慢性淋巴细胞白血病的靶向治疗

T. Kipps, M. Choi
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引用次数: 10

摘要

尽管普遍认为癌症治疗的进展将通过选择性靶向由负责肿瘤表型的突变癌基因编码的酶来实现,但慢性淋巴细胞白血病(CLL)患者治疗的最新进展却利用了其生物学知识。事实上,CLL细胞依赖于与肿瘤微环境中存在的细胞和可溶性因子的相互作用来增殖和存活。b细胞受体信号和趋化因子受体信号在其中起着重要作用。这些信号通路的阐明已经确定了药物的生理靶点,如伊鲁替尼,它抑制布鲁顿酪氨酸激酶并具有治疗效果。BCL2在CLL中高水平表达,可提高白血病细胞存活率,现已成为临床有效药物(如venetoclax)的致命弱点。在这里,我们讨论了这种靶向治疗的进展,并强调了其他疾病属性,如ROR1的独特表达,可以单独或与其他靶向治疗联合靶向临床获益。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Targeted Therapy in Chronic Lymphocytic Leukemia
Abstract Despite a prevailing view that advances in cancer therapy will come through selective targeting of enzymes encoded by mutated oncogenes responsible for the neoplastic phenotype, recent advances in the treatment of patients with chronic lymphocytic leukemia (CLL) have instead exploited knowledge of its biology. Indeed, CLL cells depend on interactions with cells and soluble factors present in the tumor microenvironment for proliferation and survival. B-cell receptor signaling and chemokine-receptor signaling play prominent roles. Elucidation of these signaling pathways has defined physiologic targets for drugs, such as ibrutinib, which inhibit Bruton tyrosine kinase and are therapeutically effective. The characteristic high-level expression of BCL2 in CLL that can enhance leukemia-cell survival has now become an Achilles heel targeted by clinically effective drugs such as venetoclax. Here we discuss advances in such targeted therapy and highlight other disease attributes, such as the distinctive expression of ROR1, which may be targeted for clinical benefit, alone or in combination with other targeted therapies.
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