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抗原依赖性清除对抗肝素结合表皮生长因子样生长因子(HB-EGF)单克隆抗体药代动力学的影响。

Effect of antigen-dependent clearance on pharmacokinetics of anti-heparin-binding EGF-like growth factor (HB-EGF) monoclonal antibody.

作者信息

Kasai Noriyuki, Yoshikawa Yukitaka, Enokizono Junichi

机构信息

a R&D Division, Kyowa Hakko Kirin Co. Ltd., Shimotogari, Nagaizumi-cho , Sunto-gun , Shizuoka , Japan.

出版信息

MAbs. 2014;6(5):1220-8. doi: 10.4161/mabs.29792. Epub 2014 Nov 1.

Abstract

Heparin-binding EGF-like growth factor (HB-EGF) is a member of the EGF family and is an important therapeutic target in some types of human cancers. KM3566 is a mouse anti-HB-EGF monoclonal antibody that neutralizes HB-EGF activity by inhibiting the binding of HB-EGF to its receptors. Based on the results of our pharmacokinetics study, a humanized derivative antibody, KHK2866, is rapidly cleared from serum and shows nonlinear pharmacokinetics in cynomolgus monkeys. In this study, we examined the antigen-dependent clearance of an anti-HB-EGF monoclonal antibody in vivo and in vitro in order to pharmacokinetically explain the rapid elimination of KHK2866. We revealed tumor size-dependent clearance of KM3566 in in vivo studies and obtained good fits between the observed and simulated concentrations of KM3566 based on the two-compartment with a saturable route of clearance model. Furthermore, in vivo imaging analyses demonstrated tumor-specific distribution of KM3566. We then confirmed rapid internalization and distribution to lysosome of KM3566 at a cellular level. Moreover, we revealed that the amounts of HB-EGF on cell surface membrane were maintained even while HB-EGF was internalized with KM3566. Recycled or newly synthesized HB-EGF, therefore, may contribute to a consecutive clearance of KM3566, which could explain a rapid clearance from serum. These data suggested that the rapid elimination in pharmacokinetics of KM3566 is due to antigen-dependent clearance. Given that its antigen is expressed in a wide range of normal tissue, it is estimated that the rapid elimination of KHK2866 from cynomolgus monkey serum is caused by antigen-dependent clearance.

摘要

肝素结合表皮生长因子样生长因子(HB-EGF)是表皮生长因子(EGF)家族的一员,是某些类型人类癌症中的重要治疗靶点。KM3566是一种小鼠抗HB-EGF单克隆抗体,通过抑制HB-EGF与其受体的结合来中和HB-EGF活性。根据我们的药代动力学研究结果,一种人源化衍生抗体KHK2866在血清中迅速清除,在食蟹猴中呈现非线性药代动力学。在本研究中,我们在体内和体外研究了抗HB-EGF单克隆抗体的抗原依赖性清除,以便从药代动力学角度解释KHK2866的快速消除。我们在体内研究中揭示了KM3566的肿瘤大小依赖性清除,并基于具有饱和清除途径的二室模型,使观察到的和模拟的KM3566浓度之间获得了良好的拟合。此外,体内成像分析证明了KM3566的肿瘤特异性分布。然后,我们在细胞水平上证实了KM3566的快速内化和向溶酶体的分布。此外,我们发现即使HB-EGF与KM3566一起内化,细胞表面膜上的HB-EGF量仍能维持。因此,回收或新合成的HB-EGF可能有助于KM3566的持续清除,这可以解释其从血清中的快速清除。这些数据表明,KM3566药代动力学中的快速消除是由于抗原依赖性清除。鉴于其抗原在广泛的正常组织中表达,据估计食蟹猴血清中KHK2866的快速消除是由抗原依赖性清除引起的。

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