- 作者:Tze-Kiong Er ; Chih-Chieh Chen ; Yin-Hsiu Chien ; Wen-Chen Liang ; Tzu-Min Kan ; Yuh-Jyh Jong
- 关键词:GAA ; acid 伪-glucosidase ; HRM ; high resolution melting ; DBS ; dried blood spot ; PCR ; polymerase chain reaction ; WCN ; weighted contact number ; DHPLC ; denaturing high performance liquid chromatography
- 刊名:Clinica Chimica Acta
- 出版年:15 February, 2014
- 年:2014
- 卷:429
- 期:Complete
- 页码:18-25
- 全文大小:1510 K
Background
Pompe disease is an inherited autosomal recessive deficiency of acid 伪-glucosidase (GAA) and is due to pathogenic sequence variants in the corresponding GAA gene. While the analysis of enzyme activity remains the diagnostic test of choice for individuals with Pompe disease, mutation analysis remains for establishing a definitive diagnosis.Methods
High resolution melting (HRM) analysis was performed to screen GAA mutations. Genomic DNA was extracted from peripheral blood samples of the two patients with Pompe disease and 250 normal controls. Exons 2 through 20 of the GAA gene were screened by the HRM analysis. The results were subsequently confirmed by direct sequencing.
Results
This assay proved to be feasible in detecting seven known (c.2T>C, c.1726G>A, c.1845G>A, c.1935C>A, c.1958C>A, c.2238G>C, and c.2815_2816del) GAA mutations. Each mutation could be readily and accurately identified in the difference plot curves. We estimated the carrier frequency of the most common mutation, c.1935G>A (p.D645E), in the Taiwanese population to be 0.2%.
Conclusions
In clinical practice, we suggest that HRM analysis is assumed as a fast and reliable method for screening GAA gene mutations especially the most common mutations which are responsible for Pompe disease among the Taiwanese populations.