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一种用于在毕赤酵母中临床级生产HIV抑制剂5P12-RANTES的可扩展低成本cGMP工艺。

A scalable low-cost cGMP process for clinical grade production of the HIV inhibitor 5P12-RANTES in Pichia pastoris.

作者信息

Cerini Fabrice, Gaertner Hubert, Madden Knut, Tolstorukov Ilya, Brown Scott, Laukens Bram, Callewaert Nico, Harner Jay C, Oommen Anna M, Harms John T, Sump Anthony R, Sealock Robert C, Peterson Dustin J, Johnson Scott K, Abramson Stephan B, Meagher Michael, Offord Robin, Hartley Oliver

机构信息

Department of Pathology and Immunology, Faculty of Medicine, University of Geneva, Geneva, Switzerland.

BioGrammatics Inc., Carlsbad, CA 92011, USA.

出版信息

Protein Expr Purif. 2016 Mar;119:1-10. doi: 10.1016/j.pep.2015.10.011. Epub 2015 Oct 24.

Abstract

In the continued absence of an effective anti-HIV vaccine, approximately 2 million new HIV infections occur every year, with over 95% of these in developing countries. Calls have been made for the development of anti-HIV drugs that can be formulated for topical use to prevent HIV transmission during sexual intercourse. Because these drugs are principally destined for use in low-resource regions, achieving production costs that are as low as possible is an absolute requirement. 5P12-RANTES, an analog of the human chemokine protein RANTES/CCL5, is a highly potent HIV entry inhibitor which acts by achieving potent blockade of the principal HIV coreceptor, CCR5. Here we describe the development and optimization of a scalable low-cost production process for 5P12-RANTES based on expression in Pichia pastoris. At pilot (150 L) scale, this cGMP compliant process yielded 30 g of clinical grade 5P12-RANTES. As well as providing sufficient material for the first stage of clinical development, this process represents an important step towards achieving production of 5P12-RANTES at a cost and scale appropriate to meet needs for topical HIV prevention worldwide.

摘要

由于仍然没有有效的抗HIV疫苗,每年大约有200万新发HIV感染病例,其中超过95%发生在发展中国家。人们呼吁开发可制成局部用药的抗HIV药物,以预防性传播过程中的HIV传播。由于这些药物主要用于资源匮乏地区,因此将生产成本降至最低是绝对必要的。5P12-RANTES是人类趋化因子蛋白RANTES/CCL5的类似物,是一种高效的HIV进入抑制剂,其作用方式是有效阻断主要的HIV共受体CCR5。在此,我们描述了基于毕赤酵母表达的5P12-RANTES可扩展低成本生产工艺的开发和优化。在中试规模(150 L)下,这种符合cGMP标准的工艺生产出了30 g临床级5P12-RANTES。该工艺不仅为临床开发的第一阶段提供了足够的材料,也是朝着以适合全球局部预防HIV需求的成本和规模生产5P12-RANTES迈出的重要一步。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/629a/4725576/46482011be6a/gr1.jpg

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