Aligos Therapeutics, Inc., San Francisco, CA 94080, USA.
SAMDI Tech, Inc., Chicago, IL 60616, USA.
Molecules. 2022 May 3;27(9):2918. doi: 10.3390/molecules27092918.
Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is the cause of the COVID-19 pandemic. While the development of vaccines and the emergence of antiviral therapeutics is promising, alternative strategies to combat COVID-19 (and potential future pandemics) remain an unmet need. Coronaviruses feature a unique mechanism that may present opportunities for therapeutic intervention: the RNA polymerase complex of coronaviruses is distinct in its ability to proofread and remove mismatched nucleotides during genome replication and transcription. The proofreading activity has been linked to the exonuclease (ExoN) activity of non-structural protein 14 (NSP14). Here, we review the role of NSP14, and other NSPs, in SARS-CoV-2 replication and describe the assays that have been developed to assess the ExoN function. We also review the nucleoside analogs and non-nucleoside inhibitors known to interfere with the proofreading activity of NSP14. Although not yet validated, the potential use of non-nucleoside proofreading inhibitors in combination with chain-terminating nucleosides may be a promising avenue for the development of anti-CoV agents.
严重急性呼吸综合征冠状病毒 2 (SARS-CoV-2) 是 COVID-19 大流行的病因。虽然疫苗的开发和抗病毒疗法的出现前景广阔,但对抗 COVID-19(和潜在的未来大流行)的替代策略仍然是未满足的需求。冠状病毒具有独特的机制,这可能为治疗干预提供机会:冠状病毒的 RNA 聚合酶复合物在基因组复制和转录过程中具有独特的校对和去除错配核苷酸的能力。这种校对活性与非结构蛋白 14 (NSP14) 的外切酶 (ExoN) 活性有关。在这里,我们回顾了 NSP14 及其他 NSP 在 SARS-CoV-2 复制中的作用,并描述了已开发用于评估 ExoN 功能的测定方法。我们还回顾了已知干扰 NSP14 校对活性的核苷类似物和非核苷抑制剂。尽管尚未得到验证,但非核苷校对抑制剂与链终止核苷联合使用的潜在用途可能是开发抗 CoV 药物的一个有前途的途径。
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