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基因编辑治疗镰状细胞病和输血依赖型地中海贫血症——治愈在望。

Gene editing for sickle cell disease and transfusion dependent thalassemias- A cure within reach.

机构信息

From Atrium Health Levine Children's Hospital, Charlotte, NC.

From Sarah Cannon Research Institute and the Tristar Centennial Children Hospital, Nashville TN.

出版信息

Semin Hematol. 2023 Jan;60(1):3-9. doi: 10.1053/j.seminhematol.2022.12.001. Epub 2022 Dec 31.

Abstract

Sickle cell disease (SCD) is associated with significant morbidity and shortened life expectancy. Similarly, patients with transfusion dependent beta thalassemia (TdT) require life-long transfusion therapy, chelation therapy and significant organ dysfunction. Allogeneic transplantation from a matched family donor provided the only curative option for patients with SCD and TdT. Unfortunately, less than 20% of patients have a fully matched related donor and results using unrelated donor transplant were associated with high rate of complications. Ex vivo gene therapy through globin gene addition has been investigated extensively and recent encouraging preliminary data resulted in regulatory approval in patients with TdT. Recent improvements in our understanding of the molecular pathways controlling erythropoiesis and globin switching from fetal hemoglobin to adult hemoglobin offer a new and exciting therapeutic options. Rapid and substantial advances in genome editing tools using CRISPR/Cas9, have raised the possibility of genetic editing and correction in patient derived hematopoietic stem and progenitor cells. We will review results of gene editing approach that can induce fetal hemoglobin production in patients with SCD and TdT.

摘要

镰状细胞病(SCD)与显著的发病率和预期寿命缩短有关。同样,依赖输血的β地中海贫血(TdT)患者需要终身输血治疗、螯合治疗和重要的器官功能障碍。来自匹配的家族供体的同种异体移植为 SCD 和 TdT 患者提供了唯一的根治方法。不幸的是,只有不到 20%的患者有完全匹配的相关供体,而且使用无关供体移植的结果与高并发症率相关。通过珠蛋白基因添加的体外基因治疗已被广泛研究,最近令人鼓舞的初步数据导致了 TdT 患者的监管批准。我们对控制红细胞生成和从胎儿血红蛋白到成人血红蛋白的珠蛋白转换的分子途径的理解的最新进展提供了新的令人兴奋的治疗选择。使用 CRISPR/Cas9 的基因组编辑工具的快速和实质性进展,提高了对患者来源的造血干细胞和祖细胞进行基因编辑和纠正的可能性。我们将回顾可诱导 SCD 和 TdT 患者产生胎儿血红蛋白的基因编辑方法的结果。

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