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首页> 外文期刊>The Journal of investigative dermatology. >Isolation of pathogenic monoclonal anti-desmoglein 1 human antibodies by phage display of pemphigus foliaceus autoantibodies.
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Isolation of pathogenic monoclonal anti-desmoglein 1 human antibodies by phage display of pemphigus foliaceus autoantibodies.

机译:通过天疱疮性天疱疮自身抗体的噬菌体展示分离病原性单克隆抗桥粒芯蛋白1人类抗体。

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摘要

Pemphigus foliaceus (PF) is a blistering disease caused by autoantibodies to desmoglein 1 (Dsg1) that cause loss of epidermal cell adhesion. To better understand PF pathophysiology, we used phage display to isolate anti-Dsg1 mAbs as single-chain variable fragments (scFvs) from a PF patient. Initial panning of the library isolated only non-pathogenic scFvs. We then used these scFvs to block non-pathogenic epitopes and were able to isolate two unique scFvs, each of which caused typical PF blisters in mice or human epidermis models, showing that a single mAb can disrupt Dsg1 function to cause disease. Both pathogenic scFvs bound conformational epitopes in the N terminus of Dsg1. Other PF sera showed a major antibody response against the same or nearby epitopes defined by these pathogenic scFvs. Finally, we showed restriction of the heavy-chain gene usage of all anti-Dsg1 clones to only five genes, which determined their immunological properties despite promiscuous light-chain gene usage. These mAbs will be useful for studying Dsg1 function and mechanisms of blister formation in PF and for developing targeted therapies and tools to monitor disease activity.
机译:天疱疮天疱疮(PF)是一种起泡性疾病,由针对去铁血球蛋白1(Dsg1)的自身抗体引起,导致表皮细胞粘附力下降。为了更好地了解PF的病理生理,我们使用噬菌体展示从PF患者中分离出抗Dsg1 mAb作为单链可变片段(scFvs)。库的最初淘选仅分离出非病原性scFv。然后,我们使用这些scFvs阻断非致病性表位,并能够分离出两个独特的scFvs,每个scFvs在小鼠或人表皮模型中引起典型的PF水泡,表明单个mAb可以破坏Dsg1功能以引起疾病。两个致病性scFvs绑定Dsg1 N末端的构象表位。其他PF血清显示出针对这些致病性scFv定义的相同或附近表位的主要抗体反应。最后,我们显示了将所有抗Dsg1克隆的重链基因使用限制为只有五个基因,尽管使用了轻链基因,但它们确定了其免疫学特性。这些单克隆抗体可用于研究PF中Dsg1的功能和水疱形成的机制,以及开发针对性的疗法和工具来监测疾病的活动。

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