Abstract

The highest rates of fetal alcohol syndrome (FAS) in the world have been found in South Africa (SA) in this town targeted for prevention research. Rates of FAS were 46 and 75 per 1,000 in waves I and II of research and a preliminary rate in Wave III is 79. A high prevalence of FAS exists in other parts of SA. Prevention research has broad implications for programs in SA, the US, and developing populations. This is a multi-site, efficacy trial of a comprehensive, public health model, community-wide, FAS prevention program defined by the Institute of Medicine (IOM). It utilizes both comparative community and pre/post prevention designs with assessment via rigorous diagnosis of FAS in children and infants and also change in measures from a random sample drinking practices survey. Rigorous program evaluation will also assess specific indicated, selected, and universal prevention techniques applied by indigenous workers. The prevention site (urban and rural components) is matched with four comparison communities which will be analyzed in aggregate and as distinct entities to assess confounding influences. Utilizing lOM-recommended techniques of research and prevention applied previously in American Indian communities, this study will determine the efficacy of community-wide prevention of FAS in SA, and which specific components are most viable. Nested studies within the prevention design also address basic research for further specificity of epidemiologic and clinical characteristics of: FAS, adult drinking, and maternal risk factors for FAS.
Specific aims are to: 1.) assess the efficacy of the IOM, FAS prevention program;2.) directly measure the prevention efficacy of the epidemiology """"""""research only"""""""" phase via change in age-specific FAS rates;3.) measure change in adult knowledge, attitudes, beliefs, and drinking behavior (KABB) as well as community readiness for change;4.) link the level of participation in prevention activities to specific outcomes through process evaluation;5.) further define maternal risk factors for FAS;and 6.) explore basic issues of risk and protection via nested studies. An extensive multivariate data analysis plan is provided for each aim. Prevention is implemented by: seven on-site prevention personnel, University of Cape Town-based staff, and U.S. and SA investigators/trainers. In indicated prevention, maternal risk is reduced via: case management of high risk individuals, access to birth control, and enhanced nutrition;brief interventions using principles of motivational interviewing and community reinforcement approach;and individual empowerment/skills building. Selective and universal prevention use: screening for alcohol abuse;targeted messages to change norms and KABB;policy advocacy;and community education and dialogue.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01AA015134-04
Application #
7683869
Study Section
Community-Level Health Promotion Study Section (CLHP)
Program Officer
Scott, Marcia S
Project Start
2006-09-25
Project End
2011-08-31
Budget Start
2009-09-01
Budget End
2010-08-31
Support Year
4
Fiscal Year
2009
Total Cost
$1,093,826
Indirect Cost

  Institution

Name
University of New Mexico
Department
Type
Organized Research Units
DUNS #
868853094
City
Albuquerque
State
NM
Country
United States
Zip Code
87131

  Publications

May, Philip A; Hasken, Julie M; De Vries, Marlene M et al. (2018) A utilitarian comparison of two alcohol use biomarkers with self-reported drinking history collected in antenatal clinics. Reprod Toxicol 77:25-32
Brink, Yolandi; Cockcroft, John; Seedat, Soraya et al. (2018) The postural stability of children with foetal alcohol spectrum disorders during one-leg stance: A feasibility study. Afr J Disabil 7:319
May, Philip A; De Vries, Marlene M; Marais, Anna-Susan et al. (2017) Replication of High Fetal Alcohol Spectrum Disorders Prevalence Rates, Child Characteristics, and Maternal Risk Factors in a Second Sample of Rural Communities in South Africa. Int J Environ Res Public Health 14:
Hoyme, H Eugene; Kalberg, Wendy O; Elliott, Amy J et al. (2016) Updated Clinical Guidelines for Diagnosing Fetal Alcohol Spectrum Disorders. Pediatrics 138:
May, Philip A; Marais, Anna-Susan; de Vries, Marlene M et al. (2016) The continuum of fetal alcohol spectrum disorders in a community in South Africa: Prevalence and characteristics in a fifth sample. Drug Alcohol Depend 168:274-286
Hoyme, H Eugene; Coles, Claire D (2016) Alcohol-Related Neurobehavioral Disabilities: Need for Further Definition and Common Terminology. Pediatrics 138:
May, Philip A; de Vries, Marlene M; Marais, Anna-Susan et al. (2016) The continuum of fetal alcohol spectrum disorders in four rural communities in South Africa: Prevalence and characteristics. Drug Alcohol Depend 159:207-18
Hoyme, H Eugene; Hoyme, Derek B; Elliott, Amy J et al. (2015) A South African mixed race lip/philtrum guide for diagnosis of fetal alcohol spectrum disorders. Am J Med Genet A 167A:752-5
Gautam, P; Nuñez, S C; Narr, K L et al. (2015) Developmental Trajectories for Visuo-Spatial Attention are Altered by Prenatal Alcohol Exposure: A Longitudinal FMRI Study. Cereb Cortex 25:4761-71
Gautam, Prapti; Lebel, Catherine; Narr, Katherine L et al. (2015) Volume changes and brain-behavior relationships in white matter and subcortical gray matter in children with prenatal alcohol exposure. Hum Brain Mapp 36:2318-29

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