Genetic variants associated with lung function and susceptibility to airway diseases such as asthma or COPD might be implicated in lung function development from birth to adulthood. Here, we would be able to assess whether very low and low lung function trajectories are primarily associated with asthma, COPD, or lung function genetics, and related mechanisms. Disentangling the genetic factors derived from asthma, COPD, and lung function studies underlying the trajectory of poor pulmonary capacity across the lifespan could contribute to identifying new lung function biomarkers and to early prevent the development of chronic airway diseases. By using a PRS approach, we anticipate having better power to evaluate asthma and COPD mechanisms in lung function trajectories compared to a standard GWAS approach.

Gender-based violence (GBV) is a global public health problem. It is present in all ages and socioeconomic statuses. However, a better understanding of GBV over the life course and the long-term impact of violence exposure on health outcomes is still required. Therefore, the objective of this project is to evaluate and understand gender-based violence over the life course and the many factors involved in this violation of women's and children's human rights. To do this, we will use the ALSPAC cohort study, which include among others a range of both parent and self-reported questions related to gender-based violence, such as data on physical, psychological, and sexual violence occurring during different periods of life. Using this data, it will be possible to estimate (i) cumulative exposure to GBV; (ii) the intergenerational exposure to GBV; (ii) the differences in GBV considering gender, age, education, and income level; and (iv) the impact of violence exposure on health outcomes.

This study will assess how early interventions change the natural course of atopic dermatitis. Data will be collected and analyzed from the Avon Longitudinal Study of Parents and Children (ALSPAC), a population-based birth cohort of 14,000 children from Avon, UK. The project will assess how early use of therapy, including topical and oral agents, changes the disease course of atopic dermatitis from birth to 18 years of age. Several studies in other inflammatory diseases such as Crohn’s and rheumatoid arthritis have established the value of aggressive intervention shortly after symptom onset in producing long-term disease modification. There may be opportunities to observe a similar effect with respect to atopic dermatitis, as well as related diseases of the atopic march. Second, this study will assess the development of major comorbidities including asthma, rhinitis, and food allergy, including severity and time course in the first 18 years of life.

Research has shown that adults who look back on their childhood and say that they had a positive relationship with their parents, or felt loved by their parents, have better mental health. Indeed, these emotional memories can be more important for mental health than memories of specific behaviours that parents engaged in. However, we don’t know how the relationship between feeling loved in childhood and mental health actually comes about.
In this study, we will firstly look at how genetics relates to people saying they felt loved in childhood. People who took part in a large research study answered a question about whether they felt loved in childhood and provided a blood sample, so that we can look at their genetics. Genetic material (DNA) is made up of millions of tiny units called base pairs. At each base pair, a person can have one of two alleles. We will look at whether the allele that a person has at each base pair increases or decreases their likelihood of reporting that they felt loved in childhood. We will then look at whether there are similarities in how genetics contributes to feeling loved in childhood and depression, anxiety, and wellbeing.
This will help us to understand some of the reasons people are more or less likely to say they felt loved in childhood. It can also provide a better understanding of how feeling loved in childhood relates to mental health. All of this is important for how we understand the causes of mental health problems.

Preterm birth, the leading cause of death in children younger than five, is a risk factor for brain-based disorders, asthma, and ischemic heart disease. Lead is a toxic chemical and a known risk factor for preterm birth. Vitamin D may modify this relationship due to its probable antioxidant properties.

In a recent pan-Canadian study examining 1,851 live births from the Maternal-Infant Research on Environmental Chemicals (MIREC) cohort, prenatal exposure to low concentrations of lead increased the risk of preterm birth and spontaneous preterm birth, and the risks were stronger among mothers with insufficient vitamin D levels, suggesting that they might be more susceptible to the toxic effects of lead. However, average blood lead concentrations among mothers were low among a modest sample size, and replication of these findings is warranted.

We aim to estimate the joint association of blood lead and vitamin D with preterm birth the Avon Longitudinal Cohort of Parents and Children.

Information can be obtained from ALSPAC (B number folder) or the UK LLC on request

The placenta is a crucial organ of mammalian pregnancy, connecting mother and fetus. Impaired placentation and placental development and function are associated with common pregnancy complications including preeclmapsia, fetal growth restriction and preterm delivery.
Here we will investigate associations between placental weight, dimensions and number of cotyledons and pregnancy outcomes as well as the long term health of both mothers and their offspring. We will also use the genetic data in order to identify determinants of the placental traits.

The primary objective of the Intergenerational Cohort Consortium (ICC) is to maximise the value of some of the most mature multi-generational data to complete a series of analyses (and associated publications) providing new insights into intergenerational pathways that connect parental life histories, from infancy to parenthood, to offspring psychosocial development decades later. Key outcomes include parent psychosocial adjustment and caregiving behaviour, and offspring psychosocial development. The aim is to identify modifiable factors that act to break intergenerational cycles of disadvantage and strengthen families from one generation to the next.

Planned analyses will specifically address questions about intergenerational transmission that cannot be answered in any one cohort. These include questions about the reproducibility and generalisability of findings reported from single studies; questions about intergenerational effects of low prevalence exposures (e.g., histories of illicit drug use and self-harm), and; questions which require contributions from different cohorts to provide a more complete picture of development processes (e.g., piecing together positive pathways from childhood to young adulthood).

Further information can be found in our ICC profile paper:
https://doi.org/10.1332/175795920X15792720930280

The ICC is a consortium within our broader LifeCourse initiative:
https://lifecourse.melbournechildrens.com/
https://doi.org/10.1093/ije/dyac086

Please see associated paperwork in relevant B number folder