Detection and characterisation of [beta]-globin gene cluster deletions in Chinese using multiplex ligation-dependent probe amplification

Detection and characterisation of [beta]-globin gene cluster deletions in Chinese using multiplex ligation-dependent probe amplification

Background: Deletions in the β-globin cluster causing thalassaemia and hereditary persistence of fetal haemoglobin (HPFH) are uncommon and difficult to detect. Data in Chinese are very scarce. Aims: To use a recently available technique to investigate the frequencies and nature of β-globin cluster d...

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Veröffentlicht in:Journal of clinical pathology 2009-12, Vol.62 (12), p.1107
Hauptverfasser: So, C C, So, A C Y, Chan, A Y Y, Tsang, S T Y, Ma, E S K, Chan, L C
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container_end_page
container_issue 12
container_start_page 1107
container_title Journal of clinical pathology
container_volume 62
creator So, C C
So, A C Y
Chan, A Y Y
Tsang, S T Y
Ma, E S K
Chan, L C
description Background: Deletions in the β-globin cluster causing thalassaemia and hereditary persistence of fetal haemoglobin (HPFH) are uncommon and difficult to detect. Data in Chinese are very scarce. Aims: To use a recently available technique to investigate the frequencies and nature of β-globin cluster deletions in Chinese. Methods: 106 subjects with phenotypes of thalassaemia or HPFH and suspected to have deletions in the β-globin cluster were studied. A commercially available kit employing multiplex ligation-dependent probe amplification (MLPA) was used to screen for deletions. Gap PCR and direct nucleotide sequencing were used to characterise deletions detected. Results: 17 deletions in the β-globin cluster were found in 17 patients: 8 of Chinese (A [GAMMA]δβ)0 thalassaemia, 7 of Southeast Asian (Vietnamese) deletion and 2 of Thai (A [GAMMA]δβ)0 thalassaemia. The only type of deletion detected in δβ-thalassaemia was Chinese (A [GAMMA]δβ)0 thalassaemia. The deletional form of HPFH was rarely seen in only 1 case of Thai (A [GAMMA]δβ)0 thalassaemia. Deletions presenting as β-thalassaemia trait and raised HbF were all of the Southeast Asian (Vietnamese) deletion type. When these deletions were co-inherited with classical β-thalassaemia mutations in compound heterozygous states, the phenotypes could be very variable. Conclusions: In the Chinese population, there are only relatively few types of deletions seen in the β-globin cluster. MLPA is a fast and effective way of screening for these deletions. Characterisation of these deletions allows the development of simpler and more specific PCR-based tests for routine diagnostic use. Accurate prediction of phenotype is not always feasible. The molecular defects in many cases of HPFH still await discovery.
doi_str_mv 10.1136/jcp.2009.067538
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Data in Chinese are very scarce. Aims: To use a recently available technique to investigate the frequencies and nature of β-globin cluster deletions in Chinese. Methods: 106 subjects with phenotypes of thalassaemia or HPFH and suspected to have deletions in the β-globin cluster were studied. A commercially available kit employing multiplex ligation-dependent probe amplification (MLPA) was used to screen for deletions. Gap PCR and direct nucleotide sequencing were used to characterise deletions detected. Results: 17 deletions in the β-globin cluster were found in 17 patients: 8 of Chinese (A [GAMMA]δβ)0 thalassaemia, 7 of Southeast Asian (Vietnamese) deletion and 2 of Thai (A [GAMMA]δβ)0 thalassaemia. The only type of deletion detected in δβ-thalassaemia was Chinese (A [GAMMA]δβ)0 thalassaemia. The deletional form of HPFH was rarely seen in only 1 case of Thai (A [GAMMA]δβ)0 thalassaemia. Deletions presenting as β-thalassaemia trait and raised HbF were all of the Southeast Asian (Vietnamese) deletion type. When these deletions were co-inherited with classical β-thalassaemia mutations in compound heterozygous states, the phenotypes could be very variable. Conclusions: In the Chinese population, there are only relatively few types of deletions seen in the β-globin cluster. MLPA is a fast and effective way of screening for these deletions. Characterisation of these deletions allows the development of simpler and more specific PCR-based tests for routine diagnostic use. Accurate prediction of phenotype is not always feasible. The molecular defects in many cases of HPFH still await discovery.</description><identifier>ISSN: 0021-9746</identifier><identifier>EISSN: 1472-4146</identifier><identifier>DOI: 10.1136/jcp.2009.067538</identifier><identifier>CODEN: JCPAAK</identifier><language>eng</language><publisher>London: BMJ Publishing Group LTD</publisher><subject>Archives &amp; records ; Defects ; Genes ; Genotype &amp; phenotype ; Laboratories ; Mitochondrial DNA ; Mutation ; Patients</subject><ispartof>Journal of clinical pathology, 2009-12, Vol.62 (12), p.1107</ispartof><rights>Copyright: 2009 BMJ Publishing Group Ltd &amp; Association of Clinical Pathologists. 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Deletions presenting as β-thalassaemia trait and raised HbF were all of the Southeast Asian (Vietnamese) deletion type. When these deletions were co-inherited with classical β-thalassaemia mutations in compound heterozygous states, the phenotypes could be very variable. Conclusions: In the Chinese population, there are only relatively few types of deletions seen in the β-globin cluster. MLPA is a fast and effective way of screening for these deletions. Characterisation of these deletions allows the development of simpler and more specific PCR-based tests for routine diagnostic use. Accurate prediction of phenotype is not always feasible. 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subjects Archives & records
Defects
Genes
Genotype & phenotype
Laboratories
Mitochondrial DNA
Mutation
Patients
title Detection and characterisation of [beta]-globin gene cluster deletions in Chinese using multiplex ligation-dependent probe amplification
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