Identification of novel ligands for the Z-DNA binding protein by structure-based virtual screening

Yang Gyun Kim; Khac Minh Thai; Jieun Song; Kyeong Kyu Kim; Hyun Ju Park

doi:10.1248/cpb.55.340

Identification of novel ligands for the Z-DNA binding protein by structure-based virtual screening

Yang Gyun Kim
, Khac Minh Thai
, Jieun Song
, Kyeong Kyu Kim
, Hyun Ju Park

Department of Pharmacy

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

7 Scopus citations

Abstract

We describe the first discovery of small molecules that bind to the Z-DNA binding domain of human ADAR1 (Adenosine Deaminase Acting on RNA 1) by structure-based virtual screening of chemical database. These molecules bind to Z-DNA binding domain to inhibit the interaction with the Z-DNA. Many viruses have Z-DNA binding proteins, which are structurally similar to Z-DNA binding domain of human ADAR1, and the ability of Z-DNA binding protein to bind the Z-DNA is essential for their pathogenicity. Therefore, the molecules identified in this study may serve as novel leads for the design of agents that inhibit biological functions of those pathogenic viruses.

Original language	English
Pages (from-to)	340-342
Number of pages	3
Journal	Chemical and Pharmaceutical Bulletin
Volume	55
Issue number	2
DOIs	https://doi.org/10.1248/cpb.55.340
State	Published - Feb 2007

Keywords

Structure-based virtual screening
Z-DNA
Z-DNA binding domain

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1248/cpb.55.340

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title = "Identification of novel ligands for the Z-DNA binding protein by structure-based virtual screening",

abstract = "We describe the first discovery of small molecules that bind to the Z-DNA binding domain of human ADAR1 (Adenosine Deaminase Acting on RNA 1) by structure-based virtual screening of chemical database. These molecules bind to Z-DNA binding domain to inhibit the interaction with the Z-DNA. Many viruses have Z-DNA binding proteins, which are structurally similar to Z-DNA binding domain of human ADAR1, and the ability of Z-DNA binding protein to bind the Z-DNA is essential for their pathogenicity. Therefore, the molecules identified in this study may serve as novel leads for the design of agents that inhibit biological functions of those pathogenic viruses.",

keywords = "Structure-based virtual screening, Z-DNA, Z-DNA binding domain",

author = "Kim, \{Yang Gyun\} and Thai, \{Khac Minh\} and Jieun Song and Kim, \{Kyeong Kyu\} and Park, \{Hyun Ju\}",

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AU - Thai, Khac Minh

AU - Song, Jieun

AU - Kim, Kyeong Kyu

AU - Park, Hyun Ju

PY - 2007/2

Y1 - 2007/2

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AB - We describe the first discovery of small molecules that bind to the Z-DNA binding domain of human ADAR1 (Adenosine Deaminase Acting on RNA 1) by structure-based virtual screening of chemical database. These molecules bind to Z-DNA binding domain to inhibit the interaction with the Z-DNA. Many viruses have Z-DNA binding proteins, which are structurally similar to Z-DNA binding domain of human ADAR1, and the ability of Z-DNA binding protein to bind the Z-DNA is essential for their pathogenicity. Therefore, the molecules identified in this study may serve as novel leads for the design of agents that inhibit biological functions of those pathogenic viruses.

KW - Structure-based virtual screening

KW - Z-DNA

KW - Z-DNA binding domain

UR - https://www.scopus.com/pages/publications/33846981922

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SN - 0009-2363

VL - 55

SP - 340

EP - 342

JO - Chemical and Pharmaceutical Bulletin

JF - Chemical and Pharmaceutical Bulletin

IS - 2

ER -

Identification of novel ligands for the Z-DNA binding protein by structure-based virtual screening

Abstract

Keywords

UN SDGs

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