Worldwide Prevalence of Fetal Alcohol Spectrum Disorders: A Systematic Literature Review Including Meta-Analysis.
- Authors
- Roozen, Sylvia; Peters, Gjalt-Jorn Y; Kok, Gerjo; Townend, David; Nijhuis, Jan; Curfs, Leopold
- Year
- 2016
- Journal
- Alcoholism, clinical and experimental research
- PMID
- 26727519
- DOI
- 10.1111/acer.12939
BACKGROUND: Although fetal alcohol spectrum disorders (FASD) affect communities worldwide, little is known about its prevalence. The objective of this study was to provide an overview of the global FASD prevalence. METHODS: We performed a search in multiple electronic bibliographic databases up to August 2015, supplemented with the ascendancy and descendancy approach. Studies were considered when published in English, included human participants, and reported empirical data on prevalence or incidence estimates of FASD. Raw prevalence estimates were transformed using the Freeman-Tukey double arcsine transformation so that the data followed an approximately normal distribution. Once the pooled prevalence estimates, 95% confidence intervals and prediction intervals were calculated based on multiple meta-analyses with transformed proportions using random effects models, these estimates were transformed back to regular prevalence rates. Heterogeneity was tested using Cochran's Q and described using the I(2) statistic. RESULTS: Among studies that estimated prevalence in general population samples, considerable differences in prevalence rates between countries were found and therefore separate meta-analyses for country were conducted. Particularly high-prevalence rates were observed in South Africa for fetal alcohol syndrome (55.42 per 1,000), for alcohol-related neurodevelopmental disorder (20.25 per 1,000), and FASD (113.22 per 1,000), For partial fetal alcohol syndrome high rates were found in Croatia (43.01 per 1,000), Italy (36.89 per 1,000), and South Africa (28.29 per 1,000). In the case of alcohol-related birth defects, a prevalence of 10.82 per 1,000 was found in Australia. However, studies into FASD exhibited substantial heterogeneity, which could only partly be explained by moderators, most notably geography and descent, in meta-regressions. In addition, the moderators were confounded, making conclusions as to each moderator's relevance tentative at best. CONCLUSIONS: The worldwide pooled prevalence estimates are higher than assumed so far, but this was largely explained by geography and descent. Furthermore, prevalence studies varied considerably in terms of used methodology and methodological quality. The pooled estimates must therefore be interpreted with caution and for future research it is highly recommended to report methodology in a more comprehensive way. Finally, clear guidelines on assessing FASD prevalence are urgently needed, and a first step toward these guidelines is presented.
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In this knowledge base
| Title | Year | PMID |
|---|---|---|
| Meta-Analyses of Externalizing Disorders: Genetics or Prenatal Alcohol Exposure? | 2018 | 29063614 |
External
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| Prevalence of Prenatal Alcohol Exposure in the State of Texas as Assessed by Phosphatidylethanol in Newborn Dried Blood Spot Specimens. | Bakhireva LN et al. | โ | 2017 | โ |
| Profile of children diagnosed with a fetal alcohol spectrum disorder: A retrospective chart review. | Reid N et al. | โ | 2017 | โ |
| Radiological studies of fetal alcohol spectrum disorders in humans and animal models: An updated comprehensive review. | Nguyen VT et al. | โ | 2017 | โ |
| 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. | May PA et al. | โ | 2017 | โ |
| rs10732516 polymorphism at the <i>IGF2/H19</i> locus associates with a genotype-specific trend in placental DNA methylation and head circumference of prenatally alcohol-exposed newborns. | Marjonen H et al. | โ | 2017 | โ |
| The BAF (BRG1/BRM-Associated Factor) chromatin-remodeling complex exhibits ethanol sensitivity in fetal neural progenitor cells and regulates transcription at the miR-9-2 encoding gene locus. | Burrowes SG et al. | โ | 2017 | โ |
| The Prevalence of Fetal Alcohol Syndrome and Its Impact on a Child's Classroom Performance: A Case Study of a Rural South African School. | Lubbe M et al. | โ | 2017 | โ |
| What can be done to lessen morbidity associated with fetal alcohol spectrum disorders? | Mukherjee R et al. | โ | 2017 | โ |
| Assays of Gamma-Glutamyl Transferase and Carbohydrate-Deficient Transferrin Combination from Maternal Serum Improve the Detection of Prenatal Alcohol Exposure. | Niemelรค O et al. | โ | 2016 | โ |
| Behavioral Responses to Novelty or to a Predator Stimulus Are Not Altered in Adult Zebrafish by Early Embryonic Alcohol Exposure. | Seguin D et al. | โ | 2016 | โ |
| Cohesive Referencing Errors During Narrative Production as Clinical Evidence of Central Nervous System Abnormality in School-Aged Children With Fetal Alcohol Spectrum Disorders. | Thorne JC et al. | โ | 2016 | โ |
| Developmental Ethanol Exposure Leads to Long-Term Deficits in Attention and Its Underlying Prefrontal Circuitry. | Louth EL et al. | โ | 2016 | โ |
| Effects of sex and housing on social, spatial, and motor behavior in adult rats exposed to moderate levels of alcohol during prenatal development. | Rodriguez CI et al. | โ | 2016 | โ |
| Erratum. | โ | โ | 2016 | โ |
| Fetal Alcohol Spectrum Disorders (FASD): an Approach to Effective Prevention. | Roozen S et al. | โ | 2016 | โ |
| Fetal alcohol-spectrum disorders: identifying at-risk mothers. | Montag AC | โ | 2016 | โ |
| Objective Measures of Prenatal Alcohol Exposure: A Systematic Review. | McQuire C et al. | โ | 2016 | โ |
| Plasma miRNA Profiles in Pregnant Women Predict Infant Outcomes following Prenatal Alcohol Exposure. | Balaraman S et al. | โ | 2016 | โ |
| Recognition memory is selectively impaired in adult rats exposed to binge-like doses of ethanol during early postnatal life. | MacIlvane NM et al. | โ | 2016 | โ |
| Second-Trimester Ultrasound as a Tool for Early Detection of Fetal Alcohol Spectrum Disorders. | Montag AC et al. | โ | 2016 | โ |
| Third Trimester Equivalent Alcohol Exposure Reduces Modulation of Glutamatergic Synaptic Transmission by 5-HT1A Receptors in the Rat Hippocampal CA3 Region. | Morton RA et al. | โ | 2016 | โ |
| Phosphorylation Modulates Aspartyl-(Asparaginyl)-ฮฒ Hydroxylase Protein Expression, Catalytic Activity and Migration in Human Immature Neuronal Cerebellar Cells. | Tong M et al. | โ | 2013 | โ |