Immunogenicity of panitumumab in combination chemotherapy clinical trials.

Dohan Weeraratne, Alin Chen, Jason J Pennucci, Chi-Yuan Wu, Kathy Zhang, Jacqueline Wright, Juan José Pérez-Ruixo, Bing-Bing Yang, Arunan Kaliyaperumal, Shalini Gupta, Steven J Swanson, Narendra Chirmule, Marta Starcevic
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引用次数: 22

Abstract

Background: Panitumumab is a fully human antibody against the epidermal growth factor receptor that is indicated for the treatment of metastatic colorectal cancer (mCRC) after disease progression on standard chemotherapy. The purpose of this analysis was to examine the immunogenicity of panitumumab and to evaluate the effect of anti-panitumumab antibodies on pharmacokinetic and safety profiles in patients with mCRC receiving panitumumab in combination with oxaliplatin- or irinotecan-based chemotherapies.

Methods: Three validated assays (two screening immunoassays and a neutralizing antibody bioassay) were used to detect the presence of anti-panitumumab antibodies in serum samples collected from patients enrolled in four panitumumab combination chemotherapy clinical trials. The impact of anti-panitumumab antibodies on pharmacokinetic and safety profiles was analyzed using population pharmacokinetic analysis and descriptive statistics, respectively.

Results: Of 1124 patients treated with panitumumab in combination with oxaliplatin- or irinotecan-based chemotherapy with postbaseline samples available for testing, 20 (1.8%) patients developed binding antibodies and 2 (0.2%) developed neutralizing antibodies. The incidence of anti-panitumumab antibodies was similar in patients with tumors expressing wild-type or mutant KRAS and in patients receiving oxaliplatin- or irinotecan-based chemotherapies. No evidence of an altered pharmacokinetic or safety profile was found in patients who tested positive for anti-panitumumab antibodies.

Conclusions: The immunogenicity of panitumumab in the combination chemotherapy setting was infrequent and similar to the immunogenicity observed in the monotherapy setting. Panitumumab immunogenicity did not appear to alter pharmacokinetic or safety profiles. This low rate of immunogenicity may be attributed to the fully human nature of panitumumab.

Abstract Image

Abstract Image

帕尼单抗在联合化疗临床试验中的免疫原性。
背景:Panitumumab是一种针对表皮生长因子受体的全人源抗体,用于标准化疗后疾病进展的转移性结直肠癌(mCRC)的治疗。本分析的目的是检查帕尼珠单抗的免疫原性,并评估抗帕尼珠单抗抗体对接受帕尼珠单抗联合奥沙利铂或伊立替康化疗的mCRC患者药代动力学和安全性的影响。方法:采用三种验证方法(两种筛选免疫测定法和一种中和抗体生物测定法)检测4项帕尼单抗联合化疗临床试验患者血清样本中抗帕尼单抗抗体的存在。抗帕尼单抗抗体对药代动力学和安全性的影响分别采用群体药代动力学分析和描述性统计进行分析。结果:在1124例接受帕尼单抗联合奥沙利铂或伊立替康化疗的患者中,有基线后样本可用于检测,20例(1.8%)患者产生结合抗体,2例(0.2%)患者产生中和抗体。在表达野生型或突变型KRAS的肿瘤患者和接受奥沙利铂或伊立替康化疗的患者中,抗帕尼单抗抗体的发生率相似。在抗帕尼单抗抗体检测阳性的患者中,没有发现药代动力学或安全性改变的证据。结论:帕尼珠单抗在联合化疗环境中的免疫原性少见,且与单药治疗环境中观察到的免疫原性相似。帕尼珠单抗的免疫原性似乎没有改变药代动力学或安全性。这种低免疫原性可能归因于帕尼单抗的完全人性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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