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通过用培养的人黑色素瘤细胞淘选合成噬菌体展示单链抗体片段文库分离得到的人单链抗体片段多样性有限。

Limited diversity of human scFv fragments isolated by panning a synthetic phage-display scFv library with cultured human melanoma cells.

作者信息

Noronha E J, Wang X, Desai S A, Kageshita T, Ferrone S

机构信息

Department of Microbiology and Immunology, New York Medical College, Valhalla 10595, USA.

出版信息

J Immunol. 1998 Sep 15;161(6):2968-76.

PMID:9743360
Abstract

To broaden the specificity of the Abs recognizing human melanoma-associated Ags (MAAs), we have isolated human single-chain fragment of the V region (scFv) fragments by panning the synthetic phage Ab library (#1) with the human melanoma cell lines S5 and SK-MEL-28. All of the isolated scFv fragments reacted with the mouse mAb defined high molecular weight melanoma-associated Ag (HMW-MAA). scFv #70 immunoprecipitates the two characteristic subunits of HMW-MAA, while scFv #28 only immunoprecipitates its large subunit. These results challenge the current view regarding the structure of HMW-MAA and indicate that it consists of two independent subunits. The human scFv fragments share some similarities with the mouse anti-HMW-MAA mAb. Like mAb 149.53 and 225.28, scFv #28 reacts with rat B49 neural cells that express a homologue of HMW-MAA. scFv #70 reacts with a determinant that is spatially close to the one identified by mAbs 149.53, VT68.2, and VT86. Besides suggesting similarities in the recognition of human melanoma cells by the mouse and human Ab repertoire, these results indicate that the Abs isolated from synthetic Ab libraries resemble those that are found in natural Ab repertoires. The restricted diversity of the scFv fragments that were isolated by panning synthetic Ab libraries with different melanoma cell lines suggests that certain Ags, like HMW-MAA, are immunodominant in vitro. This phenomenon, which parallels the in vivo immunodominance of certain Ags, implies that the antigenic profile of the cells used for panning determines the specificity of the preponderant population of isolated Abs.

摘要

为了拓宽识别人类黑色素瘤相关抗原(MAA)的抗体的特异性,我们通过用人黑色素瘤细胞系S5和SK-MEL-28筛选合成噬菌体抗体文库(#1),分离出了人类V区单链片段(scFv)。所有分离出的scFv片段都与小鼠单克隆抗体定义的高分子量黑色素瘤相关抗原(HMW-MAA)发生反应。scFv #70免疫沉淀HMW-MAA的两个特征性亚基,而scFv #28仅免疫沉淀其大亚基。这些结果对目前关于HMW-MAA结构的观点提出了挑战,并表明它由两个独立的亚基组成。人类scFv片段与小鼠抗HMW-MAA单克隆抗体有一些相似之处。与单克隆抗体149.53和225.28一样,scFv #28与表达HMW-MAA同源物的大鼠B49神经细胞发生反应。scFv #70与一个在空间上与单克隆抗体149.53、VT68.2和VT86识别的决定簇相近的决定簇发生反应。这些结果除了表明小鼠和人类抗体库在识别人类黑色素瘤细胞方面存在相似性外,还表明从合成抗体文库中分离出的抗体与天然抗体库中发现的抗体相似。通过用不同的黑色素瘤细胞系筛选合成抗体文库而分离出的scFv片段的有限多样性表明,某些抗原,如HMW-MAA,在体外具有免疫优势。这种与某些抗原在体内的免疫优势相似的现象意味着,用于筛选的细胞的抗原谱决定了分离出的优势抗体群体的特异性。

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