Process Development of a Macrocyclic Peptide Inhibitor of PD-L1.
Subha MukherjeeAmanda RogersGardner CreechChao HangAntonio RamirezMichael DummeldingerShawn BrueggemeierClaudio MapelliSerge ZaretskyMasano HuangRegina BlackMichael B PeddicordNicolas CuniereJames KempsonJoseph PawluczykMartin AllenRodney ParsonsChris SfouggatakisPublished in: The Journal of organic chemistry (2024)
This article outlines the process development leading to the manufacture of 800 g of BMS-986189, a macrocyclic peptide active pharmaceutical ingredient. Multiple N-methylated unnatural amino acids posed challenges to manufacturing due to the lability of the peptide to cleavage during global side chain deprotection and precipitation steps. These issues were exacerbated upon scale-up, resulting in severe yield loss and necessitating careful impurity identification, understanding the root cause of impurity formation, and process optimization to deliver a scalable synthesis. A systematic study of macrocyclization with its dependence on concentration and pH is presented. In addition, a side chain protected peptide synthesis is discussed where the macrocyclic protected peptide is extremely labile to hydrolysis. A computational study explains the root cause of the increased lability of macrocyclic peptide over linear peptide to hydrolysis. A process solution involving the use of labile protecting groups is discussed. Overall, the article highlights the advancements achieved to enable scalable synthesis of an unusually labile macrocyclic peptide by solid-phase peptide synthesis. The sustainability metric indicates the final preparative chromatography drives a significant fraction of a high process mass intensity (PMI).