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靶向动脉粥样硬化病变的人源单链抗体片段的鉴定:通过体内噬菌体展示单轮筛选

Identification of human scFvs targeting atherosclerotic lesions: selection by single round in vivo phage display.

作者信息

Robert Rémy, Jacobin-Valat Marie-Josée, Daret Danièle, Miraux Sylvain, Nurden Alan T, Franconi Jean-Michel, Clofent-Sanchez Gisèle

机构信息

Résonance Magnétique des Systèmes Biologiques, Centre National Recherche Scientifique (CNRS), UMR 5536, Université Bordeaux 2 Victor Ségalen, 146 rue Léo Saignat, 33076 Bordeaux, France.

出版信息

J Biol Chem. 2006 Dec 29;281(52):40135-43. doi: 10.1074/jbc.M609344200. Epub 2006 Oct 26.

DOI:10.1074/jbc.M609344200
PMID:17068330
Abstract

Our aim was to investigate by in vivo biopanning the lesions developed early in atherosclerosis and identify human antibodies that home to diseased regions. We have designed a two-step approach for a rapid isolation of human Monoclonal phage-display single-chain antibodies (MoPhabs) reactive with proteins found in lesions developed in an animal model of atherosclerosis. After a single round of in vivo biopanning, the MoPhabs were eluted from diseased sections of rabbit aorta identified by histology and NMR microscopy. MoPhabs expressed in situ were selected by subtractive colony filter screening for their capacity to recognize atherosclerotic but not normal aorta. MoPhabs selected by our method predominantly bind atherosclerotic lesions. Two of them, B3.3G and B3.GER, produced as scFv fragments, recognized an epitope present on the surface in early atherosclerotic lesions and within the intimal thickness in more complex plaques. These human MoPhabs homed to atherosclerotic lesions in ApoE(-/-) mice after in vivo injection. A protein of approximately 56 kDa recognized by B3.3G was affinity-purified and identified by mass spectrometry analysis as vitronectin. This is the first time that single round in vivo biopanning has been used to select human antibodies as candidates for diagnostic imaging and for obtaining insight into targets displayed in atherosclerotic plaques.

摘要

我们的目的是通过体内生物淘选来研究动脉粥样硬化早期形成的病变,并鉴定归巢于病变区域的人源抗体。我们设计了一种两步法,用于快速分离与动脉粥样硬化动物模型中病变部位发现的蛋白质发生反应的人源单克隆噬菌体展示单链抗体(MoPhabs)。经过一轮体内生物淘选后,从经组织学和核磁共振显微镜鉴定的兔主动脉病变切片中洗脱MoPhabs。通过消减菌落滤膜筛选原位表达的MoPhabs,以筛选其识别动脉粥样硬化而非正常主动脉的能力。通过我们的方法筛选出的MoPhabs主要结合动脉粥样硬化病变。其中两个,B3.3G和B3.GER,作为单链抗体片段产生,识别早期动脉粥样硬化病变表面以及更复杂斑块内膜厚度内存在的一个表位。体内注射后,这些人源MoPhabs归巢于载脂蛋白E基因敲除(ApoE(-/-))小鼠的动脉粥样硬化病变部位。通过B3.3G识别的一种约56 kDa的蛋白质经亲和纯化,并通过质谱分析鉴定为玻连蛋白。这是首次使用单轮体内生物淘选来选择人源抗体作为诊断成像的候选物,并深入了解动脉粥样硬化斑块中显示的靶点。

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