AI Article Synopsis
- Thalassaemia stems from over 250 mutations in the beta globin gene, impacting hematopoietic stem cell differentiation and causing ineffective red blood cell production.
- The traditional focus on managing symptoms with transfusions and iron chelation therapy has hindered progress toward developing cell-based treatments, despite advancements in understanding the disease since the identification of the beta039 mutation in 1979.
- Recent progress in treating hematopoietic stem cell disorders emphasizes a 'target cell strategy,' suggesting a shift toward innovative treatments for thalassaemia that identify suitable candidates through risk stratification, highlighting its nature as a congenital HSC disorder.
Article Abstract
Thalassaemia, caused by over 250 mutations in the beta globin gene, changes the haematopoietic stem cell (HSC) differentiation, leading to ineffective erythropoiesis. This Wider Perspective article overlooks its underlying nature as a benign HSC disorder with a significant impact on the erythroid cell lineage. The simplicity of managing symptoms through transfusions and iron chelation therapy has shifted the focus away from the development of cell-based treatments. The identification of the beta039 mutation by Chang and Kan in 1979 marked a turning point, suggesting as main approach the molecular level by correcting the beta globin chain imbalances through gene insertion and editing. However, challenges of technology have delayed the implementation of these strategies for over four decades. In contrast, the past two decades have witnessed significant advances in the treatment of HSC disorders of the myeloid clone which are driven by a 'target cell strategy'. Many current and innovative treatments for thalassaemia are now adopting this approach, highlighting the importance of identifying suitable candidates through risk stratification. This manuscript explores the evolving understanding of thalassaemia syndromes as congenital HSC disorders of the erythroid clone and examines the implications of this perspective for the development of future treatments.
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| http://dx.doi.org/10.1111/bjh.19919 | DOI Listing |
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