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首页> 外文期刊>Journal of Immunological Methods >Phage-display selection on tumor histological specimens with laser capture microdissection.
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Phage-display selection on tumor histological specimens with laser capture microdissection.

机译:通过激光捕获显微切割在肿瘤组织学标本上进行噬菌体展示选择。

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摘要

A method was developed to obtain phage-display ligands that bind to a select population of cells in histological specimens of freshly harvested solid human cancers. It combines phage-display panning with laser capture microdissection (LCM). This method allows selection of phage ligands bound to subpopulations of specific cells contained in tumor tissue on histological sections. Naive phage scFv library was incubated directly on a histological section of human breast cancer that was snap frozen immediately after surgical resection. Tumor and stromal cells were captured by LCM and bound phages were recovered by bacterial infection. Individual phage clones selected after panning were evaluated for their binding ability by immunofluorescence staining on tumor tissue from the same patient. One phage-display antibody clone selected on tumor stroma showed selective binding on tumor stroma but did not bind to malignant cell population. The expressed scFv of this clone showed no significant binding to normal tissue, or 13 other breast cancers, or 4 colon cancer samples. Using the same method, phage display antibody clones were selected on tumor cells which showed binding to tumor cells and normal tissue. This method is applicable for selection of ligands to virtually any portion of a histological specimen amenable to LCM. This may speed the process of generating ligands to any subset of cells or noncellular feature present on histological specimens.
机译:已开发出一种方法来获得与新鲜收获的实体人类癌症的组织学样本中的选定细胞群结合的噬菌体展示配体。它结合了噬菌体展示淘选与激光捕获显微切割(LCM)。该方法允许选择与组织学切片上肿瘤组织中包含的特定细胞亚群结合的噬菌体配体。天真噬菌体scFv文库直接在人乳腺癌的组织切片上孵育,该切片在手术切除后立即速冻。 LCM捕获肿瘤和基质细胞,并通过细菌感染回收结合的噬菌体。淘选后选择的单个噬菌体克隆通过对同一患者的肿瘤组织进行免疫荧光染色来评估其结合能力。在肿瘤基质上选择的一种噬菌体展示抗体克隆在肿瘤基质上显示出选择性结合,但不与恶性细胞群体结合。表达的该克隆的scFv与正常组织,13种其他乳腺癌或4种结肠癌样品无明显结合。使用相同的方法,在显示与肿瘤细胞和正常组织结合的肿瘤细胞上选择噬菌体展示抗体克隆。该方法适用于选择适合LCM的组织学标本的几乎任何部分的配体。这可以加速产生组织标本上存在的细胞或非细胞特征的任何子集的配体的过程。

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