Hai Yan Hong scite author profile

Hai Yan Hong

5Publications

293Citation Statements Received

83Citation Statements Given

How they've been cited

363

288

How they cite others

169

Affiliations

Kyungpook National University

Publications

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Targeting Bladder Tumor CellsIn vivoand in the Urine with a Peptide Identified by Phage Display

Lee

Hong

et al. 2007

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Bladder cancer is one of the most common tumors of the genitourinary tract. Here, we use phage display to identify a peptide that targets bladder tumor cells. A phage library containing random peptides was screened for binding to cells from human bladder tumor xenografts. Phage clones were further selected for binding to a bladder tumor cell line in culture. Six clones displaying the consensus sequence CXNXDXR X

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Detection of apoptosis in a rat model of focal cerebral ischemia using a homing peptide selected from in vivo phage display

Hong

Choi

Kim

et al. 2008

Journal of Controlled Release

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Phage display selection of peptides that home to atherosclerotic plaques: IL‐4 receptor as a candidate target in atherosclerosis

Hong

Lee

Kwak

et al. 2008

J Cellular Molecular Medi

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Imaging or drug delivery tools for atherosclerosis based on the plaque biology are still insufficient. Here, we attempted to identify peptides that selectively home to atherosclerotic plaques using phage display. A phage library containing random peptides was ex viv screened for binding to human atheroma tissues. After three to four rounds of selection, the DNA inserts of phage clones wer sequenced. A peptide sequence, CRKRLDRNC, was the most frequently occurring one. Intravenously injected phage displaying the CRKRLDRNC peptide was observed to home to atherosclerotic aortic tissues of low-density lipoprotein receptor-deficient (Ldlr−/–) mice at higher levels than to normal aortic tissues of wild-type mice. Moreover, a fluorescein- or radioisotope-conjugated synthetic CRKRLDRNC peptide, but not a control peptide, homed in vivo to atherosclerotic plaques in Ldlr−/– mice, while homing of the peptide to other organs such as brain was minimal. The homing peptide co-localized with endothelial cells, macrophages and smooth muscle cells a mouse and human atherosclerotic plaques. Homology search revealed that the CRKRLDRNC peptide shares a motif of interleukin-receptor (IL-4) that is critical for binding to its receptor. The peptide indeed co-localized with IL-4 receptor (IL-4R) at atherosclerotic plaques. Moreover, the peptide bound to cultured cells expressing IL-4R on the cell surface and the binding was inhibited by the knock-down of IL-4R. These results show that the CRKRLDRNC peptide homes to atherosclerotic plaques through binding to IL-4R as its target and may be a useful tool for selective drug delivery and molecular imaging of atherosclerosis.

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A new atherosclerotic lesion probe based on hydrophobically modified chitosan nanoparticles functionalized by the atherosclerotic plaque targeted peptides

Park

Hong

Moon

et al. 2008

Journal of Controlled Release

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Identification of a peptide ligand recognizing dysfunctional endothelial cells for targeting atherosclerosis

Thapa

Hong

Purushotham

et al. 2008

Journal of Controlled Release

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Hai Yan Hong

Targeting Bladder Tumor CellsIn vivoand in the Urine with a Peptide Identified by Phage Display

Detection of apoptosis in a rat model of focal cerebral ischemia using a homing peptide selected from in vivo phage display

Phage display selection of peptides that home to atherosclerotic plaques: IL‐4 receptor as a candidate target in atherosclerosis

A new atherosclerotic lesion probe based on hydrophobically modified chitosan nanoparticles functionalized by the atherosclerotic plaque targeted peptides

Identification of a peptide ligand recognizing dysfunctional endothelial cells for targeting atherosclerosis

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