A series of alkylamido- (1) and alkylaminobiphenyl (2) derivs. were synthesized as possible bioisosters of reported ACAT inhibitors phenylpyridazine analogs. Both 1 and 2 were tested on the human ACAT-1 and ACAT-2 isoforms. The amino derivs. 2 were found to be inactive, contrary to the related pyridazine derivs. By contrast, the ortho-substituted amides 1a and 1d showed an interesting activity. These results support the essential role of the pyridazine nucleus. Modeling studies were also performed
Biphenyl versus phenylpyridazine derivatives : the role of the heterocycle in a series of acyl-CoA : cholesterol acyl transferase inhibitors / A. Gelain, D. Barlocco, B.M. Kwon, T.S. Jeong, K.R. Im, L. Legnani, L. Toma. - In: JOURNAL OF MEDICINAL CHEMISTRY. - ISSN 0022-2623. - 51:5(2008), pp. 1474-1477.
Biphenyl versus phenylpyridazine derivatives : the role of the heterocycle in a series of acyl-CoA : cholesterol acyl transferase inhibitors
A. GelainPrimo
;D. BarloccoSecondo
;
2008
Abstract
A series of alkylamido- (1) and alkylaminobiphenyl (2) derivs. were synthesized as possible bioisosters of reported ACAT inhibitors phenylpyridazine analogs. Both 1 and 2 were tested on the human ACAT-1 and ACAT-2 isoforms. The amino derivs. 2 were found to be inactive, contrary to the related pyridazine derivs. By contrast, the ortho-substituted amides 1a and 1d showed an interesting activity. These results support the essential role of the pyridazine nucleus. Modeling studies were also performed
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