Selecting a stable solid form of remdesivir using microcrystal electron diffraction and crystal structure prediction

Sivakumar Sekharan; Xuetao Liu; Zhuocen Yang; Xiang Liu; Li Deng; Shigang Ruan; Yuriy Abramov; GuangXu Sun; Sizhu Li; Tian Zhou; Baime Shi; Qun Zeng; Qiao Zeng; Chao Chang; Yingdi Jin; Xuekun Shi

doi:10.1039/d1ra03100g

Selecting a stable solid form of remdesivir using microcrystal electron diffraction and crystal structure prediction

RSC Adv. 2021 May 12;11(28):17408-17412. doi: 10.1039/d1ra03100g. eCollection 2021 May 6.

Authors

Sivakumar Sekharan¹, Xuetao Liu², Zhuocen Yang², Xiang Liu², Li Deng², Shigang Ruan², Yuriy Abramov¹, GuangXu Sun², Sizhu Li², Tian Zhou², Baime Shi², Qun Zeng², Qiao Zeng², Chao Chang², Yingdi Jin², Xuekun Shi²

Affiliations

¹ XtalPi Inc. 245 Main St, Floor 11 Cambridge MA 02142 USA sivakumar.sekharan@xtalpi.com.
² Jingtai Technology Co. Ltd Floor 4, No. 9, Yifenghua Industrial Zone, 91 Huaning Road, Longhua District Shenzhen Guangdong Province 518109 China.

Abstract

Therapeutic options in response to the coronavirus disease 2019 (COVID-19) outbreak are urgently needed. In this communication, we demonstrate how to support selection of a stable solid form of an antiviral drug remdesivir in quick time using the microcrystal electron diffraction (MicroED) technique and a cloud-based and artificial intelligence implemented crystal structure prediction platform. We present the MicroED structures of remdesivir forms II and IV and conclude that form II is more stable than form IV at ambient temperature in agreement with experimental observations. The combined experimental and theoretical study can serve as a template for formulation scientists in the pharmaceutical industry.