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. 2021 Apr;29(2):643-647.
doi: 10.19746/j.cnki.issn.1009-2137.2021.02.054.

[Progress in Gene Therapy of Sickle Cell Disease Based on Hemoglobin F--Review]

[Article in Chinese]
Hao Liang  1 Yun-Xia Wang  1 Xu-Yan Li  1 Ya-Qi Wang  1 Yan Su  2
Affiliations

[Progress in Gene Therapy of Sickle Cell Disease Based on Hemoglobin F--Review]

[Article in Chinese]
Hao Liang et al. Zhongguo Shi Yan Xue Ye Xue Za Zhi. 2021 Apr.

Abstract
in English, Chinese

Sickle cell disease (SCD) is a single gene genetic disease, which seriously threatens the life span and quality of patients. On the basis of the pathogenesis of SCD and the alternative therapy based on fetal hemoglobin F (HbF), the research progress of transcription factors involved in the regulation of HbF gene expression, such as BCL11A, ZBTB7A, KLF-1, c-MYB and SOX6, as well as the application of CRISPR / Cas9, TALEN, zinc finger nuclease and other gene editing technologies in this field has been made, providing a solid theoretical basis for the exploration of new treatment schemes for β- like hemoglobin diseases, such as sickle cell disease and β- thalassemia.

题目: 基于血红蛋白F的镰状细胞病基因治疗的研究进展.

摘要: 镰状细胞病(SCD)是一种单基因遗传病,严重威胁患者寿命和生活质量。本文从SCD的发病机制及基于胎儿血红蛋白F(HbF)的替代治疗入手,回顾了近年对BCL11A、ZBTB7A、KLF-1、c-MYB和SOX6等参与HbF基因表达调控的转录因子的研究进展,以及CRISPR/Cas9、TALEN、锌指核酸酶等基因编辑技术在该领域的应用,为SCD及β-地中海贫血等β-样血红蛋白病的新治疗方案的探索提供坚实的理论基础.

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