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A combined approach with rituximab plus anti-TRAIL-R agonistic antibodies for the treatment of haematological malignancies.

机译:利妥昔单抗加抗TRAIL-R激动抗体的联合治疗血液系统恶性肿瘤的方法。

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摘要

Molecular targeted therapies have changed the landscape of cancer research. Agonistic monoclonal antibodies (MoAbs) targeting TRAIL-death receptors (TRAIL-Rs) have been developed and currently used in clinical trials. Binding of such antibodies to TRAIL-R1 and TRAIL-R2 results in death inducing signalling complex (DISC) formation and induction of apoptosis, which represents a natural mechanism of cell growth control and an ideal target for drug development. These novel fully humanized compounds have been associated with conventional chemotherapy in the treatment of advanced solid malignancies, including different types of lymphoma. Here we outline the rationale and potential of a new molecular-based strategy combining agonistic anti-TRAIL-death receptor monoclonal antibodies plus the pioneer of the new biological frontiers of cancer therapy: rituximab.
机译:分子靶向疗法改变了癌症研究的前景。针对TRAIL-死亡受体(TRAIL-Rs)的激动性单克隆抗体(MoAbs)已经开发出来,目前正在临床试验中使用。此类抗体与TRAIL-R1和TRAIL-R2的结合导致死亡诱导信号复合物(DISC)的形成和细胞凋亡的诱导,这代表了细胞生长控制的自然机制和药物开发的理想靶标。这些新型的完全人源化的化合物已与常规化疗相关联,可用于治疗晚期实体恶性肿瘤,包括不同类型的淋巴瘤。在这里,我们概述了一种新的基于分子的策略的原理和潜力,该策略结合了激动性的抗TRAIL-死亡受体单克隆抗体以及癌症治疗新的生物领域的先驱者:利妥昔单抗。

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