Process Development of the HCV NS5B Site D Inhibitor MK-8876

Michael J. Williams,Qinghao Chen,Lorenzo Codan,Renee K. Dermenjian,Spencer D. Dreher,Andrew W. Gibson,Xianliang He,Yan Jin,Stephen P. Keen,Alfred Y. Lee,David R. Lieberman,Wei Lin,Guiquan Liu,Mark McLaughlin,Mikhail Reibarkh,Jeremy P. Scott,Sophie Strickfuss,Lushi Tan,Richard J. Varsolona,Feng Wen

Process Development of the HCV NS5B Site D Inhibitor MK-8876

2016

We describe the route development and multikilogram-scale synthesis of an HCV NS5B site D inhibitor, MK-8876. The key topics covered are (1) process improvement of the two main fragments; (2) optimization of the initially troublesome penultimate step, a key bis(boronic acid) (BBA)-based borylation; (3) process development of the final Suzuki–Miyaura coupling; and (4) control of the drug substance form. These efforts culminated in a 28 kg delivery of the desired active pharmaceutical ingredient.

Keywords:

Borylation
Organic chemistry
NS5B
Boronic acid
Chemistry
Active ingredient
process improvement
process development

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