The Comprehensive Genetic Test for Diamond-Blackfan Anemia utilizes next-generation sequencing (NGS) to examine 14 genes associated with ribosomal protein defects and erythropoiesis 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 Diamond-Blackfan Anemia is a targeted genetic test designed to evaluate inherited causes of red blood cell aplasia. It focuses on identifying genetic alterations associated with Diamond-Blackfan anemia and related conditions such as transient erythroblastopenia of childhood (TEC). Diamond-Blackfan anemia (DBA) is a rare congenital disorder primarily characterized by impaired erythropoiesis, leading to anemia early in life. The comprehensive genetic test for Diamond-Blackfan anemia includes the analysis of both coding and non-coding variants, allowing for a comprehensive assessment of genetic contributions. It is commonly used in individuals presenting with early-onset anemia, particularly when clinical features suggest an underlying hereditary bone marrow failure syndrome.
The comprehensive genetic test for Diamond-Blackfan anemia includes genes that are primarily involved in ribosomal structure and function, such as RPS19, RPL5, RPL11, RPS26, and GATA1. These genes play a critical role in ribosome biogenesis, a fundamental cellular process responsible for protein synthesis. Disruption in ribosomal protein production affects erythroid progenitor cells, which are particularly sensitive to impaired ribosome function, leading to defective red blood cell development. GATA1 is essential for erythroid differentiation and maturation. The comprehensive genetic test for Diamond-Blackfan anemia is indicated in individuals with suspected congenital red cell aplasia or unexplained early-onset anemia consistent with Diamond-Blackfan anemia or related conditions.
The clinical presentation of Diamond-Blackfan anemia is heterogeneous, ranging from mild to severe anemia. It is typically characterized by normochromic, often macrocytic anemia, accompanied by reticulocytopenia and normal white blood cell and platelet counts. In many cases, symptoms manifest within the first year of life. Approximately half of affected individuals present with congenital anomalies, including craniofacial abnormalities, upper limb defects, cardiac malformations, and genitourinary anomalies. Growth restriction is also commonly observed. Disease severity varies significantly, with some individuals requiring long-term corticosteroid therapy or regular blood transfusions, while others may exhibit milder phenotypes. Complications such as iron overload and increased risk of malignancies, including myelodysplastic syndrome and osteosarcoma, have been reported.
The purpose of the comprehensive genetic test for Diamond-Blackfan anemia is to support the identification of pathogenic variants associated with Diamond-Blackfan anemia, thereby facilitating accurate diagnosis and improved clinical classification. It contributes to distinguishing Diamond-Blackfan anemia from other causes of anemia with overlapping features and supports risk stratification and long-term disease monitoring. The detection of causative genetic alterations provides valuable insights into disease mechanisms and helps inform clinical decision-making regarding patient management and surveillance for associated complications, including malignancy risk.
A higher genetic risk is confirmed when pathogenic mutations are found in genes associated with ribosomal protein function or erythroid differentiation. 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.
