School of Veterinary Medicine, University of Wisconsin-Madison, Madison, WI, USA.
Vet Comp Oncol. 2012 Sep;10(3):174-83. doi: 10.1111/j.1476-5829.2011.00261.x. Epub 2011 Jan 31.
Combining drugs with known single-agent activity that lack overlapping dose-limiting toxicities (DLT) and exert antitumour activity through different mechanisms could improve clinical outcome. As toceranib and vinblastine meet these requisites, a phase I trial was performed in combination in dogs with mast cell tumours. The DLT for the simultaneous combination was neutropenia and the maximally tolerated dose was vinblastine (1.6 mg m(-2) every other week) concurrent with toceranib (3.25 mg kg(-1) PO, every other day). This represents greater than a 50% reduction in dose intensity for vinblastine (compared with single-agent use) and as such does not support this combination based on current drug combination paradigms. Although a strict adherence to dose paradigms speaks against the combination, evidence of significant activity (71% objective response) and enhanced myelosuppression suggest additive or synergistic activity. A prospective randomized evaluation comparing this combination with standard single-agent treatments would seem prudent to interrogate this potential.
将具有已知单一活性药物与缺乏重叠剂量限制毒性(DLT)的药物联合使用,并通过不同机制发挥抗肿瘤活性,可能会改善临床结果。由于toceranib 和长春碱符合这些要求,因此在患有肥大细胞瘤的犬中进行了联合的 I 期试验。同时联合使用的剂量限制毒性是中性粒细胞减少症,最大耐受剂量是长春碱(1.6 mg/m²,每两周一次)与 toceranib(3.25 mg/kg,每天两次)同时使用。这代表长春碱的剂量强度降低了 50%以上(与单药使用相比),因此基于当前的药物联合模式,不支持这种联合用药。尽管严格遵守剂量模式不利于联合用药,但有明显活性(71%的客观缓解率)和增强的骨髓抑制的证据表明存在相加或协同作用。为了探讨这种潜在可能性,似乎需要进行一项前瞻性随机评估,比较这种联合用药与标准单药治疗的效果。