Ligand profiling and identification technology for searching bioactive ligands

Moon Chang Baek; Sun Jin Kim; Kyungmoo Yea; Youndong Kim; Byung Dae Lee; Jaeyoon Kim; Hae Jeong Lee; Mee Hee Kang; Sun Kyu Choi; Jong In Kim; Taehoon G. Lee; Pann Ghill Suh; Sung Ho Ryu

doi:10.1002/pmic.200500511

Ligand profiling and identification technology for searching bioactive ligands

Moon Chang Baek, Sun Jin Kim, Kyungmoo Yea, Youndong Kim, Byung Dae Lee, Jaeyoon Kim, Hae Jeong Lee, Mee Hee Kang, Sun Kyu Choi, Jong In Kim, Taehoon G. Lee, Pann Ghill Suh, Sung Ho Ryu

Department of New Biology

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

1 Scopus citations

Abstract

We introduce a new methodology named ligand profiling and identification for effective discovery of bioactive ligands such as peptide hormones. This technology was developed from a new concept of parallel column chromatography and active fraction profiling by nano-LC MS. Traditional methods use sequential column chromatography, and thus are inevitably limited by the low abundance of the peptide of interest and by a low yield due to the many column steps. Using this new technology, insulin was successfully identified and diarginylinsulin, a minor intermediate form of insulin, was unexpectedly also identified simultaneously from 100 mg of porcine pancreatic tissue. This integrative technology could be used to search for various low-abundance peptides (or bioactive molecules) rapidly and simultaneously, by applying this to the later stages of traditional sequential purification.

Original language	English
Pages (from-to)	1741-1749
Number of pages	9
Journal	Proteomics
Volume	6
Issue number	6
DOIs	https://doi.org/10.1002/pmic.200500511
State	Published - Mar 2006

Keywords

Identification
Ligand
Peptidome
Profiling

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10.1002/pmic.200500511

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title = "Ligand profiling and identification technology for searching bioactive ligands",

abstract = "We introduce a new methodology named ligand profiling and identification for effective discovery of bioactive ligands such as peptide hormones. This technology was developed from a new concept of parallel column chromatography and active fraction profiling by nano-LC MS. Traditional methods use sequential column chromatography, and thus are inevitably limited by the low abundance of the peptide of interest and by a low yield due to the many column steps. Using this new technology, insulin was successfully identified and diarginylinsulin, a minor intermediate form of insulin, was unexpectedly also identified simultaneously from 100 mg of porcine pancreatic tissue. This integrative technology could be used to search for various low-abundance peptides (or bioactive molecules) rapidly and simultaneously, by applying this to the later stages of traditional sequential purification.",

keywords = "Identification, Ligand, Peptidome, Profiling",

author = "Baek, \{Moon Chang\} and Kim, \{Sun Jin\} and Kyungmoo Yea and Youndong Kim and Lee, \{Byung Dae\} and Jaeyoon Kim and Lee, \{Hae Jeong\} and Kang, \{Mee Hee\} and Choi, \{Sun Kyu\} and Kim, \{Jong In\} and Lee, \{Taehoon G.\} and Suh, \{Pann Ghill\} and Ryu, \{Sung Ho\}",

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doi = "10.1002/pmic.200500511",

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T1 - Ligand profiling and identification technology for searching bioactive ligands

AU - Baek, Moon Chang

AU - Kim, Sun Jin

AU - Yea, Kyungmoo

AU - Kim, Youndong

AU - Lee, Byung Dae

AU - Kim, Jaeyoon

AU - Lee, Hae Jeong

AU - Kang, Mee Hee

AU - Choi, Sun Kyu

AU - Kim, Jong In

AU - Lee, Taehoon G.

AU - Suh, Pann Ghill

AU - Ryu, Sung Ho

PY - 2006/3

Y1 - 2006/3

N2 - We introduce a new methodology named ligand profiling and identification for effective discovery of bioactive ligands such as peptide hormones. This technology was developed from a new concept of parallel column chromatography and active fraction profiling by nano-LC MS. Traditional methods use sequential column chromatography, and thus are inevitably limited by the low abundance of the peptide of interest and by a low yield due to the many column steps. Using this new technology, insulin was successfully identified and diarginylinsulin, a minor intermediate form of insulin, was unexpectedly also identified simultaneously from 100 mg of porcine pancreatic tissue. This integrative technology could be used to search for various low-abundance peptides (or bioactive molecules) rapidly and simultaneously, by applying this to the later stages of traditional sequential purification.

AB - We introduce a new methodology named ligand profiling and identification for effective discovery of bioactive ligands such as peptide hormones. This technology was developed from a new concept of parallel column chromatography and active fraction profiling by nano-LC MS. Traditional methods use sequential column chromatography, and thus are inevitably limited by the low abundance of the peptide of interest and by a low yield due to the many column steps. Using this new technology, insulin was successfully identified and diarginylinsulin, a minor intermediate form of insulin, was unexpectedly also identified simultaneously from 100 mg of porcine pancreatic tissue. This integrative technology could be used to search for various low-abundance peptides (or bioactive molecules) rapidly and simultaneously, by applying this to the later stages of traditional sequential purification.

KW - Identification

KW - Ligand

KW - Peptidome

KW - Profiling

UR - https://www.scopus.com/pages/publications/33645472063

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DO - 10.1002/pmic.200500511

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JO - Proteomics

JF - Proteomics

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ER -

Ligand profiling and identification technology for searching bioactive ligands

Abstract

Keywords

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