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Hemoglobin
international journal for hemoglobin research
Volume 32, 2008 - Issue 4
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Original

Detection of β-Thalassemia Mutations Using a Multiplex Amplification Refractory Mutation System Assay

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Pages 403-409 | Received 04 May 2007, Accepted 05 Oct 2007, Published online: 07 Jul 2009
 

Abstract

We developed two sets of a multiplex amplification refractory mutation system (M-ARMS) assay to identify specific β-thalassemia (β-thal) mutations that are common in Thailand. The first one was for the detection of mutants with codon 17 (A>T), IV S-I-1 (G >T)), codons 41/42 (−TCT T) and codons 71/72 (+A), while the second one was for the −87 (C>A), −28 (A>G) and IVS-II-654 (C>T). Application of the proposed assay to 282 persons with β-thal trait revealed a positive result in 276 cases (97.8%). There were 258 cases (91.5%) positive for the set 1 M-ARMS assay and 18 cases (6.4%) were positive for set 2. Six cases (2.2%) were negative for both sets 1 and 2, and were further characterized by DNA sequencing. The mutations detected by the set 1 M-ARMS assay were 113 cases (40.1%) of codons 41/42, 95 (33.7%) of codon 17, 41 (14.5%) of IVS-I-1 and nine cases (3.2%) of codons 71/72, while by set 2 there were 12 cases (4.2%) of −28, four cases(1.4%) of −87 and two cases (0.7%) of IVS-II-654. Mutations undetectable by M-ARMS assay were two cases of codons 27/28 (+C), one case of codon 35 (C>A), one of codon 43 (G>T), one of −31 (A>G) and one of IVS-I-5 (C>G).

The M-ARMS assay proved to be a valuable tool for the analysis of β-thal mutations. The method is robust, accurate, simple, speedy and cost-effective. The application of this assay will facilitate genetic counseling and prenatal diagnosis for severe thalassemia in high-risk pregnancies.

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