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Optimizing frontline therapy of CLL based on clinical and biological factors

机译:基于临床和生物因素的CLL优化前线治疗

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The heterogeneity of the clinical course of chronic lymphocytic leukemia (CLL) ranges from an indolent course, where patients do not require therapy for many years, to a very aggressive disease, where treatment is required soon after diagnosis and relapses may occur early. The improved tools for prognostication allow predicting the outcome of patients with increasing reliability. Some markers also allow selecting more specific therapies with improved activity in the presence of certain genetic or clinical features of CLL. Of these markers, TP53 dysfunction, age, the presence of comorbidities and the immunoglobulin heavy-chain variable region gene mutational status, or serum markers such as β_(2)-microglobulin have shown independent prognostic value in multiple prospective trials. During the last 10 years, multiple novel agents have become available. The advent of oral kinase inhibitors or Bcl-2 antagonists has provided highly effective options with acceptable toxicity. This manuscript summarizes the current evidence of the available treatment options and proposes an integrated algorithm for the frontline therapy of CLL.
机译:慢性淋巴细胞白血病(CLL)临床过程的异质性来自惰性课程,患者不需要治疗多年来,对一个非常侵略性的疾病,在诊断后很快需要治疗,可能会尽早发生治疗。预测的改进工具允许预测患者的结果增加。一些标记还允许在CLL的某些遗传或临床特征存在下选择更具体的疗法。在这些标志物中,TP53功能障碍,年龄,血管蛋白的存在和免疫球蛋白重链可变区基因突变状态,或血清标记物如β-(2)-microglobulin,在多次前瞻性试验中显示出独立的预后价值。在过去的10年中,多种新型药剂可用。口腔激酶抑制剂或BCL-2拮抗剂的出现提供了高效的选择,具有可接受的毒性。此手稿总结了可用治疗方案的当前证据,并提出了一种用于CLL的前线疗法的综合算法。

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    《Hematology》 |2017年第1期|共8页
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