Previous studies have demonstrated that maternal thyroid dysfunction is associated with a number of neurodevelopmental disorders, such as attention deficit hyperactivity disorder and epilepsy. However, the association between maternal thyroid dysfunction and other health outcomes in offspring were either investigated in single study, or not examined. One single study conducted in 998 maternal-child pairs in Canada demonstrated that maternal hypothyroidism was associated with increased risk of congenital heart disease (CHD) in offspring (OR=1.68; 95% CI: 1.02-2.78). Another retrospective cohort study showed that children born to mothers with hypothyroidism have increased risk of hypoglycemia (RR=2.9; 95% CI: 1.4-6.2) and total endocrine morbidity (RR=2.1; 95% CI: 1.2-3.8). It was also observed that offspring of mothers with subclinical hypothyroid during the third trimester of pregnancy had higher systolic blood pressure. It remains unclear if the above associations exist in other populations. Whereas, inconsistent findings were observed for the risk of diabetes in children born to mothers with various thyroid diseases. It is known that thyroid dysfunction in adults may affect a number of cardiometabolic traits. This project aims to evaluate the observational and causal association between maternal thyroid dysfunction and various cardiometabolic traits in offspring.

Stark inequalities in health already exist in the UK, with people from lower socioeconomic backgrounds suffering from greater levels of ill health across multiple domains. The covid-19 pandemic potentially threatens to worsen these health inequalities. The ‘lockdown’ changed people’s behaviour radically, but the socioeconomic differences in these experiences are not well understood. Some groups of society may have increased health-promoting behaviours – for example, engaging in more physical activity and preparing more food within the home. Other groups may have experienced adverse changes in health-related behaviours – for example, smoking more or consuming more alcohol in response to the stress and anxiety induced by the pandemic. It is possible these differences are socioeconomically patterned, and could therefore worsen pre-existing inequalities. Another key factor likely to influence patterns of behaviour change during the pandemic is household/family structure. For example, parents with children and individuals shielding or living with a household member who was shielding may have been less able to engage with health-promoting behaviours.

Data from the Office for National Statistics demonstrate that between 23rd March and 5th April 2020, 27% of the UK workforce were furloughed due to the COVID-19 lockdown. Many others lost jobs, or had working hours and income reduced. The adverse financial and employment consequences of the covid-19 lockdown are concentrated in already vulnerable groups of society – they are more likely to be experienced by people in insecure or low-paid jobs. The young adults in ALSPAC are in the age groups most likely to have been affected by furlough, job losses, and loss of pay or hours (https://www.resolutionfoundation.org/publications/young-workers-in-the-c...). Detailed pre-pandemic data from the ALSPAC cohort offers the opportunity to better understand which groups of society were more likely to be impacted financially by the lockdown. We will explore whether SEP, adverse childhood experiences, pre-existing mental health problems, obesity, smoking, alcohol use, shielding or living with a household member who was shielding, and family structure are associated with greater likelihood of adverse financial changes during covid-19, and hence whether the lockdown is likely to exacerbate health challenges for these groups.

New-onset hypertension during pregnancy occurs in up to 10% of women. People born to pregnancies complicated by hypertension (i.e. gestational hypertension and preeclampsia) are at increased risk for cardiovascular disorders, including hypertension and stroke, in later life. The underlying disease process is identifiable in the first decades of life with evidence of emerging damage to their hearts and blood vessels. Phenotypic changes that have been observed in early postnatal life and as they reach young adulthood include higher blood pressure, altered heart structure and function, as well as a reduced number, size, and function of small blood vessels. However, to date, longitudinal data in the same individuals, as well as a multi-systems, deep phenotyping approach to characterizing cardiovascular physiology in offspring of hypertensive pregnancies, remains limited. By using ALSPAC, we will be able to make use of the previously collected demographic, anthropometric, and phenotypic data collected. We will also design a new study in 200 young adults, of which 100 will be born to hypertensive pregnancies and 100 born to normotensive pregnancies. These participants will be invited by the ALSPAC team to travel to Oxford for a 3 hour study visit, including blood sample collection, exercise stress testing, blood pressure and imaging of the small blood vessels in the eye, brain MRI, as well heart scans using both MRI and echocardiography at rest and during exercise. By studying and tracking changes both temporally and spatially across multiple organs, we will be able to better describe and quantify the multi-dimensional landscape of hypertensive disease progression.

Autism is a lifelong condition characterised by difficulties with social interaction, social communication and repetitive behaviours. In recent decades, the number of children and adults diagnosed with autism has increased. As autism is heritable, genetic risk may explain why there are some individuals with mild autistic traits but they may not meet the criteria for an autism diagnosis and subsequent treatment or other support requirements. As more children with autism and mild autistic traits reach adulthood, the need for support from health and other services will likely increase. However, few large, population based longitudinal studies involving adults with autism/autistic traits exist, representing a research gap.

During this phase of my PhD project, I will study how autism and autism traits, including genetic risk for autism, may be associated with BMI and disordered eating behaviours in adulthood. Children with autism often having sensory issues and unusual eating preferences, which could have an effect on growth and health in adult life. It has been reported that social communication difficulties may increase the risk of disordered eating patterns in adolescence. This implies that maintaining a healthy BMI may be challenging during this period and that there is a possible increased risk of disordered eating behaviours and eating disorders in adulthood for those with social communication difficulties. This phase of my PhD project is focussed on whether autistic individuals are more likely to have high BMI and disordered eating behaviours in adulthood. Changes in growth during late childhood into late adolescence will also be studied to assess whether there are critical periods that are suitable for intervention.

The obesity epidemic is one of the most important health challenges of the 21st century.
Identifying genetic factors predisposing to weight gain is crucial for identifying biological processes important for weight-control and help identify individuals already at young age that might benefit from health interventions and thereby reducing their risk for disorders such as type 2 diabetes that follow in its footpath.

While there is great progress deciphering the genetic factors influencing weight in in adulthood, and at birth, there is a huge knowledge gap on the role of the genomes of the child and its parents in infancy and childhood into puberty. This is very unfortunate, as it is firmly established that the BMI-development during the first 6 years of life are strong predictors of obesity in adolescence . Results from our own ongoing work in the Norwegian Mother, Father and Child and work of others show that it is possible to find novel genetic variants with specific and substantial effect on weight development during infancy with high quality data and large GWAS sample sizes.

Neonatal jaundice is a yellowish discoloration of the eyes and skin in a newborn baby as a consequence of high bilirubin levels. While jaundice in most newborn is normal, a subset of patients with elevated bilirubin levels may develop excess sleepiness or poor feeding, whereas patients with excessive bilirubin levels are at risk for severe brain damage. In this project we aim to identify genetic risk factors for the development of high bilirubin levels in the newborn. This information can aid in risk prediction and the onset of early treatment for hyperbilirubinemia in the newborn.

Eyesight Problems and Psychotic Illnesses: What’s the Link?
Psychotic illnesses affect just under 1% of people in England. Symptoms include hearing voices and experiencing confusing and distressing thoughts. These often begin in early adulthood, and can have a major effect on people’s lives.
People with psychotic illnesses seem to have more eyesight problems. We are not sure why, but it might be because:
• Possibility 1: Some people with psychotic illnesses find it harder to look after their health including their eyes, for example by going to the optician’s.
• Possibility 2: The same brain changes cause eyesight problems and psychotic illnesses.
• Possibility 3: Eyesight problems increase a person’s chances of having a psychotic illnesses.
I plan to look at which of these best explains the link between eyesight problems and psychosis. If people with psychosis have less eye care (possibility 1), we need to improve this. If possibility 2 is correct, eye research might hold the key to understanding more about the brain changes that cause psychosis. Or, if eyesight problems lead to psychosis, then improving eye health could be a way of preventing or reducing psychosis.
I will start by reviewing past research, to make sure I base my work on the most up-to-date information. I will then carry out research using two large datasets: UK Biobank and the Avon Longitudinal Study of Parents and Children (ALSPAC).
UK Biobank has information on over half a million 40 to 69-year-olds including questionnaires, eyesight tests and genetic tests.
ALSPAC has information on 14,500 UK families. The children have been followed up since before birth and will be 25.
I will look at UK Biobank and ALSPAC because older and younger people are most at risk of developing psychosis. In these datasets, I will see if people with short-sight genes have more psychotic illnesses. If so, this would be evidence that poor eyesight can lead to psychosis. Genes are present before birth, so I will know that they came before any psychotic illness began. I will also find out if genes for psychotic illnesses are linked with eyesight problems. This would suggest the reverse: that psychosis leads to poor eyesight.
I will also use a third, Israeli dataset. All Israeli 17-year-olds have health checks to decide if they can join the armed forces. I will use this data to find out if teenagers with eyesight problems are more likely to have a psychotic illness over the following years. If so, I will see what level of eyesight problems are associated with developing psychosis. This will allow me to test the theory that perfect eyesight and complete blindness both protect against psychosis, with moderate eyesight problems carrying the highest risk.
Throughout this research, I will chair a group every 6 months. It will include people with psychosis, people with eyesight problems, carers, charity members and doctors. We will discuss study findings and think about how to use them to improve the experiences of people with eyesight problems and psychosis. This will include plans to publicise findings, influence healthcare and plan new studies.
When the research is finished, I will tell healthcare professionals and researchers about the results at meetings and in journals. I will also write about them in publications read by people with mental health and eyesight problems. I will offer to present findings to public groups, through links with the Royal National Institute for the Blind (RNIB) and a forum of mental health service users.
People with eyesight problems and mental health service users helped to write this summary.

The remit of the Advanced Pain Discovery Platform funding call is to better understand the mechanisms associated with pain. Our Expression of Interest is focused on psychosocial mechanisms of pain, and as part of this we wish to see how these impact on individuals across the lifespan. We wish to explore potential psychosocial correlates of pain, and build on work already conducted by members of our consortium on pain. Details of this project will be updated in due course.