John B. Etienne scite author profile

We have explored the use of steroidal glycosides as cholesterol absorption inhibitors which act through an unknown mechanism. The lead for this program was tigogenin cellobioside (1, tiqueside) which is a weak inhibitor (ED50 = 60 mg/kg) as measured in an acute hamster cholesterol absorption assay. Modification of the steroid portion of the molecule led to the discovery of 11-ketotigogenin cellobioside (5, pamaqueside) which has an ED50 of 2 mg/kg. Replacement of the cellobiose with other sugars failed to provide more potent analogs. However, large improvements in potency were realized through modification of the hydroxyl groups on the cellobiose. This strategy ultimately led to the 4", 6"-bis[(2-fluorophenyl)carbamoyl]-beta-D-cellobiosyl derivative of 11-ketotigogenin (51) with an ED50 of 0.025 mg/kg in the hamster assay, as well as the corresponding hecogenin analog 64 (ED50 = 0.07 mg/kg).

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1,5-Substituted nipecotic amides: Selective PDE8 inhibitors displaying diastereomer-dependent microsomal stability

DeNinno

Wright

Visser

et al. 2011

Bioorganic & Medicinal Chemistry Letters

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John B. Etienne

A method for the selective reduction of carbohydrate 4,6-O-benzylidene acetals

The discovery of potent, selective, and orally bioavailable PDE9 inhibitors as potential hypoglycemic agents

3‘-Aminoadenosine-5‘-uronamides: Discovery of the First Highly Selective Agonist at the Human Adenosine A₃ Receptor

Steroidal Glycoside Cholesterol Absorption Inhibitors

1,5-Substituted nipecotic amides: Selective PDE8 inhibitors displaying diastereomer-dependent microsomal stability

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John B. Etienne

A method for the selective reduction of carbohydrate 4,6-O-benzylidene acetals

The discovery of potent, selective, and orally bioavailable PDE9 inhibitors as potential hypoglycemic agents

3‘-Aminoadenosine-5‘-uronamides: Discovery of the First Highly Selective Agonist at the Human Adenosine A3 Receptor

Steroidal Glycoside Cholesterol Absorption Inhibitors

1,5-Substituted nipecotic amides: Selective PDE8 inhibitors displaying diastereomer-dependent microsomal stability

Contact Info

Product

Resources

About

3‘-Aminoadenosine-5‘-uronamides: Discovery of the First Highly Selective Agonist at the Human Adenosine A₃ Receptor