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High-resolution melting analysis for detection of MYH9 mutations
Authors:Dana Provaznikova  Tereza Kumstyrova  Roman Kotlin  Peter Salaj  Vaclav Matoska  Ingrid Hrachovinova
Affiliation:1. Institute of Haematology and Blood Transfusion, Coagulation Laboratory, Prague, Czech Republicdana.provaznikova@uhkt.cz;3. Hospital Na Homolce, Molecular Diagnosis Laboratory, Prague, Czech Republic;4. Department of Biochemistry, Institute of Haematology and Blood Transfusion, Prague, Czech Republic;5. Institute of Haematology and Blood Transfusion, Coagulation Laboratory, Prague, Czech Republic
Abstract:
May-Hegglin anomaly (MHA), Sebastian (SBS), Fechtner (FTNS) and Epstein (EPS) syndromes are rare autosomal dominant disorders with giant platelets and thrombocytopenia. Other manifestations of these disorders are combinations of the presence of granulocyte inclusions and deafness, cataracts and renal failure. Currently, MHA, SBS, FTNS and EPS are considered to be distinct clinical manifestation of a single illness caused by mutations of the MYH9 gene encoding the heavy chain of non-muscle myosin IIA (NMMHC-IIA). As the MYH9 gene has a high number of exons, it takes much time and material to use this method for the detection of MYH9 mutations. Recently, a new method has been introduced for scanning DNA mutations without the need for direct sequencing: high-resolution melting analysis (HRMA). Mutation detection with HRMA relies on the intercalation of the specific dye (LC Green plus) in double-strand DNA and fluorescence monitoring of PCR product melting profiles. In our study, we optimized the conditions and used HRMA for rapid screening of mutations in all MYH9 exons in seven affected individuals from four unrelated families with suspected MYH9 disorders. Samples identified by HRMA as positive for the mutation were analysed by direct sequencing. HRMA saved us over 85% of redundant sequencing.
Keywords:MYH9  HRMA  thrombocytopenia  giant platelets  NMMHC-IIA
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