di Bari I, Franzin R, Picerno A, Stasi A, Cimmarusti M T, Di Chiano M, Curci C, Pontrelli P, Chironna M, Castellano G, Gallone A, Sabbà C, Gesualdo L, Sallustio F
Department of Emergency and Organ Transplantation, University of Bari 'Aldo Moro', Bari, Italy.
Department of Basic Medical Sciences, Neuroscience and Sense Organs, University of Bari 'Aldo Moro', Bari, Italy.
New Microbes New Infect. 2021 May;41:100853. doi: 10.1016/j.nmni.2021.100853. Epub 2021 Feb 27.
The pandemic of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) causing coronavirus disease 2019 (COVID-19), resulting in acute respiratory disease, is a worldwide emergency. Because recently it has been found that SARS-CoV is dependent on host transcription factors (TF) to express the viral genes, efforts are required to understand the molecular interplay between virus and host response. By bioinformatic analysis, we investigated human TF that can bind the SARS-CoV-2 sequence and can be involved in viral transcription. In particular, we analysed the key role of TF involved in interferon (IFN) response. We found that several TF could be induced by the IFN antiviral response, specifically some induced by IFN-stimulated gene factor 3 (ISGF3) and by unphosphorylated ISGF3, which were found to promote the transcription of several viral open reading frame. Moreover, we found 22 TF binding sites present only in the sequence of virus infecting humans but not bat coronavirus RaTG13. The 22 TF are involved in IFN, retinoic acid signalling and regulation of transcription by RNA polymerase II, thus facilitating its own replication cycle. This mechanism, by competition, may steal the human TF involved in these processes, explaining SARS-CoV-2's disruption of IFN-I signalling in host cells and the mechanism of the SARS retinoic acid depletion syndrome leading to the cytokine storm. We identified three TF binding sites present exclusively in the Brazilian SARS-CoV-2 P.1 variant that may explain the higher severity of the respiratory syndrome. These data shed light on SARS-CoV-2 dependence from the host transcription machinery associated with IFN response and strengthen our knowledge of the virus's transcription and replicative activity, thus paving the way for new targets for drug design and therapeutic approaches.
导致2019冠状病毒病(COVID-19)的严重急性呼吸综合征冠状病毒2(SARS-CoV-2)大流行引发急性呼吸道疾病,是一场全球紧急事件。由于最近发现SARS-CoV依赖宿主转录因子(TF)来表达病毒基因,因此需要努力了解病毒与宿主反应之间的分子相互作用。通过生物信息学分析,我们研究了能够结合SARS-CoV-2序列并参与病毒转录的人类TF。特别是,我们分析了参与干扰素(IFN)反应的TF的关键作用。我们发现几种TF可由IFN抗病毒反应诱导,特别是一些由IFN刺激基因因子3(ISGF3)和未磷酸化的ISGF3诱导,它们被发现可促进几种病毒开放阅读框的转录。此外,我们发现22个TF结合位点仅存在于感染人类的病毒序列中,而不存在于蝙蝠冠状病毒RaTG13中。这22个TF参与IFN、视黄酸信号传导以及RNA聚合酶II的转录调控,从而促进其自身的复制周期。这种通过竞争的机制可能会抢夺参与这些过程的人类TF,解释了SARS-CoV-2对宿主细胞中IFN-I信号传导的破坏以及导致细胞因子风暴的SARS视黄酸耗竭综合征的机制。我们确定了仅存在于巴西SARS-CoV-2 P.1变体中的三个TF结合位点,这可能解释了呼吸道综合征更高的严重程度。这些数据揭示了SARS-CoV-2对与IFN反应相关的宿主转录机制的依赖性,并加强了我们对该病毒转录和复制活性的认识,从而为药物设计和治疗方法的新靶点铺平了道路。
