Cathepsin B-Specific Metabolic Precursor for In Vivo Tumor-Specific Fluorescence Imaging

Man Kyu Shim; Hong Yeol Yoon; Ju Hee Ryu; Heebeom Koo; Sangmin Lee; Jae Hyung Park; Jong Ho Kim; Seulki Lee; Martin G. Pomper; Ick Chan Kwon; Kwangmeyung Kim

doi:10.1002/anie.201608504

Cathepsin B-Specific Metabolic Precursor for In Vivo Tumor-Specific Fluorescence Imaging

Man Kyu Shim, Hong Yeol Yoon, Ju Hee Ryu, Heebeom Koo, Sangmin Lee, Jae Hyung Park, Jong Ho Kim, Seulki Lee, Martin G. Pomper, Ick Chan Kwon, Kwangmeyung Kim

School of Medicine

Research output: Contribution to journal › Article › peer-review

37 Scopus citations

Abstract

Recently, metabolic glycoengineering with bioorthogonal click reactions has focused on improving the tumor targeting efficiency of nanoparticles as delivery vehicles for anticancer drugs or imaging agents. It is the key technique for developing tumor-specific metabolic precursors that can generate unnatural glycans on the tumor-cell surface. A cathepsin B-specific cleavable substrate (KGRR) conjugated with triacetylated N-azidoacetyl-d-mannosamine (RR-S-Ac₃ManNAz) was developed to enable tumor cells to generate unnatural glycans that contain azide groups. The generation of azide groups on the tumor cell surface was exogenously and specifically controlled by the amount of RR-S-Ac₃ManNAz that was fed to target tumor cells. Moreover, unnatural glycans on the tumor cell surface were conjugated with near infrared fluorescence (NIRF) dye-labeled molecules by a bioorthogonal click reaction in cell cultures and in tumor-bearing mice. Therefore, our RR-S-Ac₃ManNAz is promising for research in tumor-specific imaging or drug delivery.

Original language	English (US)
Pages (from-to)	14698-14703
Number of pages	6
Journal	Angewandte Chemie - International Edition
Volume	55
Issue number	47
DOIs	https://doi.org/10.1002/anie.201608504
State	Published - Nov 14 2016

Keywords

click chemistry
drug delivery
imaging agents
metabolic glycoengineering
tumor targeting

ASJC Scopus subject areas

Catalysis
General Chemistry

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10.1002/anie.201608504

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title = "Cathepsin B-Specific Metabolic Precursor for In Vivo Tumor-Specific Fluorescence Imaging",

abstract = "Recently, metabolic glycoengineering with bioorthogonal click reactions has focused on improving the tumor targeting efficiency of nanoparticles as delivery vehicles for anticancer drugs or imaging agents. It is the key technique for developing tumor-specific metabolic precursors that can generate unnatural glycans on the tumor-cell surface. A cathepsin B-specific cleavable substrate (KGRR) conjugated with triacetylated N-azidoacetyl-d-mannosamine (RR-S-Ac3ManNAz) was developed to enable tumor cells to generate unnatural glycans that contain azide groups. The generation of azide groups on the tumor cell surface was exogenously and specifically controlled by the amount of RR-S-Ac3ManNAz that was fed to target tumor cells. Moreover, unnatural glycans on the tumor cell surface were conjugated with near infrared fluorescence (NIRF) dye-labeled molecules by a bioorthogonal click reaction in cell cultures and in tumor-bearing mice. Therefore, our RR-S-Ac3ManNAz is promising for research in tumor-specific imaging or drug delivery.",

keywords = "click chemistry, drug delivery, imaging agents, metabolic glycoengineering, tumor targeting",

author = "Shim, {Man Kyu} and Yoon, {Hong Yeol} and Ryu, {Ju Hee} and Heebeom Koo and Sangmin Lee and Park, {Jae Hyung} and Kim, {Jong Ho} and Seulki Lee and Pomper, {Martin G.} and Kwon, {Ick Chan} and Kwangmeyung Kim",

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year = "2016",

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doi = "10.1002/anie.201608504",

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AU - Ryu, Ju Hee

AU - Koo, Heebeom

AU - Lee, Sangmin

AU - Park, Jae Hyung

AU - Kim, Jong Ho

AU - Lee, Seulki

AU - Pomper, Martin G.

AU - Kwon, Ick Chan

AU - Kim, Kwangmeyung

PY - 2016/11/14

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N2 - Recently, metabolic glycoengineering with bioorthogonal click reactions has focused on improving the tumor targeting efficiency of nanoparticles as delivery vehicles for anticancer drugs or imaging agents. It is the key technique for developing tumor-specific metabolic precursors that can generate unnatural glycans on the tumor-cell surface. A cathepsin B-specific cleavable substrate (KGRR) conjugated with triacetylated N-azidoacetyl-d-mannosamine (RR-S-Ac3ManNAz) was developed to enable tumor cells to generate unnatural glycans that contain azide groups. The generation of azide groups on the tumor cell surface was exogenously and specifically controlled by the amount of RR-S-Ac3ManNAz that was fed to target tumor cells. Moreover, unnatural glycans on the tumor cell surface were conjugated with near infrared fluorescence (NIRF) dye-labeled molecules by a bioorthogonal click reaction in cell cultures and in tumor-bearing mice. Therefore, our RR-S-Ac3ManNAz is promising for research in tumor-specific imaging or drug delivery.

AB - Recently, metabolic glycoengineering with bioorthogonal click reactions has focused on improving the tumor targeting efficiency of nanoparticles as delivery vehicles for anticancer drugs or imaging agents. It is the key technique for developing tumor-specific metabolic precursors that can generate unnatural glycans on the tumor-cell surface. A cathepsin B-specific cleavable substrate (KGRR) conjugated with triacetylated N-azidoacetyl-d-mannosamine (RR-S-Ac3ManNAz) was developed to enable tumor cells to generate unnatural glycans that contain azide groups. The generation of azide groups on the tumor cell surface was exogenously and specifically controlled by the amount of RR-S-Ac3ManNAz that was fed to target tumor cells. Moreover, unnatural glycans on the tumor cell surface were conjugated with near infrared fluorescence (NIRF) dye-labeled molecules by a bioorthogonal click reaction in cell cultures and in tumor-bearing mice. Therefore, our RR-S-Ac3ManNAz is promising for research in tumor-specific imaging or drug delivery.

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Cathepsin B-Specific Metabolic Precursor for In Vivo Tumor-Specific Fluorescence Imaging

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