Margaret Browne scite author profile

A series of azetidinone cholesterol absorption inhibitors related to SCH 48461 ((-)-6) has been prepared, and compounds were evaluated for their ability to inhibit hepatic cholesteryl ester formation in a cholesterol-fed hamster model. Although originally designed as acyl CoA: cholesterol acyltransferase (ACAT) inhibitors, comparison of in vivo potency with in vitro activity in a microsomal ACAT assay indicates no correlation between activity in these two models. The molecular mechanism by which these compounds inhibit cholesterol absorption is unknown. Despite this limitation, examination of the in vivo activity of a range of compounds has revealed clear structure-activity relationships consistent with a well-defined molecular target. The details of these structure-activity relationships and their implications on the nature of the putative pharmacophore are discussed.

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Intramolecular arylations of soft enolates catalyzed by zerovalent palladium

Ciufolini¹,

Qi²,

Browne³

1988

J. Org. Chem.

100

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Trans diastereoselective synthesis of 3-alkyl substituted β-lactams via the acid chloride-imine reaction of nonactivated acid chlorides

Browne¹,

Burnett²,

Caplen³

et al. 1995

Tetrahedron Letters

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The Influence of Television News Depictions of the Images of War on Viewers

Pfau

Haigh

Shannon

et al. 2008

Journal of Broadcasting & Electronic Media

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Efficient palladium-mediated synthesis of a spirocyclic model for fredericamycin A.

Ciufolini

Browne

1987

Tetrahedron Letters

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Margaret Browne

2-Azetidinone Cholesterol Absorption Inhibitors: Structure−Activity Relationships on the Heterocyclic Nucleus

Intramolecular arylations of soft enolates catalyzed by zerovalent palladium

Trans diastereoselective synthesis of 3-alkyl substituted β-lactams via the acid chloride-imine reaction of nonactivated acid chlorides

The Influence of Television News Depictions of the Images of War on Viewers

Efficient palladium-mediated synthesis of a spirocyclic model for fredericamycin A.

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