Streamlined downstream process for efficient and sustainable (Fab')₂ antivenom preparation.

IF 1.8 3区医学 Q4 TOXICOLOGY

Journal of Venomous Animals and Toxins Including Tropical Diseases Pub Date : 2020-07-27 eCollection Date: 2020-01-01 DOI:10.1590/1678-9199-jvatitd-2020-0025

Tihana Kurtović, Marija Brgles, Maja Lang Balija, Stephanie Steinberger, Dora Sviben, Martina Marchetti-Deschmann, Beata Halassy

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引用次数: 0

Abstract

Background: Antivenoms are the only validated treatment against snakebite envenoming. Numerous drawbacks pertaining to their availability, safety and efficacy are becoming increasingly evident due to low sustainability of current productions. Technological innovation of procedures generating therapeutics of higher purity and better physicochemical characteristics at acceptable cost is necessary. The objective was to develop at laboratory scale a compact, feasible and economically viable platform for preparation of equine F(ab')₂ antivenom against Vipera ammodytes ammodytes venom and to support it with efficiency data, to enable estimation of the process cost-effectiveness.

Methods: The principle of simultaneous caprylic acid precipitation and pepsin digestion has been implemented into plasma downstream processing. Balance between incomplete IgG breakdown, F(ab')₂ over-digestion and loss of the active drug's protective efficacy was achieved by adjusting pepsin to a 1:30 substrate ratio (w/w) and setting pH at 3.2. Precipitation and digestion co-performance required 2 h-long incubation at 21 °C. Final polishing was accomplished by a combination of diafiltration and flow-through chromatography. In vivo neutralization potency of the F(ab')₂ product against the venom's lethal toxicity was determined.

Results: Only three consecutive steps, performed under finely tuned conditions, were sufficient for preservation of the highest process recovery with the overall yield of 74%, comparing favorably to others. At the same time, regulatory requirements were met. Final product was aggregate- and pepsin-free. Its composition profile was analyzed by mass spectrometry as a quality control check. Impurities, present in minor traces, were identified mostly as IgG/IgM fragments, contributing to active drug. Specific activity of the F(ab')₂ preparation with respect to the plasma was increased 3.9-fold.

Conclusion: A highly streamlined mode for production of equine F(ab')₂ antivenom was engineered. In addition to preservation of the highest process yield and fulfillment of the regulatory demands, performance simplicity and rapidity in the laboratory setting were demonstrated. Suitability for large-scale manufacturing appears promising.

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简化下游流程，实现高效、可持续的 (Fab')2 抗蛇毒血清制备。

背景：抗蛇毒血清是治疗蛇咬伤的唯一有效方法。由于目前生产的抗蛇毒血清可持续性较低，其可用性、安全性和有效性方面的许多缺点正变得越来越明显。有必要进行技术创新，以可接受的成本生产出纯度更高、理化特性更好的治疗药物。我们的目标是在实验室规模上开发一个紧凑、可行且经济上可行的平台，用于制备针对蝰蛇毒液的马 F(ab')2 抗蛇毒血清，并提供效率数据支持，以估算工艺的成本效益：方法：在血浆下游处理过程中采用了辛酸沉淀和胃蛋白酶消化同时进行的原理。通过将胃蛋白酶的底物比例（w/w）调整为 1:30，并将 pH 值设定为 3.2，实现了 IgG 不完全分解、F(ab')2 过度消化和活性药物保护效力损失之间的平衡。沉淀和消化的共同作用需要在 21 °C 下培养 2 小时。最后通过重滤和流动层析完成抛光。测定了 F(ab')2 产物对毒液致死毒性的体内中和效力：结果：在微调的条件下，只需连续进行三个步骤，就能保持最高的工艺回收率，总产率高达 74%，与其他方法相比毫不逊色。与此同时，还满足了法规要求。最终产品不含聚合体和胃蛋白酶。作为质量控制检查，对其成分进行了质谱分析。经鉴定，杂质含量极低，主要为 IgG/IgM 片段，属于活性药物。与血浆相比，F(ab')2 制剂的特异性活性提高了 3.9 倍：结论：我们设计出了一种高度简化的马 F(ab')2 抗蛇毒血清生产模式。结论：我们设计出了一种高度简化的马 F（ab'）2 抗血清生产模式。除了能保持最高的工艺产量和满足监管要求外，该模式还能在实验室环境中实现简单、快速的性能。大规模生产的适用性似乎很有希望。

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

Journal of Venomous Animals and Toxins Including Tropical Diseases 医学-毒理学

CiteScore

4.80

自引率

8.30%

发文量

审稿时长

6-12 weeks

期刊介绍： Journal of Venomous Animals and Toxins including Tropical Diseases (JVATiTD) is a non-commercial academic open access publication dedicated to research on all aspects of toxinology, venomous animals and tropical diseases. Its interdisciplinary content includes original scientific articles covering research on toxins derived from animals, plants and microorganisms. Topics of interest include, but are not limited to:systematics and morphology of venomous animals;physiology, biochemistry, pharmacology and immunology of toxins;epidemiology, clinical aspects and treatment of envenoming by different animals, plants and microorganisms;development and evaluation of antivenoms and toxin-derivative products;epidemiology, clinical aspects and treatment of tropical diseases (caused by virus, bacteria, algae, fungi and parasites) including the neglected tropical diseases (NTDs) defined by the World Health Organization.