학술논문
Practical Asymmetric Synthesis of a Calcitonin Gene-Related Peptide (CGRP) Receptor Antagonist Ubrogepant
Document Type
Article
Author
Yasuda, Nobuyoshi; Cleator, Ed; Kosjek, Birgit; Yin, Jianguo; Xiang, Bangping; Chen, Frank; Kuo, Shen-Chun; Belyk, Kevin; Mullens, Peter R.; Goodyear, Adrian; Edwards, John S.; Bishop, Brian; Ceglia, Scott; Belardi, Justin; Tan, Lushi; Song, Zhiguo J.; DiMichele, Lisa; Reamer, Robert; Cabirol, Fabien L.; Tang, Weng Lin; Liu, Guiquan
Source
Organic Process Research & Development; 20240101, Issue: Preprints
Subject
Language
ISSN
10836160; 1520586X
Abstract
The development of a scalable asymmetric route to a new calcitonin gene-related peptide (CGRP) receptor antagonist is described. The synthesis of the two key fragments was redefined, and the intermediates were accessed through novel chemistry. Chiral lactam 2was prepared by an enzyme mediated dynamic kinetic transamination which simultaneously set two stereocenters. Enzyme evolution resulted in an optimized transaminase providing the desired configuration in >60:1 syn/anti. The final chiral center was set via a crystallization induced diastereomeric transformation. The asymmetric spirocyclization to form the second fragment, chiral spiro acid intermediate 3, was catalyzed by a novel doubly quaternized phase transfer catalyst and provided optically pure material on isolation. With the two fragments in hand, development of their final union by amide bond formation and subsequent direct isolation is described. The described chemistry has been used to deliver over 100 kg of our desired target, ubrogepant.