造血干细胞移植治疗地中海贫血:综述

IF 0.4 Q4 BIOLOGY Advances in Human Biology Pub Date : 2023-01-01 DOI:10.4103/aihb.aihb_104_23
Mainul Haque, Rabeya Yousuf, Dilshad Jahan, Susmita Sinha
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引用次数: 0

摘要

地中海贫血是一种特别普遍的人类单基因疾病,由缺乏α-或β-珠蛋白链的合成引起。β-地中海贫血的临床影响更严重,因为它由相同的对基因配置组成,即地中海贫血,由于血红蛋白(Hb)水平不足而危及生命,导致严重的健康障碍和生命损失。只有少数国家成功地降低了严重β-地中海贫血的患病率,尽管可以采用全面筛查、小组咨询、产前检测和公共教育等方法。半个多世纪以来,治疗重度地中海贫血的基本要素一直是铁螯合和大量输血。在β-地中海贫血中,构成成人血红蛋白分子的珠蛋白链缺失或合成速率降低。α-珠蛋白链的异常积聚和红细胞(RBC)的错误形成导致红细胞溶血是这种遗传异常的结果。多年来,同种异体造血干细胞移植(alloo - hsct)一直是治疗重度地中海贫血患者的一种行之有效的基因替代疗法,对于接受这种疗法的患者来说,它已经取得了非常成功的结果。在过去的20年里,易感患者的后果也在稳步改善,这类患者的预期寿命延长了80%-90%。然而,在全球范围内为这些患者提供同种异体造血干细胞移植治疗存在许多困难。近年来,利用病毒载体替代自体造血干细胞中的基因已成为可能。
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Haematopoietic stem cell transplantation in thalassaemia major: A narrative review
Thalassaemia constitutes an especially prevalent human monogenic illness caused by a lack of synthesis of the α- or β-globin chains. The clinical impact of β-thalassaemia is worse since it consists of the same pair gene configuration, thalassaemia major, causing significant health discouragement and loss of life due to life threateningly insufficient haemoglobin (Hb) levels. Only a few nations have successfully reduced the prevalence of β-thalassaemia major, even though comprehensive screening, group counselling, pre-natal detection and public education can all be used. Since over ½ century ago, the fundamental elements of treatment for thalassaemia major have been iron chelation and hypertransfusion. The globin chain that makes up the adult Hb molecule is missing or synthesised at a reduced rate in β-thalassemia. The aberrant buildup of the α-globin chain and faulty formation of red blood cells (RBCs) leading to RBC haemolysis are the outcomes of this genetic abnormality. Since allogeneic haematopoietic stem cell transplantation (Allo-HSCT) has been a well-established gene replacement therapy for individuals with thalassaemia major for several years, it has had very successful outcomes for patients with access to it. Over the past 20 years, the consequences for more susceptible patients have also steadily improved, leading to 80%–90% longer-term life expectancy amongst this group of patients. However, providing Allo-HSCT as a treatment for these patients globally presents numerous difficulties. Replacing genes in autologous HSCs employing viral vectors has been possible in recent years.
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