Construction and validation of a synthetic phage-displayed nanobody library.

IF 1.6 4区医学 Q3 PHARMACOLOGY & PHARMACY Korean Journal of Physiology & Pharmacology Pub Date : 2024-09-01 DOI:10.4196/kjpp.2024.28.5.457

Minju Kim, Xuelian Bai, Hyewon Im, Jisoo Yang, Youngju Kim, Minjoo Mj Kim, Yeonji Oh, Yuna Jeon, Hayoung Kwon, Seunghyun Lee, Chang-Han Lee

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Abstract

Nanobodies derived from camelids and sharks offer unique advantages in therapeutic applications due to their ability to bind to epitopes that were previously inaccessible. Traditional methods of nanobody development face challenges such as ethical concerns and antigen toxicity. Our study presents a synthetic, phagedisplayed nanobody library using trinucleotide-directed mutagenesis technology, which allows precise amino acid composition in complementarity-determining regions (CDRs), with a focus on CDR3 diversity. This approach avoids common problems such as frameshift mutations and stop codon insertions associated with other synthetic antibody library construction methods. By analyzing FDA-approved nanobodies and Protein Data Bank sequences, we designed sub-libraries with different CDR3 lengths and introduced amino acid substitutions to improve solubility. The validation of our library through the successful isolation of nanobodies against targets such as PD-1, ATXN1 and STAT3 demonstrates a versatile and ethical platform for the development of high specificity and affinity nanobodies and represents a significant advance in biotechnology.

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合成噬菌体显示纳米抗体库的构建与验证。

从驼科动物和鲨鱼身上提取的纳米抗体具有独特的治疗应用优势，因为它们能够与以前无法触及的表位结合。传统的纳米抗体开发方法面临着伦理问题和抗原毒性等挑战。我们的研究利用三核苷酸定向诱变技术，提出了一种人工合成的、噬菌体显示的纳米抗体文库，它可以精确地组成互补性决定区（CDR）的氨基酸，重点是CDR3的多样性。这种方法避免了与其他合成抗体文库构建方法相关的常见问题，如框移突变和终止密码子插入。通过分析 FDA 批准的纳米抗体和蛋白质数据库序列，我们设计出了具有不同 CDR3 长度的子库，并引入了氨基酸替代以提高溶解度。通过成功分离出针对 PD-1、ATXN1 和 STAT3 等靶点的纳米抗体，我们的文库得到了验证，为开发高特异性和高亲和力纳米抗体提供了一个多功能的道德平台，是生物技术领域的一大进步。

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来源期刊

Korean Journal of Physiology & Pharmacology PHARMACOLOGY & PHARMACY-PHYSIOLOGY

CiteScore

3.20

自引率

5.00%

发文量

审稿时长

6-12 weeks

期刊介绍： The Korean Journal of Physiology & Pharmacology (Korean J. Physiol. Pharmacol., KJPP) is the official journal of both the Korean Physiological Society (KPS) and the Korean Society of Pharmacology (KSP). The journal launched in 1997 and is published bi-monthly in English. KJPP publishes original, peer-reviewed, scientific research-based articles that report successful advances in physiology and pharmacology. KJPP welcomes the submission of all original research articles in the field of physiology and pharmacology, especially the new and innovative findings. The scope of researches includes the action mechanism, pharmacological effect, utilization, and interaction of chemicals with biological system as well as the development of new drug targets. Theoretical articles that use computational models for further understanding of the physiological or pharmacological processes are also welcomed. Investigative translational research articles on human disease with an emphasis on physiology or pharmacology are also invited. KJPP does not publish work on the actions of crude biological extracts of either unknown chemical composition (e.g. unpurified and unvalidated) or unknown concentration. Reviews are normally commissioned, but consideration will be given to unsolicited contributions. All papers accepted for publication in KJPP will appear simultaneously in the printed Journal and online.