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Generation of a Monoclonal Antibody that Blocks Epithelial Binding of Unopsonized Particles.

机译:阻断非调理颗粒的上皮结合的单克隆抗体的产生。

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Alveolar macrophages (AMs) and epithelial cells (ECs) are the first cells in the lung to encounter inhaled environmental particles. The initial interaction between AMs and particles is mediated by specific scavenger receptors, but the nature of the structure(s) on ECs that also bind particles has not been well-described. To characterize the nature of the EC particle receptor, we screened a panel of mouse anti-human EC hybridomas for functional blockade of EC particle binding. This strategy identified a monoclonal antibody (MAb) (EPR1) that blocks binding of titanium dioxide (TiO(2)) particles to the EC line which served as the immunogen (A549), as well as to other EC lines (Beas 2-B, HTB54, HeLa, and MDA-MB-435S). EPR1 demonstrated specific labeling of ECs using immunohistology techniques and its expression could be quantitated by flow cytometry of permeabilized ECs in suspension. MAbs such as EPR1 may prove useful in further analysis of receptors for inhaled particles on lung epithelial cells.
机译:肺泡巨噬细胞(AM)和上皮细胞(EC)是肺中最早遇到吸入环境颗粒的细胞。 AM与颗粒之间的初始相互作用是由特定的清除剂受体介导的,但EC上也能与颗粒结合的结构的性质尚未得到很好的描述。为了表征EC颗粒受体的性质,我们筛选了一组功能性阻断EC颗粒结合的小鼠抗人EC杂交瘤。该策略确定了一种单克隆抗体(MAb)(EPR1),该抗体可阻止二氧化钛(TiO(2))颗粒与用作免疫原(A549)的EC系以及与其他EC系(Beas 2-B ,HTB54,HeLa和MDA-MB-435S)。 EPR1使用免疫组织学技术证明了EC的特异性标记,其表达可以通过流式细胞术对悬浮液中的通透EC进行定量。单克隆抗体(例如EPR1)可用于进一步分析肺上皮细胞吸入颗粒的受体。

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