Design, syntheses and biological evaluations of nonpeptidic caspase 3 inhibitors

Eun sook Kim; Sung eun Yoo; Kyu Yang Yi; Sunkyung Lee; Jae sung Noh; Yong Sam Jung; Eunhee Kim; Nakcheol Jeong

doi:10.5012/bkcs.2002.23.7.1003

Design, syntheses and biological evaluations of nonpeptidic caspase 3 inhibitors

Eun sook Kim, Sung eun Yoo, Kyu Yang Yi, Sunkyung Lee, Jae sung Noh, Yong Sam Jung, Eunhee Kim, Nakcheol Jeong

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

12 Citations (Scopus)

Abstract

Caspase 3, a member of cysteine protease family, is well known as a major apoptosis effector and is involved in cell death as a result of ischemic diseases such as stroke and myocardial infarction, therefore the inhibition of caspase 3 may protect those apoptotic cell damages. During the high-throughput screening of the compounds from the Korea Chemical Bank, berberine derivatives (A and B), an isoquinoline alkaloid, have been identified as potential inhibitors for caspase 3. Based on this finding we carried out molecular modeling study to identify the pharmacophoric elements of berberine structure which interact with a substrate-recognition binding site of caspase 3 and came up with several novel scaffolds. In this report, we will discuss the molecular modeling, syntheses and the enzyme inhibitory activities of these novel compounds.

Original language	English
Pages (from-to)	1003-1010
Number of pages	8
Journal	Bulletin of the Korean Chemical Society
Volume	23
Issue number	7
DOIs	https://doi.org/10.5012/bkcs.2002.23.7.1003
Publication status	Published - 2002 Jul 20

Keywords

Apoptosis
Caspase 3
Isoquinoline derivatives
Nonpeptidic inhibitor

ASJC Scopus subject areas

General Chemistry

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10.5012/bkcs.2002.23.7.1003

Cite this

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title = "Design, syntheses and biological evaluations of nonpeptidic caspase 3 inhibitors",

abstract = "Caspase 3, a member of cysteine protease family, is well known as a major apoptosis effector and is involved in cell death as a result of ischemic diseases such as stroke and myocardial infarction, therefore the inhibition of caspase 3 may protect those apoptotic cell damages. During the high-throughput screening of the compounds from the Korea Chemical Bank, berberine derivatives (A and B), an isoquinoline alkaloid, have been identified as potential inhibitors for caspase 3. Based on this finding we carried out molecular modeling study to identify the pharmacophoric elements of berberine structure which interact with a substrate-recognition binding site of caspase 3 and came up with several novel scaffolds. In this report, we will discuss the molecular modeling, syntheses and the enzyme inhibitory activities of these novel compounds.",

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T1 - Design, syntheses and biological evaluations of nonpeptidic caspase 3 inhibitors

AU - Kim, Eun sook

AU - Yoo, Sung eun

AU - Yi, Kyu Yang

AU - Lee, Sunkyung

AU - Noh, Jae sung

AU - Jung, Yong Sam

AU - Kim, Eunhee

AU - Jeong, Nakcheol

PY - 2002/7/20

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AB - Caspase 3, a member of cysteine protease family, is well known as a major apoptosis effector and is involved in cell death as a result of ischemic diseases such as stroke and myocardial infarction, therefore the inhibition of caspase 3 may protect those apoptotic cell damages. During the high-throughput screening of the compounds from the Korea Chemical Bank, berberine derivatives (A and B), an isoquinoline alkaloid, have been identified as potential inhibitors for caspase 3. Based on this finding we carried out molecular modeling study to identify the pharmacophoric elements of berberine structure which interact with a substrate-recognition binding site of caspase 3 and came up with several novel scaffolds. In this report, we will discuss the molecular modeling, syntheses and the enzyme inhibitory activities of these novel compounds.

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KW - Caspase 3

KW - Isoquinoline derivatives

KW - Nonpeptidic inhibitor

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Design, syntheses and biological evaluations of nonpeptidic caspase 3 inhibitors

Abstract

Keywords

ASJC Scopus subject areas

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