双特异性抗体MDX-H210与干扰素γ联合给药时的药代动力学-药效学关系：一项针对过度表达HER-2/neu的晚期癌症患者的多剂量I期研究。

Pharmacokinetic-pharmacodynamic relationships of the bispecific antibody MDX-H210 when administered in combination with interferon gamma: a multiple-dose phase-I study in patients with advanced cancer which overexpresses HER-2/neu.

作者信息

Lewis L D, Cole B F, Wallace P K, Fisher J L, Waugh M, Guyre P M, Fanger M W, Curnow R T, Kaufman P A, Ernstoff M S

机构信息

Department of Medicine, Dartmouth Medical School and The Norris Cotton Cancer Center, Lebanon, NH 03756, USA.

出版信息

J Immunol Methods. 2001 Feb 1;248(1-2):149-65. doi: 10.1016/s0022-1759(00)00355-0.

DOI:10.1016/s0022-1759(00)00355-0

PMID:11223076

Abstract

INTRODUCTION

MDX-H210 is a Fab'xFab' bispecific antibody (BsAb) constructed chemically by crosslinking Fab' mAb 520C9 (anti-HER-2/neu) and Fab' mAbH22 (anti-CD64).

STUDY DESIGN AND OBJECTIVES

This was a dose escalation study of intravenous MDX-H210 (1-70 mg/m(2)), preceded 24 h beforehand by subcutaneous IFNgamma (50 microg/m(2) to up-regulate FcgammaRI) administered three times a week for 3 weeks. We investigated the pharmacokinetic-pharmacodynamic relationships between MDX-H210 C(max) and AUC and (i) MDX-H210 binding to peripheral blood monocytes and neutrophils, (ii) the peak plasma G-CSF, IL-6, IL-8 and TNFalpha concentrations, and (iii) the observed clinical toxicity.

RESULTS

23 patients (19F:4M; median age 51.5; range 25-72 y) with advanced HER-2/neu positive cancers (19 breast, three prostate and one lung) were studied. Plasma MDX-H210 concentrations over time, circulating numbers of monocytes and neutrophils, percent saturation of monocyte and neutrophil FcgammaRI, and plasma concentrations over time of G-CSF, IL-6, IL-8 and TNFalpha were measured and clinical toxicity monitored. The E(max) pharmacodynamic model best fitted the relationship of MDX-H210 C(max) and the maximum percent saturation of both monocytes (E(max)=74.6; EC(50)=0.9 microg/ml) and neutrophils (E(max)=66.2; EC(50)=2.3 microg/ml) on the first day of treatment. On the last day of treatment, day 19, these parameters were E(max)=57.0% and EC(50)=0.46 microg/ml for monocytes and E(max)=61.9% and EC(50)=0.26 microg/ml for neutrophils. No positive relationship was defined between the log MDX-H210 C(max) and the log peak plasma IL-6, G-CSF, TNF or IL-8 concentrations on day 1. On day 19 these plasma cytokine concentrations were undetectable post MDX-H210 therapy. There was no consistent relationship between MDX-H210 C(max) and the observed clinical toxicities.

CONCLUSIONS

These data suggest that MDX-H210 C(max) and AUC could be related by the E(max) model to maximum percent FcgammaRI saturation on circulating monocytes and neutrophils in the patients studied. After day 1, the post MDX-H210 therapy cytokine response attenuated over time, consistent with desensitization. We did not find a relationship between log MDX-H210 C(max) and peak plasma cytokine concentrations or clinical toxicities.

摘要

引言

MDX-H210是一种通过交联Fab'mAb 520C9（抗HER-2/neu）和Fab'mAbH22（抗CD64）化学构建的Fab'xFab'双特异性抗体（BsAb）。

研究设计与目的

这是一项静脉注射MDX-H210（1-70mg/m²）的剂量递增研究，在给药前24小时皮下注射IFNγ（50μg/m²以上调FcγRI），每周三次，共3周。我们研究了MDX-H210的Cmax和AUC与以下各项之间的药代动力学-药效学关系：（i）MDX-H210与外周血单核细胞和中性粒细胞的结合；（ii）血浆中G-CSF、IL-6、IL-8和TNFα的峰值浓度；（iii）观察到的临床毒性。

结果

对23例HER-2/neu阳性晚期癌症患者（19例女性，4例男性；中位年龄51.5岁；范围25-72岁）进行了研究，其中19例为乳腺癌，3例为前列腺癌，1例为肺癌。测量了MDX-H210随时间的血浆浓度、单核细胞和中性粒细胞的循环数量、单核细胞和中性粒细胞FcγRI的饱和百分比以及G-CSF、IL-6、IL-8和TNFα随时间的血浆浓度，并监测了临床毒性。E(max)药效学模型最能拟合治疗第一天MDX-H210的Cmax与单核细胞（E(max)=74.6；EC(50)=0.9μg/ml）和中性粒细胞（E(max)=66.2；EC(50)=2.3μg/ml）的最大饱和百分比之间的关系。在治疗的最后一天，即第19天，单核细胞的这些参数为E(max)=57.0%和EC(50)=0.46μg/ml，中性粒细胞为E(max)=61.9%和EC(50)=0.26μg/ml。在第1天，MDX-H210的log Cmax与血浆中IL-6、G-CSF、TNF或IL-8的log峰值浓度之间未发现正相关关系。在MDX-H210治疗后第19天，这些血浆细胞因子浓度无法检测到。MDX-H210的Cmax与观察到的临床毒性之间没有一致的关系。

结论

这些数据表明，在本研究的患者中，MDX-H210的Cmax和AUC可通过E(max)模型与循环单核细胞和中性粒细胞上FcγRI的最大饱和百分比相关。在第1天之后，MDX-H210治疗后的细胞因子反应随时间减弱，与脱敏一致。我们未发现MDX-H210的log Cmax与血浆细胞因子峰值浓度或临床毒性之间的关系。