E. W. Collington scite author profile

Despite numerous suggestions in the literature that thromboxane A2 is involved in a variety of occlusive vascular diseases, no definitive evidence is available. Arguments have been presented to support the view that such evidence can only come from clinical studies with a highly specific thromboxane receptor-blocking drug. We have now identified such a drug, AH23848, in our laboratories. Preliminary experiments with AH23848, ([la(Z) show that it is a potent, specific thromboxane receptor-blocking drug that is orally active and has a long duration of action. It should be a valuable tool in elucidating any physiologic or pathologic role of thromboxane A2.

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Selective deprotection of alcoholic and phenolic silyl ethers

Collington

Finch

Smith

1985

Tetrahedron Letters

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α-Fluoromethyl-n-methyl-phenylsulphoximine: a new fluoromethylenation reagent

Boys

Collington

Finch

et al. 1988

Tetrahedron Letters

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Syntheses via-2-oxazolines. I. Formylation of Grignard reagents in the presence of hexamethylphosphoramide

Meyers¹,

Collington²

1970

J. Am. Chem. Soc.

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Facile and specific conversion of allylic alcohols to allylic chlorides without rearrangement

Meyers¹,

Collington²

1971

J. Org. Chem.

175

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E. W. Collington

AH23848: a thromboxane receptor-blocking drug that can clarify the pathophysiologic role of thromboxane A2.

Selective deprotection of alcoholic and phenolic silyl ethers

α-Fluoromethyl-n-methyl-phenylsulphoximine: a new fluoromethylenation reagent

Syntheses via-2-oxazolines. I. Formylation of Grignard reagents in the presence of hexamethylphosphoramide

Facile and specific conversion of allylic alcohols to allylic chlorides without rearrangement

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