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白细胞介素-18结合蛋白(IL-18BP):从发现到临床应用的漫长历程。

Interleukin-18 Binding Protein (IL-18BP): A Long Journey From Discovery to Clinical Application.

作者信息

Kim Soohyun, Yu Hyeon, Azam Tania, Dinarello Charles A

机构信息

College of Veterinary Medicine, Konkuk University, Seoul 05029, Korea.

Laboratory of Cytokine Immunology, Department of Biomedical Science and Technology, Konkuk University, Seoul 05029, Korea.

出版信息

Immune Netw. 2024 Jan 15;24(1):e1. doi: 10.4110/in.2024.24.e1. eCollection 2024 Feb.

Abstract

IL-18 binding protein (IL-18BP) was originally discovered in 1999 while attempting to identify an IL-18 receptor ligand binding chain (also known as IL-18Rα) by subjecting concentrated human urine to an IL-18 ligand affinity column. The IL-18 ligand chromatography purified molecule was analyzed by protein microsequencing. The result revealed a novel 40 amino acid polypeptide. To isolate the complete open reading frame (ORF), various human and mouse cDNA libraries were screened using cDNA probe derived from the novel IL-18 affinity column bound molecule. The identified entire ORF gene was thought to be an IL-18Rα gene. However, IL-18BP has been proven to be a unique soluble antagonist that shares homology with a variety of viral proteins that are distinct from the IL-18Rα and IL-18Rβ chains. The IL-18BP cDNA was used to generate recombinant IL-18BP (rIL-18BP), which was indispensable for characterizing the role of IL-18BP and . Mammalian cell lines were used to produce rIL-18BP due to its glycosylation-dependent activity of IL-18BP (approximately 20 kDa). Various forms of rIL-18BP, intact, C-terminal his-tag, and Fc fusion proteins were produced for and experiments. Data showed potent neutralization of IL-18 activity, which seems promising for clinical application in immune diseases involving IL-18. However, it was a long journey from discovery to clinical use although there have been various clinical trials since IL-18BP was discovered in 1999. This review primarily covers the discovery of IL-18BP along with how basic research influences the clinical development of IL-18BP.

摘要

白细胞介素-18结合蛋白(IL-18BP)最初于1999年被发现,当时通过将浓缩的人尿液通过IL-18配体亲和柱来试图鉴定一种IL-18受体配体结合链(也称为IL-18Rα)。通过蛋白质微测序分析了经IL-18配体色谱法纯化的分子。结果揭示了一种新的40个氨基酸的多肽。为了分离完整的开放阅读框(ORF),使用源自与新型IL-18亲和柱结合的分子的cDNA探针筛选了各种人和小鼠cDNA文库。鉴定出的完整ORF基因被认为是IL-18Rα基因。然而,IL-18BP已被证明是一种独特的可溶性拮抗剂,与多种不同于IL-18Rα和IL-18Rβ链的病毒蛋白具有同源性。IL-18BP cDNA被用于产生重组IL-18BP(rIL-18BP),这对于表征IL-18BP的作用是必不可少的。由于IL-18BP的糖基化依赖性活性(约20 kDa),哺乳动物细胞系被用于产生rIL-18BP。为了进行实验,产生了各种形式的rIL-18BP,包括完整的、C末端组氨酸标签和Fc融合蛋白。数据显示对IL-18活性有有效的中和作用,这对于涉及IL-18的免疫疾病的临床应用似乎很有前景。然而,从发现到临床应用经历了漫长的过程,尽管自1999年发现IL-18BP以来已经进行了各种临床试验。这篇综述主要涵盖了IL-18BP的发现以及基础研究如何影响IL-18BP的临床开发。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5e0e/10917572/0568175a9397/in-24-e1-g001.jpg

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