Proposal summaries
B4639 - Understanding the role of epigenetic regulation of thyroid function using data from TWINS UK and ALSPAC cohorts - 11/06/2024
DNA methylation (chemical marks on the DNA code) can change the activity of genes and how our cells function. There is evidence that mother’s environment can influence her baby’s DNA methylation and have lasting health consequences.
Little is known about how DNA methylation affects the genes related to the thyroid gland but it could be an important factor in thyroid disease and health.
Using large established datasets (TWINS-UK, ALSPAC), we will explore how DNA methylation at important areas of the genetic code influences thyroid hormone production in children and how the mother’s environment may contribute to these DNA methylation changes.
B4637 - The Effects of Non and Pre- and Postnatal Exposure to Paternal Anxiety on their offs - 10/06/2024
Anxiety disorders (AD) are the most prevalent
psychiatric condition in the general population worldwide, and it is estimated that
between 6.57 and 13.54% of new fathers suffer from an AD (Leiferman et al.,
2021), a considerably higher proportion than the prevalence for anxiety in men
generally estimated by the World Health Organization (World Health Organization,
2017; range between 2.2 − 3.8%). The mental health of children is robustly
associated with the mental health of their parents (Jami et al., 2021). In particular,
children whose parents suffer from ADs, compared to children whose parents do
not, have a higher risk of struggling with their mental health (e.g., Connell &
Goodman, 2002; Micco et al., 2009; Lawrence et al., 2019). However, the specific
role played by fathers in children's mental health difficulties has been underinvestigated, and the particular risk posed by paternal anxiety for offspring mental health difficulties is not well understood.
B4629 - Urban exposome and blood pressure trajectories from birth to adolescence - 26/06/2024
Previous studies exploring the influence of the urban environment on later blood pressure have mostly focused on single exposures, or a specific, related group of exposures, and have assessed the influence on blood pressure at specific ages. However, we are simultaneously and cumulatively exposed to various environmental exposures, including air pollution, traffic, noise, natural spaces, built environment, food environment, meteorological factors and social deprivation. Therefore, further research using a more holistic view of the urban environment and assessing the longitudinal association with blood pressure using repeated measures is needed. This project will use an exposome approach to understand how a range of urban environmental exposures during pregnancy and childhood influences changes in children's blood pressure from birth to 18 years old. We will analyze data from up to 18 different cohort studies, including up to 74,000 participants.
B4632 - Effects of Socioeconomic Inequalities in Childhood Respiratory Tract Infections - 06/06/2024
Respiratory Tract Infections (RTIs) are the most common health problem in childhood, with children suffering on average 4-8 RTIs a year. Social determinants like parental education and household income, in addition to environmental and behavioural risk factors early in life, can influence susceptibility to RTI outcomes. Children living in disadvantaged socio-economic circumstances (SECs) are more likely to suffer from severe RTI outcomes, but the pathways leading to these inequalities are complex, inter-related and poorly understood. The overall objective of this project is to understand the burden of Upper and Lower Respiratory Tract Infections in children in Europe. Using federated analyses of data from the EU Child Cohort Network, the project aims to explore the social and geographic patterns and the pathways that relate social characteristics, early-life risk factors and childhood RTIs. Understanding these patterns and pathways is vital to inform preventative policy and help reduce the unfair child health differences through effective public health interventions.
B4634 - The Role of Epigenetics and Parenting in the Association Between Child Maltreatment and Depression - 06/06/2024
Child maltreatment including traumatic experiences such as physical or sexual abuse is a consistent risk factor for depressive disorders. Depression often results from a combination of environmental, biological and psychological factors. Factors that explain this association between childhood trauma and depression are still being studied. Genetic factors could be a bridge between environmental stressors and the pathophysiology of depression. Research has already shown that parenting practices could be a protective factor for depression development; however, research is needed to explore the interaction between epigenetics and parenting in predicting depression symptoms in children. This study seeks to address these gaps in the literature.
B4633 - Bilingualisms influence on Mental Health - 17/06/2024
One in 5 children in the United Kingdom speak two or more languages (Department of Education, 2020). Some studies have shown that bilingual children have greater mental health issues compared to monolingual children (Guhn, et. al., 2010). However, Halle et al. (2012) found that bilingual children had fewer mental health problems than their monolingual peers. Due to mixed results in the literature, it is unclear what the consequences for children’s and adolescents’ mental health when grown-up bilinguals. Using data from the Millennium Cohort Study (MCS), we have shown that bilingualism acts as a protective factor on mental health for children between 3 to 11 years old (Salgado-Garcia, Devine, & Krott, in preparation). Compared to monolingual children, bilingual children had lower levels of internalizing and externalizing problems when sex differences, nonverbal IQ, family background (SES), school characteristics, and language proficiency were taken into account. The current project aims to investigate the cognitive mechanisms underpinning the difference between bilingual and monolingual children’s mental health, specifically focus on executive functions and theory of mind.
B4630 - The Roles of Parent-Child Relationships and Cognitive Development in Mental Health Outcomes - 17/06/2024
Many adult mental health problems begin in childhood or adolescence. Research has found that individuals are at increased risk of poor mental health outcomes even in childhood and early adolescence. Those children who are at increased risk of childhood psychopathology are more likely to experience adverse early life conditions. Life history and life course models suggests that adverse early life conditions may increase their risk of poor mental health via cognitive dysregulation. However, most of previous studies focused on childhood maltreatment while ignored other indicators of harshness and unpredictability of early life conditions (e.g., inconsistent pattern of religiosity and parenting behaviors). Thus, the first aim of this project is to test how other indicators of harshness and unpredictability of early life conditions are associated with cognitive dysregulation, resulting in poor mental health outcomes in childhood and early adolescence.
In addition, non-heterosexual adolescents may be at greater risk of poorer mental health even in early childhood and adolescence compared with heterosexual adolescents, which cannot be fully explained by the common genetic influences, childhood gender nonconformity, and early life conditions. Instead, it is possible that psychological and “cognitive” factors (such as how one interprets the world, beliefs about the self, attention, and sense of autonomy) influence in part mental health outcomes in these adolescents. Thus, the second aim of this project is to test how cognitive factors in childhood and adolescence among non-heterosexual individuals influence their mental health outcomes.
B4628 - Socioeconomic inequalities in the cardiometabolic health effects of air pollution - 18/06/2024
Air pollution is the most important environmental risk factor for health, including for cardiovascular diseases (CVD), and there is growing evidence of its adverse effects on cardiovascular and metabolic health across the life course. Air pollution is the leading contributor to the global disease burden, contributing more than well established CVD risk factors, such as high systolic blood pressure, high glucose, high body mass index (BMI) and smoking.
The adverse cardiometabolic health effects of air pollution might be more pronounced among low-income, low-education, and ethnic minority groups, partly due to the generally increased air pollution exposures and the higher prevalence of risk factors for poorer cardiovascular health in socioeconomically disadvantaged populations. Therefore, a comprehensive understanding of the links between socioeconomic status (SES), ethnicity, air pollution, and health across different ages is crucial.
Postulated mechanisms linking air pollution to cardiometabolic health comprise oxidative stress, endothelial dysfunction, and inflammatory responses. Proteomics is a promising tool which enables precise identification and quantification of a range of proteins, including proteins related to chronic inflammation. Proteomics can help to characterise the complex biological processes between air pollution exposure and inflammation. Previous studies have shown that individuals with lower SES and ethnic minorities have higher levels of systemic inflammation; therefore, inflammatory pathways are likely an important mechanism for socioeconomic inequalities in the association between air pollution and cardiometabolic health.
This project aims to study socioeconomic inequalities in the cardiometabolic effects of air pollution across the life course and its potential mechanism via inflammation.
B4631 - Developing and evaluating public involvement guidelines for longitudinal cohort studies - 20/06/2024
There has been very little previous research on the topic of public involvement (PI) in non-clinical research. The applicants work in longitudinal population and epidemiological studies and are aware of the importance and difficulty of including the public in this work, partly because these studies do not focus on a specific medical topic or procedure but collect data on a large variety of illnesses, lifestyles, and risk factors. We are also aware that the PI groups which do exist suffer from selection bias, in that the members do not reflect either the participants in observational studies or the background population from which they are drawn. These biases mean that PI groups are not ethnically or socioeconomically diverse and do not equally represent gender groups. This has important implications for the design both of longitudinal studies themselves and secondary epidemiological research using their data if we are to avoid tokenistic involvement and healthy participant bias. Our intention is to involve PI groups in all aspects of the design and conduct of observational studies and to help us to identify future research questions. An appropriate PPI groups could also provide valuable advice on how to recruit and retain certain groups of people.
There is existing evidence (Lang 2022) that although the UK is world leading in including PPI groups in its research, perhaps because of funder stipulations, only 20% of the total number (3000) of studies investigated included PI, and of these ~ only 16% were observational research and ~15% were cohort research. However, this evidence was only drawn from one journal BMJ Open. The potential important benefits of good PI use are well known, but few seem to manage it. Also, PI is seldom if ever evaluated to see what makes a difference to the quality and impact of resulting research. We would like to conduct some research to investigate which methods of recruitment and conduct of PPI are likely to be the most effective. We would then like to start to build capacity in this area and set up some kind of educational package to ensure future proofing.
B4627 - PRECISE Personalised Exposures and Responses for Equitable Policy Action - 29/05/2024
Importance and need Ambient air pollution (AAP) causes 4.2 million premature deaths globally each year. It is a major contributor to non-communicable diseases, second only to cigarette smoking. In early-life, exposure to AAP influences the long-term risk of chronic disease development. Many diseases associated with AAP, such as respiratory illnesses , originate in childhood. Poor and ethnic minority children are disproportionately affected by AAP . Effective and equitable policy interventions targeting children are thus crucial. As a vulnerable group unable to control their exposures, children need to be considered and protected in policy transitions to clean air and net-zero.
Advancing current understandings and practice To tackle the inequitable health burden of AAP, we need to advance our understanding of where early-life exposures occur and how different children may be exposed differently and/or respond differently to the same exposures. This advanced understanding needs to be incorporated into decision-support tools, most notably health impact assessments (HIA), which can then assess equity impacts of clean air and net-zero transitions. I propose building a holistic program centred on the integration of multidisciplinary data, methods, tools, and networks. This integration will enable me to innovatively capture childhood exposure to AAP, estimate novel associations with chronic disease development, create and implement an equity oriented HIA, and foster enduring strategic coalitions and partnerships. The innovation in the exposure assessment can uncover fundamental insights into exposure disparities and health effects of AAP. The equity oriented HIA tool can have transformative impact on practice and policymaking. And creating a nucleus of diverse and engaged stakeholders can amplify the program’s impact. My approach will pave the way for addressing other complex and inequitable environmental health challenges.
Timeliness and trends I have been researching AAP and its health effects, primarily in children, over the past decade. The challenge of AAP is enduring. Whilst overall AAP levels have declined in some countries including the UK, levels are still considered too high to protect human health remaining above World Health Organisation (WHO) guidelines. Net-zero policies, such vehicles electrification, are expected to reduce AAP. However, these reductions will not be enough; tempered by a large, projected increase in future demand for transport leading to potential increases in non-exhaust emissions .
General AAP reductions also mask environmental injustice where there has been no progress in reducing the exposure gap between socioeconomic and racial groups . In the UK, the exposure gap between the poor and rich even increased in what has been cited as a failure of UK air quality policy . This failure is evident at locations important for children’s health. UK schools with high annual particulate matter less than 2.5 micrometres in diameter (PM2.5) levels (>12 μgm-3) had a significantly higher intake of pupils on free school meals (17.8%) and ethnic minorities (78.3%) compared to schools with low PM2.5 (<6 μgm-3, 6.5% on free school and 6.8% ethnic minorities) . Children spend about 30% of their time in schools . Commuting to school is another major contributor to exposure that is understudied. For example, AAP during commuting was 52% higher than exposures at school on average . Commuting mode and routes dictate exposures and vary between socioeconomic and racial groups complicating the understanding of equity impacts of e.g., transport policies targeting travel to school.
There is also sporadic evidence that the most exposed children might respond differently to their AAP exposures. This can be due to higher individual susceptibility or complex interactions with environmental, lifestyle and social characteristics. For example, despite controlling for a comprehensive set of confounders, I consistently observed larger associations between AAP and asthma and wheeze in children from families who struggled financially and children from Pakistani origins in Bradford, UK. So far, I do not have a satisfactory explanation of such differences but an indication of slightly higher exposure variability in the Pakistani but not the financially strained children. The question as to whether certain children respond differently to their exposures remains challenging to answer via traditional epidemiological studies which predominantly rely on a naïve assessment of exposure at the residential address only. Such studies are the norm and incapable of accurately representing exposure variability.
Impact Advancing current understandings of where exposures occur, how exposures vary across different children, and how different children might react differently to AAP has significant implications for policymaking. It can pinpoint which environments policies need to target to be most effective (e.g., at schools, on the route to school) and reveal any differential impact of policies on subgroups who may need more prioritization through a stratified approach to prevention (e.g., ethnic minorities).
But advancing understandings without a holistic approach to drive impact will not be enough. New knowledge needs translation into a new generation of equity oriented HIA, a key aspect of my program. I will use the HIA to test various clean air and net-zero policies solicited from and designed with stakeholders, focusing on climate policies which represent pathways in motion that can reduce both pollutant and greenhouse gas emissions. This focus strategically aligns with current national and global agendas on, and large investments in, net-zero and can reorient policy to better reduce inequities. As equity is also political and multi-sectoral, I acknowledge that my vision of reducing inequity extends well beyond the provision of new scientific information or adept decision-support tools. Actively engaging with policymakers and clustering influential partners to champion children’s health, prioritize equity and uptake novel science and tools is essential and at the heart of my program.
B4625 - Maternal postnatal stress and epigenetic pathways to childhood growth - 29/05/2024
A consensus of research has demonstrated that stress and adversity can become embodied and transmitted across generations, creating pathways by which social and economic inequality can affect human biology and health for decades. Most research has identified fetal development as a sensitive period for this transmission of stress from mother to child, with considerably less research on the postnatal period. Maternal postnatal stress has been found to shape infant stress response development, potentially creating a pathway by which maternal stress can become embodied in the next generation and influence how the next generation responds to and handles stressors. However, it is not clear how these effects on the stress response become embodied and whether these changes persist through childhood. This study proposes to test whether maternal postnatal stress in her child’s infancy and toddlerhood is related to the child’s methylation of stress-response related genes at age 7.
Similarly, previous research has demonstrated a relationship between psychosocial stress and childhood growth in weight and height. However, this relationship has been inconsistently demonstrated and the pathways by which stress affects growth are not clear. While the hypothalamic-pituitary-adrenal (HPA) axis has been implicated in this relationship, results have been inconsistent. This research project proposes to test the relationship between growth velocity throughout childhood and methylation of HPA-axis related genes at age 7, in order to determine whether alterations to stress response physiology are a mechanism by which stress can affect growth.
B4626 - Social Mechanisms of Genetic Effects - 31/05/2024
Today, it is widely accepted that most traits are both genetically heritable and affected by the environment. In the social sciences, the previous nature-nurture debate has been replaced by a new paradigm analyzing the interplay between genetics and the social environment (e.g., in sociology: Breinholt and Conley 2023; in economics: Houmark, Ronda, and Rosholm 2024; in psychology: Wertz et al. 2020). Rooted in sociology, this project analyzes how social mechanisms of genetic effects play out in three realms affecting childhood educational performance: family, daycare, and school peers, and asks how knowledge on these social mechanisms of genetic effects changes theories of justice on social stratification. The project thereby advances knowledge on the complex interplay between the social environment and genetics and addresses ethical questions re-actualized by the integration of molecular genetics in the social sciences. Addressing these issues will promote well-being of children.
B4445 - Sex differences in the longitudinal impact of birth weight phenotype-genotype mismatch in behaviour - 28/05/2024
Fetal growth and biological sex are thought to affect behaviour in childhood and adolescence. Fetal growth is often estimated with birthweight, however, birthweight can vary both as a consequence of genetic and environmental factors and furthermore a large literature has suggested that the effects of fetal growth may differ between males and females. We want to test how measured birthweight and birthweight-genetics influence lasting behaviour in males and females and if a mismatch between an individuals potential for birthweight - i.e. their genetically determined birthweight - and their actual birthweight, produces lasting behavioral changes throughout their childhood and adolescence. Finally, we will test if the effects of such a mismatch differs between males and females.
B4624 - Investigating the effects of maternal physical activity on pregnancy and perinatal outcomes an integration of multiple lines of - 24/05/2024
• The experience of pregnancy is associated with physiological and psychological change that is shown to promote sedentary behaviour and/or lower levels of physical activity (PA).
• PA in pregnancy has historically been deemed a risk factor for miscarriage, though this may result from reverse causality. Those feeling well enough to stay active early in pregnancy might already be in the early stages of miscarriage and thus experience fewer symptoms like nausea and fatigue. The perception of Pa as a risk may have led to the promotion of sedentary behaviour and reduced PA during pregnancy by clinicians and medical professionals in fear of causing harm.
• The majority of epidemiological analyses to-date, however, have reported that higher PA and reduced sedentary time are associated with improved health outcomes for pregnant people and their offspring. Furthermore, guidelines in several countries encourage safe levels of activity and exercise during pregnancy.
• Since PA in pregnancy may have benefits for the mother and/or offspring, it is important to better understand its effects in pregnancy on a range of pregnancy and perinatal outcomes.
• When conducting conventional multivariable regression analyses, sources of bias induced by confounding factors, including confounding by undiagnosed existing disease (reverse causation), present challenges when inferring causality.
• Mendelian randomisation (MR) exploits the random distribution of genetic variants from parents to offspring, independent of the influence from other traits, to reduce susceptibility to these confounding factors. However, MR may be biased by weak instruments or horizontal pleiotropy.
• Negative control designs, which use paternal exposures as the negative control, can reveal bias in associations of maternal exposures with adverse pregnancy and perinatal outcomes. The paternal exposure is unlikely to affect these outcomes but may be associated with unmeasured confounders in a similar way to the maternal exposure.
• Employing a triangulation approach using multivariable regression, Mendelian randomisation, and a paternal negative control design, this investigation seeks to explore the causal effects of PA in pregnancy on pregnancy and perinatal outcomes.
B4623 - Early years telomere dynamics - 31/05/2024
elomeres are structures at the ends of chromosomes, as cells divide, and as people age, they become progressively shorter. The length of telomeres is associated with a range of diseases including cardiovascular and cancer. People start adulthood with a broad range of telomere lengths and this length variation contributes to people’s individual risk of disease. Telomere length variation is partly genetically determined but may also be influenced by early life. We want to utilise the ALSPAC cohort to examine the dynamics of telomeres during life, by undertaking serial telomere length analysis of individuals from birth to 17 years old. We will use a method called HT-STELA that combines a low error rate with high throughput and is provided as a clinically validated diagnostic service for the NHS by TeloNostiX Ltd.
The purpose of this pilot study is to test the utility of HT-STELA in analysing genomic DNA samples from the ALSPAC cohort that have been extracted with different methodologies. By analysing a panel of serial samples, we aim to generate preliminary data that will be used in a funding application to undertake a larger study. An additional aspect of this pilot project is that the data generated will be useful to define the normal telomere length range in the younger population to improve the use of HT-STELA in clinical diagnostics.
B4622 - Identification of rare genetic variants associated with lung function using whole-exome and whole-genome sequencing data - 20/05/2024
Lung-function impairment underlies chronic obstructive pulmonary disease (COPD) and predicts mortality. Recently, over a thousand variants in over 500 genes were associated with lung function. Those variants were involved in different cell functions, providing information that brings us closer to understanding the mechanisms underlying lung function and COPD.
In this study, we will investigate a more comprehensive number of variants in genes, with a focus on those that are not that frequent in the population (frequency under 1%), to help identifying variants responsible for lung function impairment.
B4621 - Lifecourse predictors of mental health and obesity stigma data collection and analysis - 20/06/2024
This data collection and analysis in ALSPAC will form part of a larger project on health-related stigma. Following a process of expert consultation to identify the best available measurement tools and explore development of new ones, new data will be collected in ALSPAC measuring different types of stigma related to health. This will support analysis providing new insights on how these can be intervened on.
B4620 - Effects of Maternal Genetic Risk Factors for Polycystic Ovary Syndrome on Birth and Childhood Outcomes in Offspring - 17/05/2024
*Please note this new proposal will re-use the dataset that has been provided for the previous project ID B3581.*
Polycystic ovary syndrome (PCOS) is a major health concern that affects up to 10% of reproductive-aged women and is the leading cause of female infertility. This complex, heterogenous condition is characterized by ovulatory dysfunction and hyperandrogenism and is often associated with metabolic dysregulation and increased risk for adverse birth outcomes. Existing evidence suggests that the androgenic and metabolic features of PCOS can be passed down from mothers to their offspring, but the relative contributions of maternal genetics and intrauterine environmental factors to these features in offspring are not known.
Our original project ID B3581 studies metabolic and growth and developmental phenotypes in children that may be associated with PCOS. We have recently identified that a higher polygenic risk score (PRS) for PCOS is associated with higher BMI, fat-mass index, and risk of obesity in childhood and earlier age at pubarche and younger age at peak height velocity. These associations persisted after controlling for the maternal PCOS polygenic risk score, indicating that genetic risk for PCOS has direct effects in offspring. In addition, genetic risk for PCOS could also have indirect effects in children through direct effects on the intrauterine environment in their mothers. For example, mothers with PCOS have an increased risk of preterm delivery, attributed to metabolic perinatal complications, such as pre-eclampsia.
I hypothesize that maternal PCOS genetic factors and associated intrauterine environmental factors play an integral role in the development of adverse birth outcomes and childhood androgenic and metabolic features of PCOS in offspring.
B4616 - Adverse childhood experiences and oral health - 16/05/2024
Oral health inequalities start early in life. Previous studies have looked at childhood socioeconomic circumstances, the early family environment and parental behaviours in relation to child oral health. This project will focus on another important social determinant of health. Adverse childhood experiences (ACEs), such as physical abuse, emotional neglect, parental separation or imprisonment, can increase the risk of psychological problems and behavioural problems, respiratory diseases, diabetes, cardiovascular diseases and gastrointestinal diseases among children and adults.
Previous studies in dentistry have shown that ACEs are associated with childhood tooth decay, poor child oral health and lower oral health-related quality of life. ACEs have also been related to fewer dental visits and more tooth extractions in adults as well as poor oral health and greater tooth loss in older adults. Common limitations of previous studies are the use of cross-sectional data and the retrospective assessment of ACEs that introduces measurement bias. In addition, in most studies, different ACEs were combined into broad categories, thereby making it difficult to evaluate the effects of individual ACEs. Identifying which ACEs are more relevant to child oral health, their specific timing and potential underlying mechanisms can inform relevant policy and interventions at family level. Evidence from longitudinal studies will shed some lights on this important research area.
B4615 - Whole-exome sequencing as a tool to reveal rare genetic architecture of diabetes - 16/05/2024
People with diabetes taking insulin sometimes present resistance or failure to this therapy. Investigating the genetic factors influencing the resistance to insulin in people with diabetes may lead to biological insights into the causes of failure to this therapy and help improving their long-term health.
We will look into the DNA of ALSPAC participants that codes the proteins, to identify rare variants (those with a frequency <0.1%) that have a high impact on the structure and/or function of the protein. Then we will investigate if those variants have an influence on the risk of diabetes, and if they have an impact on the levels of diabetes-related traits, as insulin, glucose, etc.