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抗朊蛋白单链Fv微型抗体对朊病毒传播的旁分泌抑制作用。

Paracrine inhibition of prion propagation by anti-PrP single-chain Fv miniantibodies.

作者信息

Donofrio Gaetano, Heppner Frank L, Polymenidou Magdalini, Musahl Christine, Aguzzi Adriano

机构信息

Institute of Neuropathology, University Hospital Zurich, Schmelzbergstrasse 12, CH-8091 Zürich, Switzerland.

出版信息

J Virol. 2005 Jul;79(13):8330-8. doi: 10.1128/JVI.79.13.8330-8338.2005.

Abstract

Prion diseases are characterized by the deposition of PrP(Sc), an abnormal form of the cellular prion protein PrP(C). A growing body of evidence suggests that antibodies to PrP(C) can antagonize deposition of PrP(Sc). However, host tolerance hampers the induction of immune responses to PrP(C), and cross-linking of PrP(C) by bivalent anti-PrP antibodies is neurotoxic. In order to obviate these problems, we explored the antiprion potential of recombinant single-chain antibody (scFv) fragments. scFv fragments derived from monoclonal anti-PrP antibody 6H4, flagged with c-myc and His6 tags, were correctly processed and secreted by mammalian RD-4 rhabdomyosarcoma cells. When cocultured with cells secreting anti-PrP scFv, chronically prion-infected neuroblastoma cells ceased to produce PrP(Sc), even if antibody-producing cells were physically separated from target cells in transwell cultures. Expression of scFv with irrelevant specificity, or of similarly tagged molecules, was not curative. Therefore, eukaryotically expressed scFv exerts a paracrine antiprion activity. The effector functions encoded by immunoglobulin constant domains are unnecessary for this effect. Because of their small size and their monovalent binding, scFv fragments may represent candidates for gene transfer-based immunotherapy of prion diseases.

摘要

朊病毒疾病的特征是细胞朊病毒蛋白PrP(C)的异常形式PrP(Sc)的沉积。越来越多的证据表明,针对PrP(C)的抗体可以拮抗PrP(Sc)的沉积。然而,宿主耐受性阻碍了对PrP(C)免疫反应的诱导,并且二价抗PrP抗体对PrP(C)的交联具有神经毒性。为了避免这些问题,我们探索了重组单链抗体(scFv)片段的抗朊病毒潜力。源自单克隆抗PrP抗体6H4的scFv片段,带有c-myc和His6标签,由哺乳动物RD-4横纹肌肉瘤细胞正确加工并分泌。当与分泌抗PrP scFv的细胞共培养时,慢性朊病毒感染的神经母细胞瘤细胞停止产生PrP(Sc),即使在transwell培养中产生抗体的细胞与靶细胞物理分离。表达具有不相关特异性的scFv或类似标记的分子没有治疗效果。因此,真核表达的scFv发挥旁分泌抗朊病毒活性。免疫球蛋白恒定域编码的效应功能对此效应不是必需的。由于其小尺寸和单价结合,scFv片段可能代表基于基因转移的朊病毒疾病免疫疗法的候选物。

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