A Biocatalytic Approach to a Key Intermediate for the Synthesis of the COVID-19 Experimental Drug Molnupiravir

Ashleigh Burke; William Birmingham; Ying Zhuo; Bruna Zuculoto da Costa; Rebecca Crawshaw; Thomas Thorpe; Ian Rowles; James Finnigan; Simon J. Charnock; Sarah Lovelock; Nicholas Turner; Anthony Green

doi:10.26434/chemrxiv.13721692.v1

Catalysis

Search within Catalysis

A Biocatalytic Approach to a Key Intermediate for the Synthesis of the COVID-19 Experimental Drug Molnupiravir

08 February 2021, Version 1

This is not the most recent version. There is a

newer version

of this content available

Working Paper

Show author details

This content is a preprint and has not undergone peer review at the time of posting.

Abstract

Herein we report the conversion of cytidine 2 to N-hydroxycytidine 7 catalysed by cytidine deaminase (CD). The wild-type enzyme operates efficiently at high sustrate loadings and hydroxylamine concentrations to favor N-hydroxy-cytidine formation over uridine. Although the wild-type enzyme demonstrated good activity, we were able to further enhance the ratio of N-hydroxycytidine to uridine produced through directed evolution of CD. In particular, a T123G mutation close to the active site dramatically reduces cytidine hydrolysis activity whilst preserving desired amination activty. The approach reported provides a new route to a key intermediate for the COVID-19 experimental drug Molnupiravir 1.

Keywords

COVID_19

biocatalysis

Molnupiravir

Comments

Comments are not moderated before they are posted, but they can be removed by the site moderators if they are found to be in contravention of our Commenting Policy - please read this policy before you post. Comments should be used for scholarly discussion of the content in question. You can find more information about how to use the commenting feature here .

This site is protected by reCAPTCHA and the Google Privacy Policy and Terms of Service apply.