The Comprehensive Genetic Test for Hermansky-Pudlak Syndrome (HPS) uses next-generation sequencing (NGS) to analyze 23 genes implicated in hereditary defects in cellular trafficking, which are associated with the syndrome’s pathology. It is a targeted gene panel specifically designed to support accurate diagnosis, risk assessment, and prevention.
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The Hermansky-Pudlak Syndrome (HPS) Panel is a targeted genetic test designed to identify pathogenic variants responsible for Hermansky-Pudlak Syndrome, a rare autosomal recessive disorder characterized by oculocutaneous albinism, platelet dysfunction, and lysosomal storage defects. This panel is used in functional medicine to investigate inherited disruptions in intracellular trafficking and organelle biogenesis, particularly those affecting melanosomes, platelet-dense granules, and lysosomes. By analyzing genes implicated in HPS, the test provides molecular insight into syndromic presentations characterized by pigmentation defects, bleeding diathesis, and pulmonary or gastrointestinal complications.
Hermansky-Pudlak Syndrome results from mutations in genes that encode components of protein complexes involved in vesicle formation, transport, and fusion within specialized secretory organelles. These include the biogenesis of lysosome-related organelles complexes (BLOCs) and adaptor protein complexes such as AP-3. Mutations in genes such as HPS1, HPS3, HPS4, HPS5, HPS6, HPS7, HPS8, and AP3B1 impair trafficking to melanosomes and dense granules, leading to abnormal pigmentation and platelet storage pool deficiency. The clinical manifestations vary by subtype and range from mild oculocutaneous albinism to life-threatening pulmonary fibrosis, colitis, and immune system abnormalities.
Reduced or absent pigmentation is often observed in the skin, hair, and irises due to disrupted melanosome maturation and function. Platelet dysfunction leads to prolonged bleeding times and easy bruising, even when platelet counts are normal. In more severe subtypes such as HPS-1 and HPS-4, progressive pulmonary fibrosis may develop, often beginning in early adulthood and leading to respiratory failure if unaddressed. In some cases, granulomatous colitis or neutropenia may result from impaired lysosomal processing in immune cells. Because the syndrome affects multiple systems through shared vesicular pathways, the combination of albinism, bleeding diathesis, and lung or gut involvement suggests an underlying defect in intracellular organelle biogenesis.
The genes included in the Hermansky-Pudlak Syndrome Panel are essential for maintaining the function of organelles required for pigment production, clotting, and immune defense. Their dysfunction affects intracellular transport, vesicle tethering, and the assembly of multi-protein trafficking complexes. This test is used to uncover inherited causes of systemic dysfunction that begin with dermatological or hematological signs but extend to the respiratory and gastrointestinal systems. By identifying mutations across the HPS gene family, the panel provides a detailed map of the underlying molecular pathology. It supports comprehensive investigation of syndromes where pigmentation defects and multi-organ complications coexist.
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.
