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We do still transplant CML, don’t we?

机译:我们仍在移植CML,不是吗?

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The remarkable clinical activity of tyrosine kinase inhibitors (TKIs) in chronic myeloid leukemia (CML) has transformed patient outcome. Consequently, allogeneic stem cell transplantation (allo-SCT) is no longer the only treatment modality with the ability to deliver long-term survival. In contrast to the central position it held in the treatment algorithm 20 years ago, allografting is now largely reserved for patients with either chronic-phase disease resistant to TKI therapy or advanced-phase disease. Over the same period, progress in transplant technology, principally the introduction of re-duced intensity conditioning regimens coupled with increased donor availability, has extended transplant options in patients with CML whose outcome can be predicted to be poor if they are treated with TKIs alone. Consequently, transplantationisstillavitallyimportant,potentiallycurativetherapeuticmodalityinselectedpatientswitheitherchronic-or advanced-phase CML. The major causes of transplant failure in patients allografted for CML are transplant toxicity and disease relapse. A greater understanding of the distinct contributions made by various factors such as patient fitness, patient-donor HLA disparity, conditioning regimen intensity, and transplant toxicity increasingly permits personalized transplant decision making. At the same time, advances in the design of conditioning regimens coupled with the use of adjunctive posttransplant cellular and pharmacologic therapies provide opportunities for reducing the risk of disease relapse. The role of SCT in the management of CML will grow in the future because of an increase in disease prevalence and because of continued improvements in transplant outcome.
机译:酪氨酸激酶抑制剂(TKIs)在慢性粒细胞白血病(CML)中的卓越临床活性已经改变了患者的预后。因此,同种异体干细胞移植(allo-SCT)不再是具有长期生存能力的唯一治疗方式。与20年前在治疗算法中所占据的中心地位相反,同种异体移植现在主要保留给对TKI治疗耐药的慢性期疾病或晚期疾病的患者。在同一时期,移植技术的进步,主要是降低强度调节方案的引入以及增加的供体可利用性,已经扩大了CML患者的移植选择范围,如果仅使用TKIs治疗,其预后将很差。因此,对于某些患有慢性或晚期CML的患者,移植仍然是重要的,潜在的治疗方法。同种异体移植CML患者移植失败的主要原因是移植毒性和疾病复发。对各种因素(例如患者的身体素质,患者与供体的HLA差异,调节方案强度和移植毒性)做出的独特贡献的更深入了解,逐渐使个性化移植决策成为可能。同时,调节方案设计的进展以及移植后辅助细胞和药物疗法的使用为降低疾病复发的风险提供了机会。由于疾病患病率的增加以及移植结果的持续改善,SCT在CML管理中的作用将在未来增长。

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