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治疗性单克隆抗体和抗体片段的拼图——从全长免疫球蛋白到抗体模拟物的模块化转变。

The mosaic puzzle of the therapeutic monoclonal antibodies and antibody fragments - A modular transition from full-length immunoglobulins to antibody mimetics.

作者信息

Khatib Sami El, Salla Mohamed

机构信息

Lebanese International University, Department of Biomedical Sciences, Bekaa Campus, Khiyara, West Bekaa, Lebanon.

University of Alberta. Biochemistry Department, Faculty of Medicine and Dentistry,116St & 85 Ave, Edmonton, AB, T6G 2R3, Canada.

出版信息

Leuk Res Rep. 2022 Jun 27;18:100335. doi: 10.1016/j.lrr.2022.100335. eCollection 2022.

Abstract

The use of monoclonal antibodies represents an important and efficient diagnostic and therapeutic tool in disease management and modern science but remains limited by several factors including the uneven distribution in diseased tissues as well as undesired activation of side immune reactions. Major scientific advancements including Recombinant DNA Technology, Hybridoma Technology, and Polymerase Chain Reaction have considerably impacted the use of monoclonal antibodies providing technical and effective solutions to overcome the shortcomings encountered with conventional antibodies. Initially, the introduction of antibody fragments allowed a more uniform and deeper penetration of the targeted tissue and reduced unwanted activation of Fc-mediated immune reactions. On another level, the immunogenicity of murine-derived antibodies was overcome by humanizing their encoding genes with specific sequences of human origin andtransgenic mice able to synthesize fully human antibodies were successfully created. Moreover, the advancement of genetic engineering techniques supported by the modular structure of antibody coding genes paved the way for the development of a new generation of antibody fragments with a wide spectrum of monospecific and bispecific agents. These later could be monovalent, bivalent, or multivalent, and either expressed as a single chain, assembled in multimeric forms or stringed in tandem. This has conferred improved affinity, stability, and solubility to antibody targetting. Lately, a new array of monoclonal antibody fragments was introduced with the engineering of nanobody and antibody mimetics as non-immunoglobulin-derived fragments with promising diagnostic and therapeutic applications. In this review, we decipher the molecular basis of monoclonal antibody engineering with a detailed screening of the antibody derivatives that provides new perspectives to expand the use of monoclonal fragments into previously unexplored fields.

摘要

单克隆抗体的应用是疾病管理和现代科学中一项重要且有效的诊断和治疗工具,但仍受到多种因素的限制,包括在患病组织中的分布不均以及不必要的免疫副反应激活。包括重组DNA技术、杂交瘤技术和聚合酶链反应在内的重大科学进展,对单克隆抗体的应用产生了重大影响,为克服传统抗体所遇到的缺点提供了技术和有效的解决方案。最初,抗体片段的引入使靶向组织能够更均匀、更深入地渗透,并减少了Fc介导的免疫反应的不必要激活。在另一个层面上,通过用人源特异性序列对鼠源抗体的编码基因进行人源化,克服了鼠源抗体的免疫原性,并成功培育出能够合成完全人源抗体的转基因小鼠。此外,抗体编码基因的模块化结构支持下的基因工程技术进步,为开发新一代具有广泛单特异性和双特异性试剂的抗体片段铺平了道路。这些片段可以是单价、二价或多价的,可以表达为单链、组装成多聚体形式或串联排列。这赋予了抗体靶向更好的亲和力、稳定性和溶解性。最近,随着纳米抗体和抗体模拟物的工程化,引入了一系列新的单克隆抗体片段,它们作为非免疫球蛋白衍生的片段具有有前景的诊断和治疗应用。在这篇综述中,我们通过对抗体衍生物的详细筛选来解读单克隆抗体工程的分子基础,这为将单克隆片段的应用扩展到以前未探索的领域提供了新的视角。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4611/9272380/32dcd5eb66f2/gr1.jpg

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