The Comprehensive Genetic Test for Vitreoretinopathy utilizes next-generation sequencing (NGS) to examine 24 genes associated with inherited vitreoretinal disorders and retinal dystrophies. It is a targeted gene panel specifically designed to support accurate diagnosis, risk assessment, and prevention.
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The Comprehensive Genetic Test for Vitreoretinopathy is a targeted genetic test designed to evaluate a curated set of genes associated with inherited disorders affecting the vitreous and retina. The comprehensive genetic test for vitreoretinopathy includes the assessment of both coding and selected non-coding variants, enabling a comprehensive analysis of genetic alterations linked to vitreoretinal disease. It is applied in cases where there is a clinical suspicion or established diagnosis of vitreoretinopathy, supporting the molecular characterization of these conditions. The comprehensive genetic test for vitreoretinopathy content overlaps with broader retinal dystrophy testing, ensuring coverage of key genes implicated in overlapping retinal phenotypes and facilitating a more precise understanding of disease etiology.
The comprehensive genetic test for vitreoretinopathy includes genes that play critical roles in retinal vascular development, extracellular matrix organization, and cell signaling pathways. Notable examples include FZD4, LRP5, and NDP, which are involved in the Wnt signaling pathway essential for retinal angiogenesis and vascular integrity, as well as COL2A1 and VCAN, which contribute to the structural composition of the vitreous body. Disruption of these pathways may impair normal retinal development and maintenance. The comprehensive genetic test for vitreoretinopathy is indicated in individuals presenting with clinical features suggestive of inherited vitreoretinal disorders or related phenotypes.
Vitreoretinal diseases are characterized by progressive degeneration of the vitreous and retinal structures, resulting in a broad and heterogeneous clinical spectrum. Common manifestations include retinal detachment, optically empty vitreous, fibrillary degeneration, cataract formation, and neovascularization. The phenotypic presentation may vary significantly, even among affected individuals within the same family. Recognized conditions within this spectrum include familial exudative vitreoretinopathy (FEVR), Wagner syndrome, Stickler syndrome, Norrie disease, snowflake vitreoretinal degeneration, and Knobloch syndrome. These disorders may follow autosomal dominant, autosomal recessive, or X-linked inheritance patterns, contributing to variability in onset, severity, and disease progression.
The comprehensive genetic test for vitreoretinopathy is intended to support the identification of pathogenic variants associated with vitreoretinopathies, enabling improved diagnostic accuracy and differentiation between clinically overlapping conditions. It contributes to a deeper understanding of disease mechanisms and inheritance patterns, which may inform risk assessment and clinical management strategies. The inclusion of genes shared with retinal dystrophy panels enhances its diagnostic utility in complex cases, while the analysis of non-coding regions increases the likelihood of detecting clinically relevant variants that may otherwise be missed.
A higher genetic risk is confirmed when pathogenic mutations are found in genes associated with vitreoretinopathies. A lower risk may be inferred when no mutations are detected, though comprehensive clinical follow-up is still essential. The integration of genetic data with clinical findings and family history is critical for precise diagnosis, prognosis, and long-term patient care.
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.
