34 research outputs found
Neurodevelopmental outcomes in individuals with fetal alcohol spectrum disorder (FASD) with and without exposure to neglect : clinical cohort data from a national FASD diagnostic clinic
Disentangling the relative developmental impact of prenatal alcohol exposure from postnatal
neglect is clinically valuable for informing future service provision. In this study developmental
outcomes across groups are compared in a ânatural experimentâ.
Methods: Clinical data from 99 persons with fetal alcohol spectrum disorder (FASD) diagnoses were
audited. Developmental outcomes (diagnosis of attention deficit hyperactivity disorder, ADHD; social
and communication disorder, SCD; or autism spectrum disorder, ASD; Short Sensory Profile, SSP;
Vineland II Adaptive Behaviour Scales) were compared across two exposure groups: prenatal alcohol
only; and mixed prenatal alcohol and neglect.
Results: ADHD (74%) and ASD/SCD (68%) were common, with no significant difference between
groups (ADHD, P=0.924; ASD, P=0.742). Vineland age equivalence scores were lower than
chronological age (11.1yâprenatal alcohol onlyâand 12.7yâneglect) across all domains, especially
receptive language (3.7y for both groups). Age equivalence did not differ between groups, with the
exception of domestic daily living (neglect: 7.7y vs prenatal alcohol only: 5.8y, P=0.027). A
probable/definite difference on SSP was more common in the prenatal alcohol only (96% vs 67%,
P=0.006). For the individual subscales of SSP, there were no significant differences by neglect
category.
Discussion: Postnatal neglect in this group did not make the developmental outcome any worse,
suggesting that prenatal alcohol influences these outcomes independently. Professionals who
support families looking after a child with both FASD and a history of neglect should be aware that
the behavioural difficulties are likely to be related to prenatal alcohol exposure and not necessarily
reflective of parenting quality
Evaluating the difference in neuropsychological profiles of individuals with FASD based on the number of sentinel facial features: a service evaluation of the FASD UK National Clinic Database
It might be implied that those with Fetal Alcohol Spectrum Disorder (FASD) with fewer sentinel facial features have a âmilderâ neuropsychological presentation, or present with fewer impairments than those with more sentinel facial features. The aim of this service evaluation was to compare the neuropsychological profile of people with FASD with varying numbers of sentinel facial features. (2) A clinical sample of 150 individuals with FASD, aged between 6 and 37 years, completed various standardised assessments as part of their diagnostic profiling. These included the documented level of risk of prenatal alcohol exposure (4-Digit Diagnostic Code), sensory needs (Short Sensory Profile), cognition (Wechsler Intelligence Scale for Childrenâ4th Edition; WISC-IV), and communication and socialisation adaptive behaviours (Vineland Adaptive Behavior Scaleâ2nd Edition; VABS-II). As FASD has high comorbidity rates of Autism Spectrum Disorder (ASD) and Attention Deficit Hyperactivity Disorder (ADHD), these were also reviewed. The profiles of the âFASD with 2 or 3 sentinel facial featuresâ group (n = 41; 28 male, 13 female) were compared with the âFASD with 0 or 1 sentinel facial featuresâ group (n = 109; 50 male, 59 female) using Chi2 tests, independent sample t-tests, and Mann-Whitney U analyses (where appropriate). (3) There were no significant differences between the two comparison groups across any measure included in this service evaluation. (4) Whilst sentinel facial features remain an important aspect in recognising FASD, our service evaluation indicates that there is no significant relationship between the number of sentinel facial features and the neuropsychological profile of people with FASD in terms of severity of presentation
Prevalence of fetal alcohol spectrum disorder in Greater Manchester, UK: An active case ascertainment study
Background: Despite high levels of prenatal alcohol exposure in the UK, evidence on the prevalence of fetal alcohol spectrum disorders (FASD) is lacking. This paper reports on FASD prevalence in a small sample of children in primary school.
Methods: A 2-phase active case ascertainment study was conducted in 3 mainstream primary schools in Greater Manchester, UK. Schools were located in areas that ranged from relatively deprived to relatively affluent. Initial screening of children aged 8â9 years used prespecified criteria for elevated FASD risk (small for age; special educational needs; currently/previously in care; significant social/emotional/mental health symptoms). Screen-positive children were invited for detailed ascertainment of FASD using gold standard measures that included medical history, facial dysmorphology, neurological impairment, executive function, and behavioral difficulties.
Results: Of 220 eligible children, 50 (23%) screened positive and 12% (26/220) proceeded to Phase 2 assessment. Twenty had a developmental disorder, of whom 4 had FASD and 4 were assessed as possible FASD. The crude prevalence rate of FASD in these schools was 1.8% (95% CI: 1.0%, 3.4%) and when including possible cases was 3.6% (2.1%, 6.3%). None of these children had previously been identified with a developmental diagnosis.
Conclusions: FASD was found to be common in these schools and most of these children's needs had not previously been identified. A larger, more definitive study that uses a random sampling technique stratified by deprivation level to select schools is needed to make inferences regarding the population prevalence of FASD
Under-reporting of foetal alcohol spectrum disorders: an analysis of hospital episode statistics
<p>Abstract</p> <p>Background</p> <p>Internationally, 0.97 per 1,000 live births are affected by foetal alcohol syndrome (FAS). However, prevalence intelligence has been limited in the UK, hindering the development of appropriate services. This analysis compares hospital admissions over time, between regions and with alcohol-related admissions for adult females to assess whether established patterns (such as the North experiencing elevated harms) can be identified.</p> <p>Methods</p> <p>A retrospective analysis of hospital admissions data (April 2002 to March 2008) for foetal alcohol spectrum disorder (FASD)-related conditions: foetal alcohol syndrome (dysmorphic) (n = 457); foetus and newborn affected by maternal use of alcohol (n = 157); maternal care for (suspected) damage to foetus from alcohol (n = 285); and 322,161 women admitted due to alcohol-related conditions.</p> <p>Results</p> <p>Whilst the rate of admission for alcohol-related conditions in women aged 15-44 years increased significantly by 41% between 2002/03 and 2007/08 (p < 0.0001), no such increases were seen in the numbers of FASD-related conditions (all p < 0.05). Established regional rates of admission for alcohol-related conditions in women aged 15-44 years old were not associated with admission for FASD-related conditions.</p> <p>Conclusions</p> <p>It would be expected that the North West and North East regions, known to have higher levels of alcohol harm would have higher levels of FASD-related conditions. However, this was not reflected in the incidence of such conditions, suggesting under-reporting. With incomplete datasets, intelligence systems are severely limited, hampering efforts to develop targeted interventions. Improvements to intelligence systems, practitioner awareness and screening are essential in tackling this.</p
Fetal alcohol spectrum disorders: An overview of current evidence and activities in the UK
Estimates for the UK suggest that alcohol consumption during pregnancy and prevalence of fetal alcohol spectrum disorder (FASD) - the most common neurodevelopmental condition - are high. Considering the significant health and social impacts of FASD, there is a public health imperative to prioritise prevention, interventions and support. In this article, we outline the current state of play regarding FASD knowledge and research in the UK, which is characterised by a lack of evidence, a lack of dedicated funding and services, and consequently little policy formulation and strategic direction. We highlight progress made to date, as well as current knowledge and service gaps to propose a way forward for UK research