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Dose dependent pharmacokinetics tissue distribution and anti-tumor efficacy of a humanized monoclonal antibody against DLL4 in mice

机译:抗DLL4的人源化单克隆抗体在小鼠中的剂量依赖性药代动力学组织分布和抗肿瘤功效

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摘要

Delta-like-4 ligand (DLL4) plays an important role in vascular development and is widely expressed on the vasculature of normal and tumor tissues. Anti-DLL4 is a humanized IgG1 monoclonal antibody against DLL4. The purpose of these studies was to characterize the pharmacokinetics (PK), tissue distribution, and anti-tumor efficacy of anti-DLL4 in mice over a range of doses. PK and tissue distribution of anti-DLL4 were determined in athymic nude mice after administration of single intravenous (IV) doses. In the tissue distribution study, radiolabeled anti-DLL4 (mixture of 125Iodide and 111Indium) was administered in the presence of increasing amounts of unlabeled anti-DLL4. Dose ranging anti-DLL4 anti-tumor efficacy was evaluated in athymic nude mice bearing MV522 human lung tumor xenografts. Anti-DLL4 had nonlinear PK in mice with rapid serum clearance at low doses and slower clearance at higher doses suggesting the involvement of target mediated clearance. Consistent with the PK data, anti-DLL4 was shown to specifically distribute to several normal tissues known to express DLL4 including the lung and liver. Maximal efficacy in the xenograft model was seen at doses ≥ 10 mg/kg when tissue sinks were presumably saturated, consistent with the PK and tissue distribution profiles. These findings highlight the importance of mechanistic understanding of antibody disposition to enable dosing strategies for maximizing efficacy.
机译:Delta-like-4配体(DLL4)在血管发育中起重要作用,并在正常组织和肿瘤组织的脉管系统中广泛表达。抗DLL4是针对DLL4的人源化IgG1单克隆抗体。这些研究的目的是表征抗DLL4在一定剂量范围内的小鼠的药代动力学(PK),组织分布和抗肿瘤功效。给予单次静脉内(IV)剂量后,在无胸腺裸鼠中测定抗DLL4的PK和组织分布。在组织分布研究中,在存在越来越多的未标记抗DLL4的情况下,使用了放射性标记的抗DLL4( 125 碘化物和 111 铟的混合物)。在携带MV522人肺肿瘤异种移植物的无胸腺裸鼠中评估了剂量范围的抗DLL4抗肿瘤功效。抗DLL4在小鼠中具有非线性PK,在低剂量时具有快速的血清清除率,在高剂量时具有较慢的清除率,表明参与了靶标介导的清除。与PK数据一致,抗DLL4已显示特异性分布于已知表达DLL4的几种正常组织,包括肺和肝。当组织汇沉饱和时,在≥10 mg / kg的剂量下,可以看到异种移植模型的最大功效,这与PK和组织分布特征一致。这些发现突出了对抗体配置的机械理解的重要性,以使剂量策略能够最大化疗效。

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