加州大学圣地亚哥分校精准医学诊所新型药物组合中3种靶向药物的剂量

Mina Nikanjam, Jose Tinajero, Mary McGann, Jerry Li, Jincheng Yang, Felicity Shen, Jason K Sicklick, Shumei Kato, Edmund Capparelli, Razelle Kurzrock
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引用次数: 0

摘要

背景:晚期和转移性肿瘤基因组图谱的多样性要求基于与每种肿瘤相关的基因组特征进行联合治疗。确定新型肿瘤药物组合的安全和耐受剂量对于精准医疗方法至关重要,但也可能需要减少剂量。曲美替尼、帕博西尼和依维莫司是我们精准医学诊所最常用的新组合靶向治疗。目的:评价曲美替尼、帕博西尼和依维莫司与其他药物联合治疗晚期或转移性实体瘤的安全性和耐受性。方法:这项回顾性研究纳入了2011年12月至2018年7月在加州大学圣地亚哥分校接受曲美替尼、依维莫司或帕博西尼加其他治疗作为新组合的一部分的晚期或转移性实体瘤成年患者。如果患者接受曲美替尼、依维莫司或帕博西尼的标准组合,如达非尼加曲美替尼、依维莫司加氟维司汀、依维莫司加来曲唑、帕博西尼加来曲唑,则患者被排除在外。通过审查电子病历确定剂量和不良事件。安全、耐受的联合用药剂量定义为耐受至少1个月,无临床显著的严重不良事件。结果:71例接受曲美替尼治疗的患者中有76%,48例接受依维莫司治疗的患者中有88%,41例接受帕博西尼治疗的患者中有73%在与其他治疗联合使用时确定了安全、耐受的剂量。对于有临床显著不良事件的患者,30%的曲美替尼接受者、17%的依维莫司接受者和45%的帕博西尼接受者尝试减少剂量。当与其他疗法联合使用时,曲美替尼、帕博西尼和依维莫司的最佳剂量低于标准的单药剂量:曲美替尼为每日1mg;依维莫司每日5毫克;每天75毫克,服用帕博西尼3周,停1周。值得注意的是,依维莫司不能在这些剂量下与曲美替尼同时使用。结论:安全且耐受的新型联合疗法,包括曲美替尼、依维莫司或帕博西尼,对于精准医学方法是可行的。然而,无论是本研究的结果还是以往的研究结果都不能支持依维莫司与曲美替尼联合使用,即使是减少剂量。
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Dosing of 3 Targeted Agents in Novel Drug Combinations Used at the Precision Medicine Clinic of the University of California San Diego.

Background: The diversity in the genomic landscape of advanced and metastatic tumors calls for combination therapies based on the genomic signature associated with each tumor. Determining safe and tolerable doses for novel combinations of oncology drugs is essential for a precision medicine approach, but can also require dose reductions. Trametinib, palbociclib, and everolimus are among the targeted therapies most often used in novel combinations at our precision medicine clinic.

Objective: To evaluate the safe, tolerable dosing of trametinib, palbociclib, and everolimus when used as part of novel combinations with other agents for the treatment of advanced or metastatic solid tumors.

Methods: This retrospective study included adult patients with advanced or metastatic solid tumors who received trametinib, everolimus, or palbociclib plus other therapies as a part of novel combinations between December 2011 and July 2018 at the University of California San Diego. Patients were excluded if they received trametinib, everolimus, or palbociclib in standard combinations, such as dabrafenib plus trametinib, everolimus plus fulvestrant, everolimus plus letrozole, and palbociclib plus letrozole. Dosing and adverse events were determined through a review of the electronic medical records. A safe, tolerable drug combination dose was defined as being tolerated for at least 1 month, with no clinically significant serious adverse events.

Results: A safe, tolerable dose was determined for 76% of the 71 patients who received trametinib, 88% of the 48 patients who received everolimus, and 73% of the 41 patients receiving palbociclib when used in combination with other therapies. For patients with clinically significant adverse events, dose reductions were attempted in 30% of the trametinib recipients, in 17% of everolimus recipients, and in 45% of palbociclib recipients. When used in combination with other therapies, the optimal dosing of trametinib, palbociclib, and everolimus was lower than the standard single-agent dosing: it was 1 mg daily for trametinib; 5 mg daily for everolimus; and 75 mg daily, for 3 weeks on and 1 week off for palbociclib. Of note, everolimus could not be given concomitantly with trametinib at these doses.

Conclusion: Safe and tolerable dosing of novel combination therapies that includes trametinib, everolimus, or palbociclib is feasible for a precision medicine approach. However, neither results from this study nor results from previous studies could support the use of everolimus in combination with trametinib, even at reduced doses.

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