Structure-based Design of Prefusion-stabilized SARS-CoV-2 Spikes

Author:

Hsieh Ching-Lin,Goldsmith Jory A.,Schaub Jeffrey M.,DiVenere Andrea M.,Kuo Hung-Che,Javanmardi Kamyab,Le Kevin C.,Wrapp Daniel,Lee Alison Gene-Wei,Liu Yutong,Chou Chia-Wei,Byrne Patrick O.,Hjorth Christy K.,Johnson Nicole V.,Ludes-Meyers John,Nguyen Annalee W.,Park Juyeon,Wang Nianshuang,Amengor Dzifa,Maynard Jennifer A.,Finkelstein Ilya J.,McLellan Jason S.ORCID

Abstract

ABSTRACTThe COVID-19 pandemic caused by the novel coronavirus SARS-CoV-2 has led to accelerated efforts to develop therapeutics, diagnostics, and vaccines to mitigate this public health emergency. A key target of these efforts is the spike (S) protein, a large trimeric class I fusion protein that is metastable and difficult to produce recombinantly in large quantities. Here, we designed and expressed over 100 structure-guided spike variants based upon a previously determined cryo-EM structure of the prefusion SARS-CoV-2 spike. Biochemical, biophysical and structural characterization of these variants identified numerous individual substitutions that increased protein yields and stability. The best variant, HexaPro, has six beneficial proline substitutions leading to ∼10-fold higher expression than its parental construct and is able to withstand heat stress, storage at room temperature, and multiple freeze-thaws. A 3.2 Å-resolution cryo-EM structure of HexaPro confirmed that it retains the prefusion spike conformation. High-yield production of a stabilized prefusion spike protein will accelerate the development of vaccines and serological diagnostics for SARS-CoV-2.

Publisher

Cold Spring Harbor Laboratory

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