Discovery of MK-8718, an HIV Protease Inhibitor Containing a Novel Morpholine Aspartate Binding Group

Christopher J Bungard; Peter D Williams; Jeanine E Ballard; David J Bennett; Christian Beaulieu; Carolyn Bahnck-Teets; Steve S Carroll; Ronald K Chang; David C Dubost; John F Fay; Tracy L Diamond; Thomas J Greshock; Li Hao; M Katharine Holloway; Peter J Felock; Jennifer J Gesell; Hua-Poo Su; Jesse J Manikowski; Daniel J McKay; Mike Miller; Xu Min; Carmela Molinaro; Oscar M Moradei; Philippe G Nantermet; Christian Nadeau; Rosa I Sanchez; Tummanapalli Satyanarayana; William D Shipe; Sanjay K Singh; Vouy Linh Truong; Sivalenka Vijayasaradhi; Catherine M Wiscount; Joseph P Vacca; Sheldon N Crane; John A McCauley

doi:10.1021/acsmedchemlett.6b00135

Discovery of MK-8718, an HIV Protease Inhibitor Containing a Novel Morpholine Aspartate Binding Group

ACS Med Chem Lett. 2016 May 9;7(7):702-7. doi: 10.1021/acsmedchemlett.6b00135. eCollection 2016 Jul 14.

Authors

Christopher J Bungard¹, Peter D Williams¹, Jeanine E Ballard¹, David J Bennett¹, Christian Beaulieu², Carolyn Bahnck-Teets¹, Steve S Carroll¹, Ronald K Chang¹, David C Dubost¹, John F Fay¹, Tracy L Diamond¹, Thomas J Greshock¹, Li Hao³, M Katharine Holloway¹, Peter J Felock¹, Jennifer J Gesell¹, Hua-Poo Su¹, Jesse J Manikowski¹, Daniel J McKay², Mike Miller¹, Xu Min¹, Carmela Molinaro¹, Oscar M Moradei², Philippe G Nantermet¹, Christian Nadeau², Rosa I Sanchez¹, Tummanapalli Satyanarayana³, William D Shipe¹, Sanjay K Singh³, Vouy Linh Truong², Sivalenka Vijayasaradhi³, Catherine M Wiscount¹, Joseph P Vacca², Sheldon N Crane², John A McCauley¹

Affiliations

¹ Merck Research Laboratories , 770 Sumneytown Pike, PO Box 4, West Point, Pennsylvania 19486, United States.
² Merck Frosst Centre for Therapeutic Research , 16711 TransCanada Highway, Kirkland, Quebec H9H 3L1, Canada.
³ Albany Molecular Research Singapore Research Center , 61 Science Park Road #05-01, The Galen Singapore Science Park II, Singapore 117525.

Abstract

A novel HIV protease inhibitor was designed using a morpholine core as the aspartate binding group. Analysis of the crystal structure of the initial lead bound to HIV protease enabled optimization of enzyme potency and antiviral activity. This afforded a series of potent orally bioavailable inhibitors of which MK-8718 was identified as a compound with a favorable overall profile.

Keywords: HIV; MK-8718; inhibitor; protease.