The Comprehensive Genetic Test for Adams-Oliver Syndrome (AOS) utilizes next-generation sequencing (NGS) to examine 8 genes implicated in AOS pathogenesis. It is a targeted gene panel specifically designed to support accurate diagnosis, risk assessment, and prevention.
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The Adams-Oliver Syndrome (AOS) Panel is a specialized genetic test designed to identify mutations associated with Adams-Oliver Syndrome (AOS), a rare congenital disorder characterized by scalp and limb abnormalities. This test plays a critical role in elucidating the genetic causes of structural anomalies and vascular disruptions that are often observed in individuals with AOS. The panel is used in functional medicine to assess inherited genomic imbalances that may contribute to complex developmental phenotypes. It serves as a powerful tool in precision diagnostics, providing insight into the biological underpinnings of observed clinical traits.
Adams-Oliver Syndrome typically presents with aplasia cutis congenita (localized absence of skin), most commonly affecting the scalp) and terminal transverse limb defects, which may include shortened or absent fingers, toes, or limbs. Additional features may include congenital heart defects, cutis marmorata telangiectatica congenita, and central nervous system abnormalities. These phenotypes are believed to arise from impaired vasculogenesis and disrupted cellular signaling during embryogenesis, with several causative genes now known to be involved in this dysregulation. The AOS Panel targets genes associated with both autosomal dominant and autosomal recessive inheritance patterns, enabling detection across a broad spectrum of presentations.
Mutations identified through this panel are often linked to impaired endothelial function, disrupted cytoskeletal organization, and altered transcriptional regulation. Variants in genes such as ARHGAP31, DOCK6, EOGT, RBPJ, and NOTCH1 are known to disrupt normal cell adhesion, migration, and differentiation, resulting in the tissue malformations characteristic of the syndrome. In some cases, specific mutations may correlate with a more severe or more widespread phenotype, whereas other variants may present with milder or incomplete features. Inheritance patterns and mutation types can influence the severity and expressivity of the condition, which can be higher or lower depending on the nature and combination of genetic alterations.
Early genetic insight through the AOS Panel facilitates a deeper understanding of the molecular mechanisms contributing to limb and skin development disorders. By highlighting gene-pathway relationships and uncovering potentially pathogenic variants, this test supports advanced investigation into multisystem involvement, developmental delays, and syndromic associations. The panel provides a foundation for mapping genetic influences on embryological development, guiding decisions regarding genomic health and analysis of inherited traits.
The test is performed in a clinical laboratory accredited to ISO 15189 and certified by CLIA and CAP, ensuring the validity, accuracy and international recognition of the results.
