Literature DB >> 15681844

Targeting pancreatic islets with phage display assisted by laser pressure catapult microdissection.

Virginia J Yao1, Michael G Ozawa, Martin Trepel, Wadih Arap, Donald M McDonald, Renata Pasqualini.   

Abstract

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.

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Year:  2005        PMID: 15681844      PMCID: PMC1602338          DOI: 10.1016/S0002-9440(10)62283-3

Source DB:  PubMed          Journal:  Am J Pathol        ISSN: 0002-9440            Impact factor:   4.307


  49 in total

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Review 3.  Eph signaling: a structural view.

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Journal:  J Biol Chem       Date:  1999-04-23       Impact factor: 5.157

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  40 in total

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3.  Crystal structure and NMR binding reveal that two small molecule antagonists target the high affinity ephrin-binding channel of the EphA4 receptor.

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4.  Small molecules can selectively inhibit ephrin binding to the EphA4 and EphA2 receptors.

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Review 5.  Combinatorial peptide libraries: mining for cell-binding peptides.

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6.  Combinatorial ligand-directed lung targeting.

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7.  Potential of phage-displayed peptide library technology to identify functional targeting peptides.

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Review 8.  Emerging Roles of Vascular Endothelium in Metabolic Homeostasis.

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Review 9.  Targeting Type 1 Diabetes: Selective Approaches for New Therapies.

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10.  Selection and identification of ligand peptides targeting a model of castrate-resistant osteogenic prostate cancer and their receptors.

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