台湾重型β地中海贫血的分子基础及血液学特征，一例中国患者存在IVS-1 3'端TAG→GAG突变

Molecular basis and haematological characterization of beta-thalassaemia major in Taiwan, with a mutation of IVS-1 3' end TAG-->GAG in a Chinese patient.

作者信息

Chiou S S, Chang T T, Chen P H, Lee L S, Chen T S, Chang J G

机构信息

Department of Paediatrics, Kaohsiung Medical College Hospital, Taiwan, R.O.C.

出版信息

Br J Haematol. 1993 Jan;83(1):112-7. doi: 10.1111/j.1365-2141.1993.tb04640.x.

DOI:10.1111/j.1365-2141.1993.tb04640.x

PMID:8435318

Abstract

We studied 41 patients with beta-thalassaemia major and their parents by using a combination of polymerase chain reaction (PCR) amplification, slot-blot hybridization of allele-specific oligonucleotide (ASO), and direct genomic sequencing. Eight different point mutations were characterized. C to T substitution at nucleotide (nt) 654 of intervening sequences (IVS) 2, accounting for 46.3% of mutant beta-globin genes, is the most common mutation in Taiwan, followed by frameshift codons 41/42 with four nucleotides (TCTT) deletion for 31.7%, A to G substitution at position -28 of promotor area for 8.5%, A to T substitution at codon 17 for 6.1%, frameshift codons 27/28 (insertion of C) for 2.4%, G to T substitution at nucleotide 1 of IVS-1 for 2.4%, frameshift codons 71/72 (insertion of A) and IVS-1 3 end TAG-->GAG for 1.2%. The former four mutations showed no obvious difference between two major ethnic groups in Taiwan. As to mutations in each individual of beta-thalassaemia major, the incidence of compound heterozygotes of two different mutations is much higher than homozygotes of single mutation, 78.0% v 22.0%. Compound heterozygotes of C to T substitution at nt 654 of IVS-2 and frameshift codons 41/42 with four nucleotides deletion is the most common pattern of beta-thalassaemia mutations in each individual (41.5%). The results are somewhat different from other documented reports concerning the mutations of beta-thalassaemia in southern China. This is the first report of mutation of IVS-1 3' end TAG-->GAG which causes consensus change in Chinese people. Patients with heterozygotes of beta zero and -28 beta(+)-thalassaemia mutations would have a greater delay in initial transfusion in comparison to patients with homozygotes of both beta zero-thalassaemia mutation, but their initial clinical manifestation might be aggravated when combined with a glucose-6-phosphate dehydrogenase (G-6-PD) deficiency and an insult such as exposure to infection and certain drugs.

摘要

我们运用聚合酶链反应（PCR）扩增、等位基因特异性寡核苷酸（ASO）斑点杂交及直接基因组测序相结合的方法，对41例重型β地中海贫血患者及其父母进行了研究。鉴定出8种不同的点突变。内含子序列（IVS）2第654位核苷酸（nt）由C突变为T，占突变β珠蛋白基因的46.3%，是台湾地区最常见的突变，其次是移码密码子41/42缺失4个核苷酸（TCTT），占31.7%，启动子区-28位由A突变为G占8.5%，密码子17由A突变为T占6.1%，移码密码子27/28（插入C）占2.4%，IVS-1第1位核苷酸由G突变为T占2.4%，移码密码子71/72（插入A）及IVS-1 3'端TAG→GAG占1.2%。前4种突变在台湾地区的两个主要族群之间无明显差异。至于重型β地中海贫血患者个体中的突变情况，两种不同突变的复合杂合子发生率远高于单一突变的纯合子，分别为78.0%和22.0%。IVS-2第654位核苷酸由C突变为T与移码密码子41/42缺失4个核苷酸的复合杂合子是患者个体中最常见的β地中海贫血突变模式（41.5%）。这些结果与中国南方有关β地中海贫血突变的其他文献报道略有不同。这是IVS-1 3'端TAG→GAG突变在中国人群中导致一致性改变的首次报道。β0和-28β（+）地中海贫血突变杂合子患者与β0地中海贫血突变纯合子患者相比，首次输血延迟时间更长，但当合并葡萄糖-6-磷酸脱氢酶（G-6-PD）缺乏以及感染和某些药物等刺激因素时，其初始临床表现可能会加重。