Optimized Methods for Analytical and Functional Comparison of Biosimilar mAb Drugs: A Case Study for Avastin, Mvasi, and Zirabev

IF 2.3 Q3 PHARMACOLOGY & PHARMACY

Scientia Pharmaceutica Pub Date : 2022-05-31 DOI:10.3390/scipharm90020036

Büşra Gürel, Eda Çapkın, A. Parlar, Aylin Özkan, Meltem Çorbacıoğlu, Duygu E. Dağlıkoca, Meral Yüce

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引用次数: 6

Abstract

Bevacizumab is a humanized therapeutic monoclonal antibody used to reduce angiogenesis, a hallmark of cancer, by binding to VEGF-A. Many pharmaceutical companies have developed biosimilars of Bevacizumab in the last decade. The official reports provided by the FDA and EMA summarize the analytical performance of biosimilars as compared to the originators without giving detailed analytical procedures. In the current study, several key methods were optimized and reported for analytical and functional comparison of bevacizumab originators (Avastin, Altuzan) and approved commercial biosimilars (Zirabev and Mvasi). This case study presents a comparative analysis of a set of biosimilars under optimized analytical conditions for the first time in the literature. The chemical structure of all products was analyzed at intact protein and peptide levels by high-resolution mass spectrometry; the major glycoforms and posttranslational modifications, including oxidation, deamidation, N-terminal PyroGlu addition, and C-terminal Lys clipping, were compared. The SPR technique was used to reveal antigen and some receptor binding kinetics of all products, and the ELISA technique was used for C1q binding affinity analysis. Finally, the inhibition performance of the samples was evaluated by an MTS-based proliferation assay in vitro. Major glycoforms were similar, with minor differences among the samples. Posttranslational modifications, except C-terminal Lys, were determined similarly, while unclipped Lys percentage was higher in Zirabev. The binding kinetics for VEGF, FcRn, FcγRIa, and C1q were similar or in the value range of originators. The anti-proliferative effect of Zirabev was slightly higher than the originators and Mvasi. The analysis of biosimilars under the same conditions could provide a new aspect to the literature in terms of the applied analytical techniques. Further studies in this field would be helpful to better understand the inter-comparability of the biosimilars.

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生物类似mAb药物分析和功能比较的优化方法：以阿瓦斯汀、Mvasi和Zirabev为例

贝伐单抗是一种人源化治疗性单克隆抗体，用于通过与VEGF-a结合来减少血管生成，这是癌症的标志。在过去的十年里，许多制药公司已经开发出贝伐单抗的生物仿制药。美国食品药品监督管理局和欧洲药品管理局提供的官方报告总结了生物仿制药与原始药物相比的分析性能，但没有给出详细的分析程序。在目前的研究中，优化并报道了贝伐单抗起始药（Avastin、Altuzan）和已批准的商业生物仿制药（Zirabev和Mvasi）的分析和功能比较的几种关键方法。本案例研究在文献中首次对一组生物仿制药在优化分析条件下进行了比较分析。通过高分辨率质谱法在完整的蛋白质和肽水平上分析所有产物的化学结构；比较了主要的糖型和翻译后修饰，包括氧化、脱酰胺、N-末端PyroGlu添加和C-末端Lys剪切。SPR技术用于揭示所有产物的抗原和一些受体结合动力学，ELISA技术用于C1q结合亲和力分析。最后，通过基于MTS的体外增殖测定来评估样品的抑制性能。主要糖型相似，但样本之间的差异较小。除C末端Lys外，翻译后修饰的测定结果相似，而Zirabev中未剪切的Lys百分比更高。VEGF、FcRn、FcγRIa和C1q的结合动力学相似或在起始物的值范围内。Zirabev的抗增殖作用略高于始发者和Mvasi。在相同条件下对生物仿制药的分析可以在应用分析技术方面为文献提供一个新的方面。该领域的进一步研究将有助于更好地了解生物仿制药的相互可比性。

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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来源期刊

Scientia Pharmaceutica Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science

CiteScore

4.60

自引率

4.00%

发文量

审稿时长

10 weeks