急性白血病治疗的终点是什么?旧的定义和新的挑战

B. Douglas Smith , Judith E. Karp
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引用次数: 5

摘要

急性白血病在多个层面上都是复杂的疾病,在过去的30年里,实验室的努力集中在更好地理解其分子基础及其干细胞生物学。我们现在有一系列的技术进步,使我们能够通过与临床行为直接相关的分子谱来表征个体白血病,检测最小的残留疾病,并开始基于分子考虑制定“靶向”治疗策略。围绕这一任务有许多挑战:首先,如何将这些药物与传统化疗药物结合或相互结合,以最大限度地杀死白血病细胞并提高治愈率;其次,如何在具有潜在治疗意图的最小残留疾病中使用这些靶向药物;第三,对于无法耐受或不太可能从积极治疗中获益的患者,如何使用一种或多种这些药物来减少肿瘤体积,并允许一些正常骨髓功能的恢复或诱导白血病克隆的形态和功能分化,以克服白血病相关的骨髓衰竭;最后,如何测量这些药物在分子和细胞生物学水平上的作用,以与甚至可能预测整体临床结果相关的方式。宿主生物学固有的异质性使这些挑战进一步复杂化;疾病病原学和生物学;宿主、疾病和治疗之间的相互作用最终决定了个体的临床结果。为此,我们将讨论围绕新临床试验设计和临床相关分子终点发展的选定问题,这些问题可能促进新治疗方法的发展,从而改善成人急性白血病患者的前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
What Are the Endpoints of Therapy for Acute Leukemias? Old Definitions and New Challenges

Acute leukemias are complex diseases on multiple levels, and laboratory efforts over the past 3 decades have focused on better understanding of the molecular underpinnings and their stem cell biology. We now have a panoply of technologic advances that allow us to characterize individual leukemias by molecular profiles that relate directly to clinical behavior, to detect minimal residual disease, and to begin to develop “targeted” therapeutic strategies based on molecular considerations. There are a number of challenges surrounding this task: first, how to combine these agents with traditional chemotherapeutics and/or with each other to maximize leukemic cell kill and increase the cure rate; second, how to use these targeted agents in the minimal residual disease with potential curative intent; third, for patients unable to tolerate or unlikely to benefit from aggressive approaches, how to use one or more of these agents to reduce tumor bulk and either permit some restoration of normal marrow function or induce morphologic and functional differentiation of the leukemic clone to overcome the leukemia-associated bone marrow failure; and lastly, how to measure the effects of these agents on the molecular and cellular biologic levels in ways that correlate with and might even predict overall clinical outcome. These challenges are further complicated by the inherent heterogeneity in host biology; disease etiology and biology; and interactions among host, disease, and treatment that ultimately determine individual clinical outcomes. Toward this end, we will discuss selected issues surrounding new clinical trial designs and the development of clinically relevant molecular endpoints that might facilitate the development of new treatment approaches that will improve the outlook for adults with acute leukemias.

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