Not long ago, we learned the extent to which adverse childhood experiences (ACE) lead to long-term physical and psychological health problems (Felitti et al., 1998). In the last two-and-a-half decades, there have been continuing developments in the research of why and how adverse childhood experiences lead to death and illness in adulthood. Now, thanks to current research, we have a better understanding of why and how adverse childhood experiences increase morbidity. Inflammation is increased in those with adverse childhood experiences (Rasmussen et al., 2020). Chronic inflammation increases the risk of developing cardiovascular disease, cancer, diabetes mellitus, autoimmune, and many other health concerns (Furman et al., 2019). Although researchers have investigated this issue, the topic has not been explored in this way: Despite knowing that ACE increases health concerns through inflammation, there is very little research regarding variables that promote resiliency of immune health. Additionally, there is minimal research that confronts the specific trauma experienced by those with childhood sexual abuse (CSA). The specific research problem that will be addressed through this study is that we do not know whether and to what extent environmental factors are associated with healthier immune function among survivors of CSA.

From a psychoneuroimmunological foundation, a collection of variables among survivors will be analyzed as potential protective factors. These variables include ease to talk about problems with parents, feelings of closeness to parents, religiosity, involvement in sports or other after-school activities, religiosity, and feeling close to someone. Then, various inflammatory biomarkers will be analyzed and a relationship between factors and biomarkers will be explored.

Are non-parental caregivers important for children and young people’s wellbeing, even in societies with strong nuclear family and intensive parenting norms? This mixed-method project uses the “Children of the 90s” cohort study to investigate the role of alloparents (non-parental caregivers) in England, examining the biosocial pathways between different forms of local childrearing systems and adolescent outcomes.

CONTEXT: Western family structures are often described as nuclear, and in the UK, this is coupled with intensive parenting norms. Childrearing is seen as a private matter, and parents (particularly mothers) are predominantly viewed as being responsible for raising children. From an evolutionary anthropological perspective, this way of raising children is highly unusual: anthropological studies from across populations show that non-parental caregivers (alloparents) are ubiquitous and crucial contributors to childcare, although who helps and how they help vary. Humans have therefore been hypothesised to have evolved a unique system of “cooperative childrearing,” co-evolving with an extended period of dependence through childhood and adolescence. In essence, it takes a village to raise a child.

CURRENT CHALLENGE: Despite intensive parenting norms, families in the UK exist within varied and complex systems of support. However, while evolutionary theory points to the importance of non-parental caregivers, much of our knowledge around raising children centre on parenting with particular focus on early years. There is limited focus on alloparenting, and few studies investigate the impact of alloparental care in middle childhood despite the reliance on continued after-school/weekend childcare for many families. It is therefore unclear how families exist within local systems of childrearing, and how these systems impact children and young people’s health and wellbeing. A comprehensive understanding of the wider childrearing system is crucial to design effective policy and practice impacting parents, children, and young people.

PROJECT AIMS: This project extends the focus of childrearing from parenting to incorporate alloparenting, building a comprehensive understanding of childrearing systems in middle childhood and their pathways to adolescent wellbeing in England (UK).
Specifically, this project aims to (1) identify and classify the different typologies of childrearing systems beyond parenting within England, and (2) investigate the biosocial pathways between alloparenting, markers of stress, and adolescent outcomes including affect (anxiety/depression), socio-emotional development, and health-related risky behaviours. We use data from Avon Longitudinal Study of Parents and Children (“Children of the 90s”) which uniquely holds detailed data on alloparenting during middle childhood (age 6-12), together with biomarkers of stress/inflammation (cortisol, c-reactive protein, interleukin-6). We apply an innovative combination of quantitative and qualitative methods by quantitatively identifying typologies of caregiving (latent class analysis), deepening our understanding of these typologies by using the longitudinal data to constructing life history case studies, then test the hypothesised causal pathways through structural equation modelling.

PROJECT BENEFITS: By extending the focus of caregiving to incorporate alloparents and taking an innovative mixed-method approach, this project contributes to an in-depth understanding of middle-childhood caregiving systems and their impact on young people within a parent-focused culture; and, in doing so, we improve our understanding of human childrearing systems more broadly. Overall, this project will: improve cross-disciplinary knowledge around optimal childrearing practices in middle childhood; contribute to methodological development by applying a novel combination of mixed methods to longitudinal cohort data; and contribute knowledge towards effective policy and practice development for children and families in England and beyond.

DNA methylation (DNAm) plays a central role in gene regulation. However, it is unknown how DNAm patterns change. For example, through genetic factors or physiological states.
Longitudinal birth cohort studies such as ALSPAC provide an unique opportunity to study DNAm patterns over time and to link it to varying physiological states. Quantitative traits comprising your physiological state (such as BMI, glucose and inflammation levels) have varying patterns over time. Similarly eczema and asthma have varying disease patterns over time. Identifying changes in DNAm preceding a change in physiological state or a disease status may lead to identification of a marker that predicts disease outcome.(1)
Multiple studies have identified genetic variants associated with DNAm (mQTL: methylation quantitative trait locus) by combining genome wide genotype information with DNAm levels.(2) The Genetics of DNA methylation Consortium brought together a large number of cohorts to identify mQTLs in blood and investigated whether the mQTLs play a role in disease etiology.(3) Modelling DNAm trajectories with genetic variation could improve our understanding of biological mechanisms.

1. Chen R, Xia L, Tu K, Duan M, Kukurba K, Li-Pook-Than J, et al. Longitudinal personal DNA methylome dynamics in a human with a chronic condition. Nat Med. 2018;24(12):1930-9.
2. Gaunt TR, Shihab HA, Hemani G, Min JL, Woodward G, Lyttleton O, et al. Systematic identification of genetic influences on methylation across the human life course. Genome Biol. 2016;17:61.
3. Min JL, Hemani G, Hannon E, Dekkers KF, Castillo-Fernandez J, Luijk R, et al. Genomic and phenotypic insights from an atlas of genetic effects on DNA methylation. Nat Genet. 2021;53(9):1311-21.

Resilience is known to be the process and outcome of successfully adapting to difficult or challenging life experiences. Promoting resilience is helpful to minimizing the detrimental impact of life stressors which may be unavoidable at times. While interventions aiming to enhance resilience are increasing among different age groups, there remains gaps in our understanding of how and when resilience manifest, as well as the role of negative and positive emotions in this process. This project aims to use intergenerational data from ALSPAC to investigate predictors of the trajectories of resilient behavior, and connections between maternal resilience and offspring resilience from the prenatal stages through childhood years. This includes identifying time and environmental predictors that can be useful in designing future interventions to assist individuals who are at risk in coping with stress and difficult situations.

There is a lot of variability in lung structure among healthy adults. This variability in lung structure is thought to arise during growth - a concept that is referred to as “dysanapsis” (from the Greek, dys=unequal and anaptixy = growth). Dysanapsis is strongly associated with lung disease and death later in life, but the origins of dysanapsis are poorly understood. A recent genetic investigation identified several variants associated with dysanapsis, but when dysanapsis genetic risk manifests in childhood and whether it interacts with environmental or social factors to impair lung function is unknown. This study has two objectives: i) describe the relationship between dysanapsis genetic risk and lung function at various timepoints during lung growth; ii) test whether environmental exposures (environmental tobacco smoke) or social deprivation modify these relationships. No new measurements or samples are required for this study.

Heavy menstrual bleeding (HMB) and menstrual pain (MP) can have a significant negative impact on financial, social, physical and mental wellbeing. Yet people often present late and their symptoms are dismissed. This study will reveal who is at risk of these problematic menstrual symptoms, when they are experienced throughout the lifecourse, and how they might affect depressive symptoms. The findings will inform the prediction of HMB and MP to ensure appropriate management, as well as new ways to predict, prevent, and treat adverse effects of these problematic menstrual symptoms on mental health.

Approximately 10-20% of children and adolescents experience socio-emotional difficulties severe enough to merit a diagnosis of a mental health disorder. More than 40% of these youth develop at least one other mental illness throughout their life. A developmental perspective that investigates the interrelations between different domains of socio-emotional development from early life to adulthood can offer important insights into why socio-emotional difficulties commonly co-occur. Using state-of-the-art longitudinal statistical techniques, this project aims to significantly advance our understanding of the mechanisms underlying co-occurring socio-emotional difficulties. It will illuminate the roles of both genetics and psychosocial factors in linking different socio-emotional difficulties together using robust study designs that consider a range of confounders and providing the best available evidence yet on the causal mechanisms underlying the co-occurrence of socio-emotional difficulties. As well as informing preventions and interventions, this will contribute to better, more comprehensive theories of the developmental roots of mental health.

Urinary incontinence (UI), defined as the complaint of any involuntary leakage of urine is a highly prevalent condition that can have adverse consequences for emotional well-being and quality of life in addition to being of economic importance to health services.
The cause of UI is not completely understood and includes psychological and physiological factors outside the lower urinary tract. The hypersensitivity of the bladder in urinary incontinence has guided researchers to consider psychological factors including anxiety and depression that may be of importance.
The comorbidity between UI and affective disorders including anxiety and depression is well established, but the precise nature of this relationship is unknown. Much of the existing research examining the relationship between UI and anxiety/depression is cross-sectional and is therefore unable to disentangle the temporal relationship between whether poor mental health is a cause or a consequence of UI.
The use of bidirectional MR can help to differentiate causality from correlation by testing the causal effects independently in each direction using single nucleotide polymorphisms (SNPs) found to be robustly associated with each trait in different genome-wide association studies (GWAS).  We will use GWAS summary statistics in a two-sample MR analysis to examine bidirectional causal relationships between anxiety/depression/neuroticism and UI in females. Two subtypes of UI will be explored. Stress urinary incontinence (SUI) is defined as a loss of urine associated with physical exertion, coughing or sneezing whilst urgency urinary incontinence (UUI) is loss of urine associated with a sudden compelling need (an urgency) to void.

Muscle strength and cognitive function are partially driven by genes inherited from parents. Reduction in muscle strength and cognitive function is associated with multiple adverse health outcomes including disability and mortality. Previous studies identified genes commonly associated with muscle strength and cognitive performance. However, impacts of genetic determinants of muscle strength and cognitive function on physical fitness and mental health longitudinally have not been fully studied mainly due to data unavailability. ALSPAC (Avon Longitudinal Study of Parents and Children) has collected physical fitness (hand grip strength, body DXA scan) and mental health (depression, anxiety, life events, etc.) data from mothers and children longitudinally, along with genetic data. Our aim is to leverage this dataset to better understand how genetic predispositions to muscle strength and cognitive performance contribute to physical fitness and mental health over time.

Reduction in physical fitness and motor function is associated with accelerated aging reflected by changes in DNA methylation, another heritable mark that can be modified by behavioral and environmental factors. Associations of DNA methylation with longitudinal physical fitness and mental health have not been fully understood. Using data from the ALSPAC, we plan to study the longitudinal association of physical fitness and mental health with DNA methylation throughout the genome. Furthermore, we plan to evaluate the biochemical effects of genes and/or DNA methylation marks associated with longitudinal physical fitness and mental health, by studying their associations with levels of different biochemicals (called ‘metabolites’) in child and mother’s blood samples using the metabolomics data in ALSPAC.