TitleDesign and Synthesis of Tri-substituted Chiral Pyrrolidin-2-one Derivatives as CCR4 Antagonists
AuthorsSun, Wei
Tian, Linjie
Qi, Hui
Jiang, Dan
Wang, Ying
Li, Song
Xiao, Junhai
Yang, Xiaohong
AffiliationJilin Univ, Sch Pharmaceut Sci, Changchun 130021, Jilin, Peoples R China.
Beijing Inst Pharmacol & Toxicol, Lab Computer Aided Drug Design & Discovery, Beijing 100850, Peoples R China.
Peking Univ, Ctr Human Dis Genom, Beijing 100083, Peoples R China.
KeywordsCCR4 antagonists
tri-substituted chiral pyrrolidin-2-one derivatives
synthesis
CHEMOKINE-LIKE FACTOR-1
MOLECULAR-CLONING
FUNCTIONAL LIGAND
RECEPTOR 4
T-CELLS
EXPRESSION
TARC
Issue Date2013
Publisher中国化学英文版
CitationCHINESE JOURNAL OF CHEMISTRY.2013,31,(9,SI),1144-1152.
AbstractA series of tri-substituted chiral pyrrolidin-2-one derivatives have been designed and synthesized as CC chemokine receptor 4 (CCR4) antagonists. The structure of CCR4 was built by homology modeling. Asymmetric synthesis was applied to synthesize the R,R configuration chiral pyrrolidin-2-one scaffold. The stereoisomeric configurations of the compounds were identified by 2D H-1-H-1 COSY spectroscopy and 1D NOESY spectroscopy. This method was more economical and convenient than traditional X-ray single crystal diffraction. In addition, the interactions between these compounds and the N-terminal extracellular tail of CCR4 were studied using capillary zone electrophoresis. The CCR4 chemotaxis inhibition effect was tested in CCR4-transfected HEK293 cells. Several compounds showed potent activities as CCR4 antagonists. Among these compounds, 1c is the most active one. Its apparent binding constant of CZE experiment result is (1.569 +/- 0.11)x10(5) L<bold></bold>mol(-1), and its percentage inhibition of the HEK293/CCR4 cells migration with the concentration of 1 mu mol<bold></bold>L-1 in DMSO is 59%. And compound 1f has slightly higher affinity to N-terminal of CCR4 according to its apparent binding constant than 1b because of the introduced ester linkage. Further studies on the mechanism of these compounds are in progress.
URIhttp://hdl.handle.net/20.500.11897/220821
ISSN1001-604X
DOI10.1002/cjoc.201300363
IndexedSCI(E)
中国科学引文数据库(CSCD)
Appears in Collections:待认领

Web of Science®



Checked on Last Week

Scopus®



Checked on Current Time

百度学术™



Checked on Current Time

Google Scholar™





License: See PKU IR operational policies.