This work aims to improving our understanding of the emergence of mental health problems across childhood, adolescence and young adulthood. We will investigate how different biological and environmental factors interact to drive or prevent the onset of mental ill-health.

Respiratory disease, the third largest cause of death in England, affects one in five people. Hospital admissions for lung diseases drive NHS winter pressures, costing £11billion annually. Reducing the impact of respiratory disease and associated health inequalities is a UK Government priority (UK Life Sciences Vision 2021).
In collaboration with ALSPAC we will focus on
• Workstream 2: Asthma and chronic obstructive pulmonary disease (COPD)

Using advanced imaging and novel mathematical approaches, we will identify spatio-temporal brain networks that show altered dynamics in young adults with genetic risk for Alzheimer's disease. The PhD will provide grounding in network neuroscience — an evolving field using network theories to study the brain across multiple scales and modalities.

Dental caries a complex chronic disease of multifactorial etiology that affects a children worldwide. Its risk factors include a susceptible tooth, fermentable sugars and caries bacteria. Certain upstream factors have also been implicated in the etiology of dental caries and they are those that promote a favorable oral environment for dental caries susceptibility and progression. One of such upstream factors is prenatal smoking. The prenatal period is a sensitive time for fetal growth and development, including the development of the primary tooth germ that commences at the end of the 5th week of gestation. Exposure to prenatal smoking during this critical period not only affects the health and wellbeing of the developing fetus but also the quality of the developing tooth. Previous studies that have found an association between prenatal smoking and dental caries in the child relied on self-reported smoking during pregnancy, and thus, susceptible misreporting and recall bias of actual smoking status. This current study utilizes an objective measure of exposure to smoking in-utero in the form of newborn DNA methylation (DNAm) measured in cord blood collected at birth.

Disordered sleep is commonly reported in autism from a young age, as are symptoms of mental illness. Mental health and sleep are known to influence each other in a bidirectional manner within the general population, but the nature of the association between sleep and mental health problems in autism is poorly understood. Moreover, the underlying causes of sleep problems in autism are unknown. Thus, current treatments for sleep problems are largely ineffective in autistic people, and they also face severe consequences of mental ill health, such as high rates of suicidality and in-patient care. We aim to characterise the relationship between sleep problems and mental ill health, and identify factors underpinning the sleep problems in autism and in people with autistic traits. We will focus specifically on childhood and adolescence as this comprises the typical age-range of onset for problems in both sleep and mental health. Our approach to answering these questions will involve statistical modelling of longitudinal data on sleep and mental health in ALSPAC.

The concept of exposome refers to the totality of the environmental exposures (diet, lifestyle, occupational and environmental factors, …) from conception onwards, including its external and internal components. Among non-communicable respiratory diseases, chronic obstructive pulmonary disease (COPD) and cystic fibrosis (CF) are two highly debilitating diseases that are of particular interest to consider in parallel in a human exposome study. The overall objective of the REMEDIA project is to determine how and to what extent the exposome affects the severity and morbidity of COPD and CF throughout the progression of disease, thus providing key elements to design more tailored prevention and care programs. We assess exposome and health data from several cohorts and population registers to determine, at various times of life, whether specific exposome(s) is(are) associated with particular phenotypes of COPD/CF in terms of severity, morbidity, exacerbations and co-morbidities. Yet, lung function development starts in utero and continue up to early adulthood, when a maximal lung function is reached. It is therefore of crucial importance to understand the impact of exposome on this key determinant of adult pulmonary health.

We hypothesize that lung diseases occurrence and lung function development during the youth is both influenced directly by individual/contextual components of the exposome and indirectly (mediated) via more complex pathways. Human research on this topic has generally focused on single exposure–health effect relationships. Our objective is to consider a broader definition to the exposome accounting for its multiple facets at the individual/contextual levels, also taking into account the potential clustering of exposures which may often be observed in combination (e.g. air pollution, socioeconomic indicators and individual health-related behaviours).

Consequently, the specific objective to be addressed using the ALPSAC cohort is to investigate whether there are specific exposome components, in isolation and/or in combination (clusters), linked to lung function trajectories and maximal achieved lung function at early adulthood, taken as an early determinant of COPD and CF outcome.

Multimorbidity (MM) happens when two or more different diseases are present at the same time in an individual. This is
common between physical and psychiatric diseases with almost half of people with a psychiatric disease also having a
physical disease. As well as about a third of people with a physical disease also having a psychiatric disease. These
patients have worse quality of life than those with a single disease, they often struggle to get the best care and are at risk of
living less long. A common and serious type of MM is between internalizing diseases (depression and anxiety) and
cardiovascular disease (ICV-MM). Still, very little is understood as to how ICV-MM develops and why it happens. We do
know however that both internalizing disease and cardiovascular risk (e.g., obesity, cholesterol) tend to begin before
adulthood.
To really understand how ICV-MM risk develops, we need large studies of people of all ages whose health has been followed
over time. Studies of children are crucial because they can tell us about early risks for development of ICV-MM later in life.
This is important for developing better plans to prevent at-risk children developing ICV-MM.
We know that genes influence risk of both internalizing and cardiovascular disease and that some people are at high
genetic risk. We also know that certain conditions that start early in life (neurodevelopmental conditions) such as
intellectual disability, autism and ADHD increase risk of developing ICV MM later. Children's environments can also
increase this risk, for example, stressful experiences such as poverty and physical or sexual abuse. But how exactly genes,
neurodevelopmental conditions and early environmental risks influence the development of ICV-MM over the lifespan is still
not understood.
Certain groups are known to be at increased risk of ICV-MM, such as people of South Asian heritage and women, but we
don't know why this is. Better understanding of how ICV-MM develops in different groups in society will help doctors give
patients care that is matched to their specific needs. It will also help doctors, governments and schools prevent ICV-MM in
at-risk children in ways that work best for them.
To really understand the complexities of ICV-MM development, a team of researchers with a wide range of expertise is
needed who together understand physical and psychiatric diseases as well as how genetics, neurodevelopmental
conditions and the environments people live in influence them throughout their lives.
Our LIfespaN multimorbidity research Collaborative (LINC) combines wide-ranging medical and research expertise in
physical and psychiatric diseases. We have brought together five very large studies in which the health of many people has
been followed over time. Rich medical data is available, including from medical records. Genetic information is also
available for these people. Other important information has also been collected such as on people's living environments,
life events and lifestyles.
These studies follow the health over time of children, adolescents and adults. We can therefore study how internalizing and
cardiovascular disease happen together in adulthood. Importantly we can then also study early risk factors in the children
before they develop these conditions. Because our child and adult samples differ in ethnicity and economic situation, we
can also study how the development of ICV-MM differs for different groups in society. Finally, because we have genetic
data, we can study how genes influence ICV-MM development in people at risk.
Our study will help us understand how ICV-MM develops and which circumstances influence this. What we learn will be
important for the prevention of ICV-MM in children who are at risk because of genetics, their sex, or ethnic or economic reasons. We will work with patients, doctors and charities to develop specific health advice in order to reduce ICV-MM in at
risk groups in the future.

To explore the associations between fetal alcohol spectrum disorder (FASD) / Prenatal alcohol exposure (PAE) and adolescent multiple risk behaviours (MRBs). We are interested in exploring the prospective associations between prenatal alcohol exposure and MRBs, such as self-harm, drug use, tobacco smoking and alcohol consumption which are known to increase through adolescence and may persist into adulthood leading to multiple and composite adverse health outcomes. Identifying at risk adolescents could be used to aid the development of interventions and preventative policy.

Some people experience symptoms caused by COVID that last longer than the original infection and these can be severe or disabling (COVID Symptom Study, 2020). This study aims to better understand why some people develop ‘long COVID’ – symptoms lasting longer than four weeks (National Institute for Health and Care Excellence, 2020) – and others do not. We will be comparing long COVID symptoms between those who have had COVID confirmed by a test, and those who believe they have had COVID but have not had a positive test. We will then explore whether this relationship is different between men and women, and between those who reported anxiety and those who didn’t. We hope that this research will help us to understand better whether psychological mechanisms contribute to the development of long COVID.