Clinical and molecular study on Fechtner syndrome--case report and literature review.

Hai-Yan YANG; Zhao-Yue WANG; Yan-Hua SU; Li-Juan CAO; Xia BAI; Chang-gen RUAN

Return

Clinical and molecular study on Fechtner syndrome--case report and literature review.

Author: Hai-Yan YANG ¹ ; Zhao-Yue WANG ; Yan-Hua SU ; Li-Juan CAO ; Xia BAI ; Chang-gen RUAN
Author Information

1. Jiangsu Institute of Hematology, The First Affiliated Hospital of Soochow University, Suzhou 215006, China.
Publication Type:Case Reports
MeSH: Adult; Codon, Nonsense; DNA Mutational Analysis; Exons; genetics; Humans; Inclusion Bodies; genetics; Male; Molecular Motor Proteins; genetics; Myosin Heavy Chains; genetics; Nephritis, Hereditary; genetics; Pedigree; Syndrome; Thrombocytopenia; genetics
From: Chinese Journal of Hematology 2007;28(3):160-164
CountryChina
Language:Chinese
Abstract:
OBJECTIVETo identify clinical and laboratory abnormalities and genetic defect of Fechtner syndrome in a Chinese family.
METHODSThe characteristic morphological features of platelets and leukocytes were examined on blood smears with Wright's-Giemsa staining and ultrastructure of platelet and leukocyte were investigated under electron microscope. Genomic DNA was isolated from peripheral blood of the proband and 9 members of his family. All the exons and exon-intron boundaries of the MYH9 gene were amplified by PCR followed by direct sequencing.
RESULTSPatients presented the characteristic clinical features including macrothrombocytopenia, leukocyte inclusions and/or hereditary nephritis. A heterozygous C to T mutation was found in the proband and three members of his family at nucleotide 5981 in exon 40 of MYH9 gene, resulting in a nonsense mutation which encoded truncated protein due to premature termination at the Arg 1933 codon.
CONCLUSIONIt is the first report of a Chinese family with Fechtner syndrome. The Arg (CGA) 1933--> stop (TGA) nonsense mutation in MYH9 gene is a causative genetic defect.