Acute Promyelocytic Leukemia (APL): A Review of the Classic and Emerging Target Therapies towards Molecular Heterogeneity

Tâmara Dauare de Almeida, F. Evangelista, A. Sabino
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引用次数: 2

Abstract

The occurrence of severe bleeding syndrome because of the PML-RARα fusion protein is a life-threatening event in APL. This protein destabilizes homeostasis, maturation, remodeling, and tissue regeneration in addition to hampering the maintenance and differentiation of hematopoietic cells into different lineages, fixing cells in the promyelocyte stage. APL is a classic example of how effective targeted therapy is and, therefore, how important the use of such therapy is to the overall survival of patients, which in this case is represented by the use of ATRA/ATO. Despite that, about 10% of cases of APL patients demonstrate resistance to treatment. Facing this scenario, we point out promising target therapies such as those recommended by the NCCN and Leukemia Net. Since this is such a heterogeneous molecular disease, it is of great importance to understand how important combined chemotherapy, target therapy, immune-based therapy, and combined therapies are in the survival of these APL patients.
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急性早幼粒细胞白血病(APL):经典和新兴靶向治疗分子异质性的综述
PML-RARα融合蛋白引起的严重出血综合征的发生是APL患者生命危险的事件。除了阻碍造血细胞向不同谱系的维持和分化外,该蛋白还破坏稳态、成熟、重塑和组织再生,将细胞固定在早幼粒细胞阶段。APL是一个典型的例子,说明靶向治疗是多么有效,因此,使用这种治疗对患者的总体生存是多么重要,在这种情况下,ATRA/ATO的使用代表了这一点。尽管如此,大约10%的APL患者表现出对治疗的耐药性。面对这种情况,我们指出有希望的靶向治疗,如NCCN和白血病网推荐的那些。由于这是一种异质性的分子疾病,因此了解联合化疗、靶向治疗、免疫治疗和联合治疗在这些APL患者的生存中的重要性是非常重要的。
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