低色素小细胞性贫血病例中α地中海贫血突变的评估:伊斯坦布尔视角
Evaluation of Alpha-Thalassemia Mutations in Cases with Hypochromic Microcytic Anemia: The İstanbul Perspective.
作者信息
Karakaş Zeynep, Koç Begüm, Temurhan Sonay, Elgün Tuğba, Karaman Serap, Asker Gamze, Gençay Genco, Timur Çetin, Yıldırmak Zeynep Yıldız, Celkan Tiraje, Devecioğlu Ömer, Aydın Filiz
机构信息
İstanbul University İstanbul Faculty of Medicine, Department of Pediatric Hematology-Oncology, İstanbul, Turkey Phone: +90 505 906 27 91 E-mail:
出版信息
Turk J Haematol. 2015 Dec;32(4):344-50. doi: 10.4274/tjh.2014.0204. Epub 2015 Aug 6.
OBJECTIVE
Alpha thalassemia syndromes are caused by mutations on one or more of the four α-globin genes. Mutations could be either more commonly deletional or non-deletional. As some deletions (3.7 and 4.2) cause α+-thalassemia, some cause (-20.5, MED, THAI, FIL) α0 -thalassemia. The aim of this study was to determine alpha thalassemia mutations in patients with unsolved hypochromic microcytic anemia and to evaluate types of mutations.
MATERIAL AND METHODS
Two hundred six patients with hypochromic microcytic anemia were evaluated for alpha thalassemia. A venous blood sample of 2 mL was drawn from each patient for DNA isolation. The samples were investigated for α-thalassemia mutations by using the Vienna Lab α-Globlin StripAssay TM commercial kit.
RESULTS
Fourteen different mutations were determined in 95 (46.1%) patients. The most common mutation was the 3.7 single gene deletion and was found in 37 patients (n=37/95, 39%). Others common mutations were the 20.5 kb double gene deletion (n=20 patients, 21%), MED double gene deletion (n=17 patients, 17.9%), α2 IVS1 (n=10 patients, 10.5%), α2 cd142 Hb Koya Dora (n=6 patients, 6.3%), α2 polyA1 (Saudi type) (n=6 patients, 6.3%), 4.2 single gene deletion (n=4 patients, 4.2%), α1 cd14 (n=2 patients, 2.1%), and -FIL mutation (n=2 patients 2.1%), respectively. Hb Adana, Hb Icaria, α2 init cd and α2 polyA2 (Turkish type) were found in 1% of the patients (n=1). Seven patients (7.4%) had α-thalassemia triplication. In our study, three mutations (Hb Icaria, α1 cd14, α2 init.cd) were determined firstly in Turkey. Seven mutations (-SEA, -THAI, Hb Constant Spring, α2 cd19, α2 cd59, α2 cd125, Hb Paksé) were not determined in this study.
CONCLUSION
Alpha thalassemia should be considered in the differential diagnosis of hypochromic microcytic anemia especially in cases without iron deficiency and b-thalassemia carrier state. Genetic testing should be performed for the suspicious cases. We also recommend that a national database with all mutations in Turkey should be created to screen the alpha thalassemia cost-effectively.
目的
α地中海贫血综合征由四个α珠蛋白基因中一个或多个基因的突变引起。突变通常分为缺失型或非缺失型。一些缺失(3.7和4.2)导致α+地中海贫血,一些导致(-20.5、MED、THAI、FIL)α0地中海贫血。本研究的目的是确定未确诊的低色素小细胞贫血患者中的α地中海贫血突变,并评估突变类型。
材料与方法
对206例低色素小细胞贫血患者进行α地中海贫血评估。从每位患者采集2 mL静脉血样本用于DNA分离。使用维也纳实验室α-珠蛋白条带检测TM商业试剂盒对样本进行α地中海贫血突变检测。
结果
在95例(46.1%)患者中确定了14种不同的突变。最常见的突变是3.7单基因缺失,在37例患者中发现(n = 37/95,39%)。其他常见突变包括20.5 kb双基因缺失(n = 20例患者,21%)、MED双基因缺失(n = 17例患者,17.9%)、α2 IVS1(n = 10例患者,10.5%)、α2 cd142 Hb Koya Dora(n = 6例患者,6.3%)、α2 polyA1(沙特型)(n = 6例患者,6.3%)、4.2单基因缺失(n = 4例患者,4.2%)、α1 cd14(n = 2例患者,2.1%)和-FIL突变(n = 2例患者,2.1%)。Hb Adana、Hb Icaria、α2 init cd和α2 polyA2(土耳其型)在1%的患者中发现(n = 1)。7例患者(7.4%)有α地中海贫血三重体。在我们的研究中,三种突变(Hb Icaria、α1 cd14、α2 init.cd)首次在土耳其被确定。本研究未确定七种突变(-SEA、-THAI、Hb Constant Spring、α2 cd19、α2 cd59、α2 cd125、Hb Paksé)。
结论
在低色素小细胞贫血的鉴别诊断中应考虑α地中海贫血,尤其是在无缺铁和β地中海贫血携带者状态的情况下。对可疑病例应进行基因检测。我们还建议创建一个包含土耳其所有突变的国家数据库,以经济有效地筛查α地中海贫血。
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