Structure-Activity Relationships of Ligand Binding to Oxysterol-Binding Protein (OSBP) and OSBP-Related Protein 4

被引:5
|
作者
Severance, Zachary C. [1 ,2 ]
Nunez, Juan I. [1 ]
Le-McClain, Anh T. [1 ]
Malinky, Cori A. [1 ]
Bensen, Ryan C. [1 ]
Fogle, Robert S. [2 ]
Manginelli, Gianni W. [1 ]
Sakers, Sophia H. [1 ]
Falcon, Emily C. [2 ]
Bui, Richard Hoang [2 ]
Snead, Kevin J. [1 ]
Bourne, Christina R. [1 ]
Burgett, Anthony W. G. [1 ,2 ,3 ]
机构
[1] Univ Oklahoma, Dept Chem & Biochem, Norman, OK 73019 USA
[2] Univ Oklahoma, Hlth Sci Ctr, Dept Pharmaceut Sci, Oklahoma City, OK 73117 USA
[3] Univ Oklahoma, Hlth Sci Ctr, Stephenson Canc Ctr, Oklahoma City, OK 73104 USA
关键词
ENTEROVIRUS REPLICATION; CELL-PROLIFERATION; OXYGENATED STEROLS; CDNA CLONING; CHOLESTEROL; TRANSPORT; REVEALS; FAMILY; INHIBITION; EXPRESSION;
D O I
10.1021/acs.jmedchem.2c01025
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Oxysterol-binding protein (OSBP) and OSBP-related protein 4 (ORP4) have emerged as potentially druggable targets in antiviral and precision cancer drug development. Multiple structurally diverse small molecules function through targeting the OSBP/ORP family of proteins, including the antiviral steroidal compounds OSW-1 and T-00127-HEV2. Here, the structure-acti v i t y relationships of oxysterols and related compound binding to human OSBP and ORP4 are characterized. Oxysterols with hydroxylation at various side chain positions (i.e., C-20, C-24, C-25, and C-27)-but not C-22-confer high affinity interactions with OSBP and ORP4. A library of 20(S)-hydroxycholesterol analogues with varying sterol side chains reveal that side chain length modifications are not well tolerated for OSBP and ORP4 interactions. This side chain requirement is contradicted by the high affinity binding of T-00127-HEV2, a steroidal compound lacking the side chain. The binding results, in combination with docking studies using homology models of OSBP and ORP4, suggest multiple modes of steroidal ligand binding to OSBP and ORP4.
引用
收藏
页码:3866 / 3875
页数:10
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