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Emergent SARS-CoV-2 variants: comparative replication dynamics and high sensitivity to thapsigargin

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Taylor & Francis Group2024-03-21 更新2026-04-16 收录
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https://tandf.figshare.com/articles/dataset/Emergent_SARS-CoV-2_variants_comparative_replication_dynamics_and_high_sensitivity_to_thapsigargin/17041679
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The struggle to control the COVID-19 pandemic is made challenging by the emergence of virulent SARS-CoV-2 variants. To gain insight into their replication dynamics, emergent Alpha (A), Beta (B) and Delta (D) SARS-CoV-2 variants were assessed for their infection performance in single variant- and co-infections. The effectiveness of thapsigargin (TG), a recently discovered broad-spectrum antiviral, against these variants was also examined. Of the 3 viruses, the D variant exhibited the highest replication rate and was most able to spread to in-contact cells; its replication rate at 24 h post-infection (hpi) based on progeny viral RNA production was over 4 times that of variant A and 9 times more than the B variant. In co-infections, the D variant boosted the replication of its co-infected partners at the expense of its own initial performance. Furthermore, co-infection with AD or AB combination conferred replication synergy where total progeny (RNA) output was greater than the sum of corresponding single-variant infections. All variants were highly sensitive to TG inhibition. A single pre-infection priming dose of TG effectively blocked all single-variant infections and every combination (AB, AD, BD variants) of co-infection at greater than 95% (relative to controls) at 72 hpi. Likewise, TG was effective in inhibiting each variant in active preexisting infection. In conclusion, against the current backdrop of the dominant D variant that could be further complicated by co-infection synergy with new variants, the growing list of viruses susceptible to TG, a promising host-centric antiviral, now includes a spectrum of contemporary SARS-CoV-2 viruses.
提供机构:
Gershkovich, Pavel; Mellits, Kenneth H.; Chang, Kin-Chow; Al-Beltagi, Sarah; Hayes, Christopher J.; Coleman, Christopher M.; Goulding, Leah V.; Chang, Daniel K.E.
创建时间:
2021-11-18
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