, despite the fact this epigenetic modification can simultaneously index both genetic and environmental risk factors. In this study, we will examine whether DNA methylation can be used to refine the classification individuals with complex disorders and better match affected individuals to personalised medications. In addition, we will also explore the relationship between epigenetic risk for complex disorders and measures of biochemical and metabolic traits to determine whether the epigenetic component of complex disorders is associated with changes in druggable, blood-based biomarkers.

Human activity is having a dramatic impact on our planet's climate, and measures to reduce carbon emissions to limit to extent of this climate change are urgently needed. In this project, using the recently-collected climate change data in ALSPAC we aim to explore the factors associated with climate change beliefs and behaviours, with a specific focus on both behaviours relating to sustainable diets (i.e., reduction of meat and/or dairy consumption) and religious/spiritual beliefs and behaviours (RSBB).

Maternal antenatal anxiety, depression, and stress increase the risk for socioemotional and behavioral problems in childhood, effects which persist into early adulthood (O’Donnell et. al, 2014; Pearson et. al, 2013; Robinson et. al, 2008). These findings are consistent with the fetal origins of mental health hypothesis, which posits that exposures in utero contribute to individual differences in mental health outcomes across the lifespan (O’Donnell, Meaney, 2017).

While the association between antenatal maternal wellbeing and child development is well-established, much less is known about the multi-generational impact of antenatal maternal wellbeing on child health and development. Existing findings from multigenerational studies focus on birth weight (Lahti-Pulkkinen et. al, 2018; Drake et. al, 2015), and antenatal lead (Sen et. al, 2015) or diethylstilbestrol exposure (Kioumourtzoglou et. al, 2018)​​. Interestingly, mouse models have shown the multi-generational effects of stress or dietary manipulations on molecular characteristics of the offspring across multiple generations (Ward et. al, 2013; Radford et. al, 2014; Jawaid, Roszkowski, Mansuy, 2018).

In this proposal, we examine multi-generational effects of maternal well-being (encompassing mental and physical health) in an index pregnancy across 2 or more generations. Our analysis framework will consider important confounds including maternal and child genetic variation and will examine candidate biological processes for the transmission of risk e.g. variation in DNA methylation.

Previous research has identified several regions of the human genome associated with high blood pressure. One such region is the NPR3 gene, encoding the natriuretic peptide receptor-C. Whilst genetic variants in this region are associated with high blood pressure, it is not known which variant/s drive the association or whether the effect on blood pressure occurs through altered expression of the NPR3 gene. This study will use existing ALSPAC data to investigate the association between the NPR3 gene and high blood pressure.

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.

The UK Office for National Statistics estimates that in 50 years’ time, there will be an additional 8.6 million people aged 65 years and over. Longer lifespan has clear benefits, but when it is associated with an increased proportion of the population suffering from age-related diseases, it can pose a burden to individual sufferers and to the economy.

Telomeres are ‘DNA tails’ at the end of chromosomes that shorten as we age, in accordance with the number of cell divisions. The rate at which telomeres shorten is also affected by genetic, environmental and pharmacological factors, which is important because premature telomere shortening is hypothesized to predispose to multiple age-related diseases, including coronary artery disease and rheumatoid arthritis. This is because cells with very short telomere lengths are less able to divide, leading to the accumulation of old, damaged or unhealthy cells within a tissue, and subsequently an increased risk of disease. A deeper understanding of which specific factors affect rates of telomere shortening might allow us to identify who is most at risk for premature telomere shortening and what sort of interventions may be effective at preventing age-related diseases.

This project will use the rich phenotype data within ALSPAC to define genetic, environmental and pharmacological factors associated with telomere length and its rate of attrition.

DNA methylation is an epigenetic change that can influence how our genes are expressed. Smoking has been found to influence DNA methylation, and these changes could be responsible for some of the negative health consequences of smoking. In comparison, the epigenetic changes associated with e-cigarette use are not well known. In this project, we will explore how e-cigarette use is associated with DNA methylation.