What question did this study set out to answer?

This research aims to create a more efficient method for producing the STING agonist MK-2118 using biocatalysis.

March 7, 2026

A Chemoenzymatic Synthesis of STING Agonist MK-2118

Key Points

This research aims to create a more efficient method for producing the STING agonist MK-2118 using biocatalysis.
Engineered an enoate-reductase for a key reduction step
Developed a 4-step chemoenzymatic synthetic route
Achieved rapid evolution of Z-selective ERED within 2 months
Produced >10 kg of MK-2118 from simple starting materials
Achieved >40% overall yield of MK-2118
Obtained product with >99% enantiomeric excess
Successfully delivered large quantities for clinical trials

Abstract

Pharmaceutical companies are increasingly leveraging the power of biocatalysis to enable the development of concise and robust commercial manufacturing processes for their therapeutics. Yet, implementation of biocatalysis via protein engineering often requires years to generate a production-ready enzyme. To enable rapid clinical supply, we engineered an enoate-reductase (ERED) to catalyze a key asymmetric reduction in a concise 4-step chemoenzymatic route toward the orally bioavailable STING agonist MK-2118. Within 2 months, we evolved a Z-selective ERED with high activity that delivered the desired product in high yield and exquisite enantioselectivity. The 4-step chemoenzymatic process was used to successfully deliver >10 kg of MK-2118 from readily available starting materials at 40% overall yield and >99% ee to accelerate clinical trials.

A Chemoenzymatic Synthesis of STING Agonist MK-2118

Key Points

Abstract

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