The Comprehensive Genetic Test for Platelet Function Disorders utilizes next-generation sequencing (NGS) to examine 23 genes associated with platelet dysfunction and inherited thrombocytopathies. It is a targeted gene panel specifically designed to support accurate diagnosis, risk assessment, and prevention.
More Information
The Comprehensive Genetic Test for Platelet Function Disorders is a targeted genetic test designed to evaluate inherited disorders affecting platelet function and hemostasis. The comprehensive genetic test for platelet function disorders includes the analysis of selected genes, along with selected non-coding variants, enabling a comprehensive assessment of genetic factors associated with qualitative platelet defects. It is particularly suitable for individuals with a clinical suspicion of disorders such as Bernard-Soulier syndrome, Glanzmann thrombasthenia, Gray platelet syndrome, or Hermansky-Pudlak syndrome. These conditions are characterized by impaired platelet function despite normal or near-normal platelet counts, leading to defective clot formation and increased bleeding tendency.
The comprehensive genetic test for platelet function disorders includes key genes such as GP1BA, GP1BB, GP9, ITGA2B, ITGB3, and NBEAL2, which are involved in platelet adhesion, aggregation, and granule formation. GP1BA, GP1BB, and GP9 encode components of the glycoprotein Ib receptor complex essential for platelet adhesion to the vascular wall, while ITGA2B and ITGB3 encode integrin subunits required for platelet aggregation. NBEAL2 is involved in the formation and function of platelet granules. Disruptions in these pathways impair platelet activation and clot formation. The comprehensive genetic test for platelet function disorders is indicated in individuals presenting with clinical features suggestive of inherited platelet function disorders.
The clinical spectrum of platelet function disorders includes mucocutaneous bleeding manifestations such as easy bruising, epistaxis, gingival bleeding, prolonged bleeding following injury or surgery, and heavy menstrual bleeding. Bernard-Soulier syndrome is characterized by defective platelet adhesion and may present with thrombocytopenia and enlarged platelets, while Glanzmann thrombasthenia results in impaired platelet aggregation. Gray platelet syndrome is associated with defects in platelet granules and variable bleeding severity. These conditions are rare and demonstrate significant variability in clinical presentation, ranging from mild bleeding tendencies to severe hemorrhagic episodes, often beginning in childhood.
The purpose of the comprehensive genetic test for platelet function disorders is to identify pathogenic variants associated with inherited platelet function disorders, supporting accurate diagnosis and differentiation between specific syndromes. Genetic findings contribute to improved classification of platelet disorders and provide insight into the molecular mechanisms underlying impaired platelet function. The identification of specific genetic alterations supports risk assessment and informs appropriate long-term disease monitoring strategies.
A higher genetic risk is confirmed when pathogenic mutations are found in genes associated with platelet function disorders, including GP1BA, ITGA2B, and NBEAL2. 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 laboratory evaluation 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.
