The Comprehensive Genetic Test for Hereditary Hemochromatosis utilizes next-generation sequencing (NGS) to examine 5 genes associated with hereditary hemochromatosis and iron metabolism disorders. 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 Hereditary Hemochromatosis is a targeted genetic test designed to evaluate hereditary causes of iron metabolism disorders, particularly hereditary hemochromatosis. The comprehensive genetic test for hereditary hemochromatosis includes the analysis of 5 genes, along with selected non-coding variants, enabling a focused assessment of genetic factors associated with abnormal iron regulation. It is primarily used in individuals with a clinical suspicion of iron overload or disorders affecting iron absorption and storage. These conditions are characterized by excessive intestinal iron absorption, leading to progressive accumulation of iron in tissues and potential organ damage over time.
The comprehensive genetic test for hereditary hemochromatosis includes key genes such as HFE, HFE2, HAMP, TFR2, and SLC40A1, which are involved in the regulation of systemic iron homeostasis. HFE plays a central role in controlling iron absorption through its interaction with transferrin receptors, while HFE2 and HAMP are critical regulators of hepcidin, the main hormone controlling iron balance. TFR2 contributes to iron sensing, and SLC40A1 encodes ferroportin, responsible for iron export from cells. Proper function of these pathways is essential for maintaining iron equilibrium. Disruptions lead to increased iron absorption and tissue deposition. The comprehensive genetic test for hereditary hemochromatosis is indicated in individuals with elevated iron parameters or clinical features suggestive of hereditary hemochromatosis.
The clinical spectrum of hereditary hemochromatosis is variable and ranges from asymptomatic iron overload to progressive organ damage. Common manifestations include fatigue, joint pain, liver dysfunction, skin hyperpigmentation, diabetes, and cardiomyopathy. The disease may present in adulthood, although some forms, such as juvenile hemochromatosis, manifest earlier with more severe progression. Iron accumulation primarily affects the liver, heart, pancreas, and endocrine organs. Despite relatively common genetic variants, clinical expression is highly variable, and many individuals with pathogenic mutations may remain asymptomatic due to low disease penetrance.
The purpose of the comprehensive genetic test for hereditary hemochromatosis is to identify pathogenic variants associated with hereditary hemochromatosis and related iron metabolism disorders, supporting accurate diagnosis and differentiation from secondary causes of iron overload. Genetic findings contribute to improved understanding of iron regulation and support appropriate disease classification. The identification of specific genetic alterations assists in risk assessment, prognosis evaluation, and the development of individualized long-term monitoring strategies.
A higher genetic risk is confirmed when pathogenic mutations are found in genes associated with hereditary hemochromatosis, including HFE, HFE2, HAMP, TFR2, and SLC40A1. 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 biochemical 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.
