George E
Department of Pathology, Faculty of Medicine, Universiti Kebangsaan Malaysia, Kuala Lumpur, Malaysia.
Southeast Asian J Trop Med Public Health. 1995;26 Suppl 1:225-8.
Beta-thalassemia in West Malaysia is caused by 14 molecular defects with differing clinical severity. In Chinese patients from West Malaysia, the main beta-thalassemia mutations seen were (a) a 4 base pair-TCTT deletion in codon 41-42 [frameshift mutation (FSC 41-42)]; (b) a C to T substitution at the second intervening sequence (IVS2-654); (c) an A to G substitution in the TATA box [-28 (A to G)], and (d) an A to T substitution in codon 17[17 A to T]. In the Malays, the main mutations seen were (a) a G to C in nucleotide 5 at the intervening sequence I [IVS1-5 (G to C)]; (b) G to T substitution in nucleotide I at the intervening sequence I [IVS1-1 (G to T)]; (c) a A to T substitution in codon 17 (17 A to T); (d) removal of C from codon 35 [codon 35 (-C)], and (e) a 4 base pairs-TCTT deletion in codon 41-42 [frameshift mutation (FSC 41-42)]. A scoring system (Tha1 CS) has been formulated to predict clinical severity. It is the type of beta-thalassemia mutation present that decides on the clinical phenotype. The most severe beta-thalassemia mutation is assigned a score of 4. A score of 8 indicates severe thalassemia.
马来西亚西部的β地中海贫血由14种分子缺陷引起,临床严重程度各异。在马来西亚西部的华裔患者中,主要观察到的β地中海贫血突变有:(a) 密码子41 - 42处4个碱基对-TCTT缺失 [移码突变 (FSC 41 - 42)];(b) 第二个内含子序列 (IVS2 - 654) 处C突变为T;(c) TATA框 [-28 (A突变为G)] 处A突变为G,以及(d) 密码子17处A突变为T [17 A to T]。在马来人中,主要观察到的突变有:(a) 内含子序列I的第5个核苷酸处G突变为C [IVS1 - 5 (G to C)];(b) 内含子序列I的第1个核苷酸处G突变为T [IVS1 - 1 (G to T)];(c) 密码子17处A突变为T (17 A to T);(d) 密码子35处C缺失 [密码子35 (-C)],以及(e) 密码子41 - 42处4个碱基对-TCTT缺失 [移码突变 (FSC 41 - 42)]。已经制定了一个评分系统 (Tha1 CS) 来预测临床严重程度。决定临床表型的是所存在的β地中海贫血突变类型。最严重的β地中海贫血突变得分为4分。8分表示重度地中海贫血。
