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Targeting Pancreatic Islets with Phage Display Assisted by Laser Pressure Catapult Microdissection

机译:激光压力弹射器显微切割辅助通过噬菌体显示靶向胰岛

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摘要

Heterogeneity of the microvasculature in different organs has been well documented by multiple methods including in vivo phage display. However, less is known about the diversity of blood vessels within functionally distinct regions of organs. Here, we combined in vivo phage display with laser pressure catapult microdissection to identify peptide ligands for vascular receptors in the islets of Langerhans in the murine pancreas. Protein database analyses of the peptides, CVSNPRWKC and CHVLWSTRC, showed sequence identity to two ephrin A-type ligand homologues, A2 and A4. Confocal microscopy confirmed that most immunoreactivity of CVSNPRWKC and CHVLWSTRC phage was associated with blood vessels in pancreatic islets. Antibodies recognizing EphA4, a receptor for ephrin-A ligands, were similarly associated with islet blood vessels. Importantly, binding of both islet-homing phage and anti-EphA4 antibody was strikingly increased in blood vessels of pancreatic islet tumors in RIP-Tag2 transgenic mice. These results indicate that endothelial cells of blood vessels in pancreatic islets preferentially express EphA4 receptors, and this expression is increased in tumors. Our findings show in vivo phage display and laser pressure catapult microdissection can be combined to reveal endothelial cell specialization within focal regions of the microvasculature.
机译:已经通过包括体内噬菌体展示在内的多种方法很好地证明了不同器官中微脉管系统的异质性。然而,对于器官功能上不同的区域内的血管多样性知之甚少。在这里,我们结合了体内噬菌体展示和激光压力弹射显微切割技术,以鉴定鼠胰腺朗格汉斯胰岛中血管受体的肽配体。对肽CVSNPRWKC和CHVLWSTRC的蛋白质数据库分析显示与两个麻黄素A型配体同源物A2和A4具有序列同一性。共聚焦显微镜证实,CVSNPRWKC和CHVLWSTRC噬菌体的大多数免疫反应性与胰岛的血管有关。识别EphA4(ephrin-A配体的受体)的抗体与胰岛血管相似。重要的是,在RIP-Tag2转基因小鼠的胰腺胰岛肿瘤的血管中,胰岛归巢噬菌体和抗EphA4抗体的结合显着增加。这些结果表明胰腺胰岛中的血管内皮细胞优先表达EphA4受体,并且在肿瘤中这种表达增加。我们的发现表明体内噬菌体展示和激光压力弹射器显微解剖可以结合起来揭示微血管的焦点区域内的内皮细胞特化。

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