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Effect of alpha thalassaemia trait and enhanced gamma chain production on disease severity in beta thalassaemia major and intermedia.

机译:α地中海贫血性状和增强的γ链产生对严重地中海贫血和中间地中海贫血疾病严重程度的影响。

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摘要

One hundred and twenty patients with homozygous beta thalassaemia were selected to determine the clinical effects of certain genetic factors which may modify disease severity. Genetic analysis defined specific beta thalassaemia mutations, the alpha thalassaemia genotype, and the presence of an XmnI restriction enzyme site, associated with increased fetal haemoglobin (HbF) production under certain conditions. Genotypic data with globin chain synthesis were related to the age when regular transfusions began and subsequent pubertal development. This study showed that the major determinants of disease severity in beta thalassaemia were the beta thalassaemia mutations, with co-inheritance of alpha thalassaemia trait and coinheritance of a high HbF determinant acting as ameliorating factors. The presence of an alpha thalassaemia deletion significantly reduced initial disease severity, although the effect on pubertal development was less clear. It is concluded that detailed genetic analysis should be performed in all newly diagnosed patients with thalassaemia. This, in conjunction with clinical assessment, will help to predict disease severity and prognosis.
机译:选择了120名纯合性β地中海贫血患者,以确定可能改变疾病严重程度的某些遗传因素的临床效果。遗传分析定义了特定的β地中海贫血突变,α地中海贫血基因型以及XmnI限制酶位点的存在,在某些情况下会增加胎儿血红蛋白(HbF)的产生。球蛋白链合成的基因型数据与开始定期输血的年龄以及随后的青春期发育有关。这项研究表明,β地中海贫血中疾病严重程度的主要决定因素是β地中海贫血突变,α地中海贫血性状的共遗传和高HbF决定因素的共遗传是改善因素。尽管对青春期发育的影响尚不清楚,但α地中海贫血缺失的存在可显着降低初始疾病的严重程度。结论是,应对所有新诊断的地中海贫血患者进行详细的遗传分析。结合临床评估,将有助于预测疾病的严重程度和预后。

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