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抗桥粒芯糖蛋白 3 抗体 AK23 的标准化生产用于翻译性寻常型天疱疮研究。

Standardized Production of Anti-Desmoglein 3 Antibody AK23 for Translational Pemphigus Vulgaris Research.

机构信息

Department for Biomedical Research, Molecular Dermatology and Stem Cell Research, University of Bern, Bern, Switzerland.

Department of Dermatology, Inselspital, Bern University Hospital, University of Bern, Bern, Switzerland.

出版信息

Curr Protoc. 2024 Aug;4(8):e1118. doi: 10.1002/cpz1.1118.

Abstract

Antibody-mediated receptor activation is successfully used to develop medical treatments. If the activation induces a pathological response, such antibodies are also excellent tools for defining molecular mechanisms of target receptor malfunction and designing rescue therapies. Prominent examples are naturally occurring autoantibodies inducing the severe blistering disease pemphigus vulgaris (PV). In the great majority of patients, the antibodies bind to the adhesion receptor desmoglein 3 (Dsg3) and interfere with cell signaling to provoke severe blistering in the mucous membranes and/or skin. The identification of a comprehensive causative signaling network downstream of antibody-targeted Dsg3 receptors (e.g., shown by pharmacological activators or inhibitors) is currently being discussed as a basis to develop urgently needed first-line treatments for PV patients. Although polyclonal PV IgG antibodies have been used as proof of principle for pathological signal activation, monospecific anti-Dsg3 antibodies are necessary and have been developed to identify pathological Dsg3 receptor-mediated signal transduction. The experimental monospecific PV antibody AK23, produced from hybridoma cells, was extensively tested in our laboratory in both in vitro and in vivo models for PV and proved to recapitulate the clinicopathological features of PV when generated using the standardized production and purification protocols described herein. © 2024 The Author(s). Current Protocols published by Wiley Periodicals LLC. Basic Protocol 1: Bovine IgG stripping from FBS and quality control Basic Protocol 2: AK23 hybridoma expansion and IgG production Basic Protocol 3: AK23 IgG purification Basic Protocol 4: AK23 IgG quality control Support Protocol 1: Detection of endotoxin levels Support Protocol 2: Detection and removal of mycoplasma.

摘要

抗体介导的受体激活被成功用于开发医学治疗方法。如果这种激活引起病理性反应,那么这些抗体也是定义靶受体功能障碍的分子机制和设计挽救治疗方法的极好工具。一个突出的例子是自然发生的自身抗体诱导严重的水疱病天疱疮(PV)。在绝大多数患者中,抗体与粘附受体桥粒芯糖蛋白 3(Dsg3)结合,并干扰细胞信号转导,导致粘膜和/或皮肤严重水疱。目前正在讨论抗体靶向 Dsg3 受体的全面因果信号网络(例如,通过药理学激活剂或抑制剂显示)的鉴定,作为开发 PV 患者急需的一线治疗方法的基础。尽管多克隆 PV IgG 抗体已被用作病理性信号激活的原理证明,但单特异性抗 Dsg3 抗体是必需的,并已开发出来以识别病理性 Dsg3 受体介导的信号转导。从杂交瘤细胞产生的实验性单特异性 PV 抗体 AK23,在我们的实验室中已在 PV 的体外和体内模型中进行了广泛测试,并证明当按照本文所述的标准化生产和纯化方案生成时,可再现 PV 的临床病理特征。© 2024 作者。Wiley Periodicals LLC 出版的《当代协议》。基本方案 1:从 FBS 中去除牛 IgG 并进行质量控制基本方案 2:AK23 杂交瘤的扩增和 IgG 生产基本方案 3:AK23 IgG 的纯化基本方案 4:AK23 IgG 的质量控制支持方案 1:检测内毒素水平支持方案 2:检测和去除支原体。

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