Abstract of the R21 titled “Investigating DNA methylation changes during pregnancy as a mechanism for altering disease risk in women”

Pregnancy is an important transition period that parous women (those who have given birth) undergo and it is linked to changes in risk of various diseases as compared to nulliparous women (those who have never given birth). The number of completed pregnancies changes the risk of autoimmune disease, Alzheimer’s disease, cancers of the ovary, breast and liver, as well as asthma death later in life. However, it is unknown how these disease risks are altered by the child-bearing experience. DNA methylation (DNA-m) - the addition of a methyl group to cytosine in cytosine-phosphate-guanine (CpG) dinucleotides sequences in DNA - has been shown to be associated with multiple health outcomes later in life, such as atopy, eczema, hypertension, diabetes mellitus, and cancer. Our preliminary studies have shown that more CpGs (5.6% vs 0.7%) change levels of methylation during pregnancy (measured between age 18 years and again during pregnancy in women not yet pregnant at age 18) compared to pre-pregnancy (between ages 10 and 18 years), which may represent a plausible mechanism for altering post-pregnancy disease risks in parous women if these changes remain after pregnancy. To better understand the links between methylation changes during pregnancy and parous-related diseases later in life, we propose to identify pregnancy-related CpGs with significant pre- and post-pregnancy methylation changes through an epigenome-wide study. In Specific Aim 1, we will identify CpGs with significant methylation changes in parous women between ages 18 and 26-27 years compared to nulliparous women over the same time period. Then in Specific Aim 2, we will focus on the CpGs identified in Specific Aim 1 and test what proportion of them change from age 18 years to pregnancy and remain stable after parturition up to age 26-27 years. This proposed research has the potential to significantly contribute to 1) the discovery of biomarkers affected by a healthy pregnancy, 2) a better assessment of the long-term effects of parity on women in later life, and 3) the future development of epigenetic tools to detect these modified disease risks. Our collaborative research team is well-positioned to do this work with complementary expertise in genetics and epigenetics, reproductive epidemiology and (bio)statistics, and clinical medicine. We have a long track record of successful collaboration investigating DNA methylation changes during critical transition periods,
such as puberty and pregnancy.

The current project is a student project linked to the already approved project: B3840 Developmental pathways to mental health
problems.

Prosocial behaviour and inhibitory control are essential components of social competence and self-regulation, respectively, and both are considered important in child development, and in preventing behavioural problems in children and adolescence. Current knowledge about the developmental relationships between prosocial behaviour and inhibitory control is however limited. In light of the existing literature, a deeper understanding of the developmental relations between prosocial behaviour and inhibitory control may have implications for interventions aimed at preventing problem behaviour in children.

Loneliness is a deeply troubling experience of feeling unwanted by, excluded from and/or unworthy of the social companionship a person desires. Our concern relating to loneliness is part of a global concern for the strong mental health of adolescents which addresses to how young people experience life as they shift from childhood to adulthood, a turbulent time in their development. Our proposed research aims to use an innovative interdisciplinary mixed-methods approach to help grow the evidence base on how loneliness drives poor mental health in order to design new solutions that most effectively nurture the relationships that sustain people.

This project aims to understand how access to green space in pregnancy, infancy and early childhood impacts subsequent child cardiometabolic health (BMI/obesity and blood pressure). Although research is mixed, there is some evidence that access to green space may be associated with lower childhood BMI/obesity and blood pressure (Luo et al., 2020; Markevych et al., 2014). As childhood BMI and blood pressure predict these traits in adulthood, and that these are key risk factors for cardiovascular disease, child cardiometabolic health is a serious public health concern; if access to green space can lower BMI and blood pressure, this may constitute a potentially modifiable public health intervention.

We will use a structured life course approach to answer this question, which is able to distinguish between different life course trajectories, such as critical periods, sensitive periods, accumulation of risk, and others (Smith et al., 2016; Ben-Shlomo & Kuh, 2002). We will use repeated data on access to green space to explore if and how this is related to child cardiometabolic health in ALSPAC children. In addition, this project will explore whether there is an interaction between socioeconomic position and access to green space in shaping these outcomes. These analyses will also be replicated in an independent UK cohort (Born in Bradford; BiB)

References:
Ben-Shlomo, Y. & Kuh, D. (2002). What is a Life Course Approach to Chronic Disease Epidemiology? Conceptual Models in Life Course Epidemiology. Int. J. Epidemiol., 31, 285–293.
Luo, Y.N., Huang, W.Z., Liu, X.X., Markevych, I., Bloom, M.S., Zhao, T., et al. (2020). Greenspace with overweight and obesity: A systematic review and meta-analysis of epidemiological studies up to 2020. Obes. Rev., 21, 1–28.
Markevych, I., Thiering, E., Fuertes, E., Sugiri, D., Berdel, D., Koletzko, S., et al. (2014). A cross-sectional analysis of the effects of residential greenness on blood pressure in 10-year old children: Results from the GINIplus and LISAplus studies. BMC Public Health, 14, 1–11.
Smith, A.D.A.C., Hardy, R., Heron, J., Joinson, C.J., Lawlor, D.A., Macdonald-Wallis, C., et al. (2016). A structured approach to hypotheses involving continuous exposures over the life course. Int. J. Epidemiol., 45, 1271–1279.

Cognitive dysfunction is proposed to be a feature and risk factor for depression. Evidence from observational and experimental studies suggest a role of low-grade systemic inflammation in depression, which could also be relevant for cognitive dysfunction. Existing cross-sectional studies suggest that inflammation is associated with cognitive dysfunction, particularly poor memory, processing speed, executive function and emotional bias. Limited longitudinal evidence, often based on the elderly population, also suggest a potential link between inflammation and impaired learning, memory, attention, and general cognitive functioning and decline. While these studies point to a potential role of inflammation in cognition, there are key unanswered questions.

First, much of the existing evidence around inflammation and cognition is based on the elderly population, so it is unclear whether inflammation is associated with cognition earlier in the life course. Second, it is unclear whether inflammation plays a causal role in cognitive dysfunction, as cytokine elevation could alternatively be a consequence of cognitive impairment (i.e., reverse causality) or due to confounding. I propose to address these issues using epidemiological approaches.

Our project aims to estimate the prevalence and distribution, in terms of geography and socioeconomic status, of lead exposure in England and its costs in terms of children’s wellbeing and development. While scholars and practitioners believe lead exposure to be widespread in England, a dearth of data on this issue has so far hindered policymaking. This proposal seeks funding for the initial project stage - a secondary data analysis, building on international evidence to project exposure burden in England, based on the existing data and the piloting of surveys to collect primary data to map exposure sources and prevalence.

ALSPAC collected samples at the 24 year clinic to preserve RNA. This can be used to look at which genes are being expressed in blood. We are hoping to obtain money to analyse some of these samples by a process called RNA sequencing. This will allow us to see which genes are switched on in different people. The data generated will create a resource for molecular research.

Across the developed world, employment has declined in middle-wage "routine" jobs and increased strongly in jobs requiring a degree. Recent evidence from the U.S. and Sweden indicates this change is associated with an increase in the demand for jobs requiring social skills. Over the last 30 years the UK labour market has witnessed a well-documented increase in the supply of graduates while the occupational structure has shifted towards managerial jobs. However, there is no strong evidence as yet that these changes have benefitted workers with higher social abilities.

In this project we will investigate the labour market returns to social skills in the context of the UK. Thanks to the availability of long-running cohort studies, the UK offers an opportunity to examine unique data on individual’s characteristics, such as cognitive, socio-emotional, and physical abilities. ALSPAC is particularly suitable to our purposes as it collects detailed information on these abilities.

The changing labour market is at the centre of some of the most important social policy debates worldwide, especially those focused on the effect of artificial intelligence on the demand for different types of skills. We will contribute to these debates by providing novel evidence of the relationship between different types of skills and labour market outcomes.

In this project we plan to use longitudinal observational data and human genetics to examine the relationship between leptin and anorexia nervosa

Leptin is a hormone with pleiotropic functions that affect several tissues in animal and human subjects (Hebebrand, 2006) and is shown to be involved in eating behaviour (Farooqi, 2007). Several symptoms in individuals with anorexia nervosa have been reported to be related to low leptin levels (Hebebrand, 2006) and a recent MR investigation found that a low endogenous leptin synthesis represented a risk factor for developing anorexia nervosa (Peters, 2021). Whether this association is dependent on leptin levels at particular time periods in the lifecourse is yet to be determined. In this project we plan to use longitudinal observational data and human genetics to examine the relationship between leptin in childhood and anorexia nervosa later in the lifecourse.