Our goal is to add a limited number of additional variables to our current data analyses using the ALSPAC data. We currently have information on the level of response to alcohol and demography at age 12-13, know the outcome regarding a limited number of alcohol-related variables at age 14-15, and have models of how the level of response to alcohol relates to alcoholic outcomes in teenagers and adults from several additional studies (the Collaborative Study on Genetics of Alcoholism, the San Diego Prospective Study adults, and the San Diego Prospective Study adolescents). However, to date none of these structural equation models have been tested in subjects in their early teens. Therefore, if several additional areas of data can be made available to us within the next week or so, we will be able to test whether aspects of the structural equation models generated in late teenagers and adults apply to the ALSPAC population using predictors from age 12-13. The published structural equation models have utilized both the MPlus approach and the AMOS programs as described in the references offered below. To carry out these analyses, we would be grateful for any of the following variables.

1. Age 11 (KW file) and age 13 (TA file) for all SDQ scores. Of particular importance are summarizing scores for externalizing and internalizing symptoms. We do not need specific items. The variables we would like include KW6600a to KW6605c. NOTE: I could not locate the SDQ variables for the 13-year clinic (TA file).

2. Stop-Signal (SS Task Score) from the 10-year clinic. Specifically, we need the number of failures for the hard and easy inhibition items. The specific variable names are: FDCM210 to FDCM222 and FDCM230 to FDCM233.

3. Scores for the TEA-CH test of Sky Search, Sky Search Dual Task, and Opposite Worlds Task from the 11-year clinic. These include variables FEAT060 to FEAT065, FEAT141, FEAT146 to FEAT148, FEAT225, FEAT226, FEAT228, FEAT229.

4. Scores from the Counting Span Task at the 10-year clinic. These variables are FDCM110, FDCM111, FDCM130 to FDCM133.

5. The mother's alcohol, nicotine, and cannabinol use at 18 weeks gestation, as well as the alcohol and nicotine use at 32 weeks gestation. It would also be valuable to have the mother's use of heroin, cocaine, amphetamines, or other drugs at 18 weeks gestation. The variable names for these items include B650 to B679, B700 to B714, B720 to B724, B752 to B760, B767 to B769, C361 to C373, C490, C491, C492.

6. From the puberty questionnaire (including Tanner) scores at the 11-year and 13-year clinics. Specific names include PUB407 to PUB497. NOTE: I could not locate the puberty variables for the 13-year clinic.

7. From the Arnett Sensation Seeking data, variables would include: FESS020 to FESS039, FESS050, FESS051.

Specific Aims:

1. To determine the levels of maternal thyroid function tests which result in impaired development of the offspring.

a. To determine the levels of TSH, free thyroxine, thyroglobulin, and thyroid peroxidase antibody in the sera of pregnant women at known times in the pregnancy

b. To compare maternal thyroid function with the neurodevelopment of the child at age 8 years, and determine the association between maternal thyroid levels and specific effects in domains of IQ, attention, behavior, speech and language skills, social cognition, gender behavior, executive function, and manual dexterity in the ALSPAC dataset, controlling for potential confounders such as maternal smoking status and socioeconomic status.

c. To determine which maternal factors (e.g. age, antibody status) and offspring factors (e.g. gender) modify the relationship between trimester-specific thyroid status and development of the offspring.

2. To determine the levels of maternal thyroid function tests which result in fetal demise.

3. To develop trimester-specific normative ranges for thyroid hormone levels during pregnancy, based on the relationship with impaired development and fetal loss.

We propose to examine the following research question:

What aspects of the child's diet are related to bone structure in children either before and/or during puberty (depending on when the measures were made)?

Aspects of the diet will include:

• Overall assessment of the diet using dietary patterns
• Individual nutrients
• Individual foods and food groups
• Longitudinal measures of dietary effects (from prenatal to the current time)

Aspects of the bone structure to be examined will include:

• Bone size (assessed by area of the whole skeleton derived from total body DXA scans, width of the femoral neck derived from DXA scans of the hip, and cross sectional area of the tibia derived from pQCT scans).
• Bone shape (reflected by the ratio of length and width of the humerus based on a novel method we have recently developed19).
• Cortical thickness (based on hip DXA scans and tibial pQCT scans).
• Trabecular bone mass (based on bone mineral density (BMD) of the spine obtained from sub-regional analysis of total body DXA scans).
• Bone strength (reflected by cross sectional moment of inertia derived from hip DXA scans and tibial pQCT scans).

No outline received

The aim of this study is to investigate whether the CCR5 ?32 mutation is associated with immune related phenotypic outcome. It was proposed that abrogation of CCR5 bias the immune system toward a T-helper-2-driven response(Lucotte and Mercier, 1998). As a consequence we hypothesize that the presence of a CCR5?32 mutation is negatively correlated with the incidence of viral childhood infections and positively correlated with atopic disorders. Corresponding phenotypic outcomes will be obtained from the child-based questionnaires completed by a parent at different ages as well as from biological samples (e.g. skin prick test, IgE). Effect modification by environmental exposure will be investigated. The data will be analyzed using established statistical methods for genetic studies, primarily via regression models adjusted for potential confounding factors. Potential population admixture will be allowed for in the analysis.

Genotyping will be done until end of July. Subsequently the analysis will be performed. The results will published in a scientific journal.

No outline received

Objectives:

1. Investigate the association between measures of social cognition and social functioning in the children and PLIKS and whether a particular measure of social cognition is particularly associated with PLIKS

2. Investigate the relationship between social cognition in the parents and these same measures in the children

3. Investigate the relationship between measures of social functioning and PLIKS and how this progresses over time

Social cognition has been the focus of much recent interest and is has been defined by social psychologists as a domain of cognition that involves the perception, interpretation and processing of social information (Ostrum, 1984). Social cognition involves stimuli which are more complex and labile than non- social stimuli. To process a social stimulus, the perceiver must draw upon a larger body of stored information (knowledge, attitudes, biases etc). Furthermore, the relationship between the perceiver and the stimulus is usually interactive. The definition can be broad and a number of abilities such as emotion perception, social perception, social knowledge and attributional bias are included (Brune, 2005). Theory of mind, the cognitive capacity to represent one's own and another person's mental states for instance, in terms of thinking, believing or pretending has also been classified as a social cognitive ability.

There is a great deal of cross-sectional data that finds that people with schizophrenia are much more likely to have deficits in social cognition. However, there are very few longitudinal studies that have been able to investigate such an association. The psychotic like symptoms (PLIKS) measures in ALSPAC provide an opportunity to investigate social cognition in relation to this intermediate outcome.

We propose to use the following measures of social cognition available in ALSPAC:

Emotion recognition - the Diagnostic Analysis of Non Verbal Accuracy (DANVA-2-CF), a test of the recognition of facial emotions through the presentation of photographs of 24 children's facial expressions (12 female and 12 male participants showing an equal number of high and low intensity, happy, sad, angry and fearful faces) (Nowicki & Carton, 1993; Nowicki & Duke, 1994) was completed by the child at aged 8. The test was also completed by the childs parents

Theory of mind/Emotion attribution - A computerized test designed by Blakemore and colleagues (Boraston et al, 2006) was completed by the child aged 13 and the parent. The task consisted of series of short (5s) animations. These featured an "emotional" triangle, interacting with a circle. They were designed to evoke an attribution of emotion to the triangle, which was rated in terms of anger, happiness, sadness or fear from its pattern of movement and how animate ("living") it appeared to be.

Although classical measures of social functioning such as employment fail to apply to this age group, measures of social behaviour are also available in the cohort. These include:

Social communication - the Social and Communication Disorders Checklist (SCDC) (Skuse & Scourfield, 2005) has 12 questions measuring social communication and was completed by the parent with regard to the child at age 8

Social functioning - the number and satisfaction with friends (child rated) and teacher ratings of social interaction at school (available at age 8, 10 and 11).

The overall aim of the Healing Foundation UK Centre for cleft research supported by the VTCT (Vocational Training Charitable Trust) based in Bristol will be to generate important new knowledge to advance our understanding of the causes of cleft lip and/or palate, inform treatment and ultimately improve the lives of children, adolescents and adults born with cleft lip and/or palate.

Aims

We wish to investigate the relationship between JH and chronic musculoskeletal pain and other aspects of musculoskeletal health in ALSPAC as follows:-

1. Relationship between JH and chronic musculoskeletal pain in adolescence.

* Prospective analyses will investigate whether JH, as defined by Beighton score greater than 6 at age 13, is associated with an increased risk of chronic musculoskeletal pain at age 17, as assessed by questionnaire.

* Factors which influence any association between JH and chronic musculoskeletal pain will be explored, such as lower socio-economic status and clumsiness. We would also look at parental JH and chronic pain patterns.

2. Health and social impacts of JH.

* Prospective studies will investigate whether JH at age 13 is associated with adverse health impacts associated with chronic musculoskeletal pain at age 17, as assessed by questionnaire.

* Cross sectional and prospective studies will examine associations between JH at age 13, and physical activity as assessed by accelerometry at age 13 and 15.

3. Relationship between JH and other aspects of musculoskeletal health.

Cross sectional and prospective analyses will determine whether JH at age 13 is related to bone mass as measured by DXA (age 13 and 15) and pQCT (age 15), or to scoliosis (ages 13 and 15).