Syntheses and SAR studies of 4-(heteroarylpiperdin-1-yl-methyl)-pyrrolidin-1-yl-acetic acid antagonists of the human CCR5 chemokine receptor.

Kothandaraman Shankaran,Karla L. Donnelly,Shrenik K. Shah,Ravindra N. Guthikonda,Malcolm Maccoss,Sander G. Mills,Sandra L. Gould,Lorraine Malkowitz,Salvatore J. Siciliano,Martin S. Springer,Anthony Carella,Gwen Carver,Daria J. Hazuda,Karen Holmes,Joseph Kessler,Janet Lineberger,Michael D. Miller,Emilio A. Emini,William A. Schleif

Syntheses and SAR studies of 4-(heteroarylpiperdin-1-yl-methyl)-pyrrolidin-1-yl-acetic acid antagonists of the human CCR5 chemokine receptor.

2004

Kothandaraman Shankaran
Karla L. Donnelly
Shrenik K. Shah
Ravindra N. Guthikonda
Malcolm Maccoss
Sander G. Mills
Sandra L. Gould
Lorraine Malkowitz
Salvatore J. Siciliano
Martin S. Springer
Anthony Carella
Gwen Carver
Daria J. Hazuda
Karen Holmes
Joseph Kessler
Janet Lineberger
Michael D. Miller
Emilio A. Emini
William A. Schleif

Efforts toward the exploration of the title compounds as CCR5 antagonists are disclosed. The basis for such work stems from the fact that cellular proliferation of HIV-1 requires the cooperative assistance of both CCR5 and CD4 receptors. The synthesis and SAR of pyrrolidineacetic acid derivatives as CCR5 antagonists displaying potent binding and antiviral properties in a HeLa cell-based HIV-1 infectivity assay are discussed.

Keywords:

HeLa
Chemical synthesis
Chemokine receptor
Cell
Organic chemistry
Carboxylic acid
Structure–activity relationship
Stereochemistry
Biochemistry
In vitro
Acetic acid
Chemistry
Binding site

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations