Department of Laboratory Medicine, Unit of Clinical Microbiology, Karolinska Institute, Stockholm, Sweden.
Acus Laboratories GmbH, Cologne, Germany.
EMBO Mol Med. 2021 Jan 11;13(1):e13426. doi: 10.15252/emmm.202013426. Epub 2020 Dec 14.
There is a critical need for safe and effective drugs for COVID-19. Only remdesivir has received authorization for COVID-19 and has been shown to improve outcomes but not decrease mortality. However, the dose of remdesivir is limited by hepatic and kidney toxicity. ACE2 is the critical cell surface receptor for SARS-CoV-2. Here, we investigated additive effect of combination therapy using remdesivir with recombinant soluble ACE2 (high/low dose) on Vero E6 and kidney organoids, targeting two different modalities of SARS-CoV-2 life cycle: cell entry via its receptor ACE2 and intracellular viral RNA replication. This combination treatment markedly improved their therapeutic windows against SARS-CoV-2 in both models. By using single amino-acid resolution screening in haploid ES cells, we report a singular critical pathway required for remdesivir toxicity, namely, Adenylate Kinase 2. The data provided here demonstrate that combining two therapeutic modalities with different targets, common strategy in HIV treatment, exhibit strong additive effects at sub-toxic concentrations. Our data lay the groundwork for the study of combinatorial regimens in future COVID-19 clinical trials.
目前迫切需要安全有效的 COVID-19 治疗药物。瑞德西韦是唯一获得 COVID-19 授权的药物,已被证明可改善预后,但不能降低死亡率。然而,瑞德西韦的剂量受到肝毒性和肾毒性的限制。ACE2 是 SARS-CoV-2 的关键细胞表面受体。在这里,我们研究了使用瑞德西韦联合重组可溶性 ACE2(高/低剂量)治疗对 Vero E6 和肾类器官的附加效果,针对 SARS-CoV-2 生命周期的两种不同方式:通过其受体 ACE2 进入细胞和细胞内病毒 RNA 复制。这种联合治疗在两种模型中均显著提高了对 SARS-CoV-2 的治疗窗口。通过在单倍体 ES 细胞中进行单个氨基酸分辨率筛选,我们报告了一个单一的关键途径,即腺苷酸激酶 2,这是瑞德西韦毒性所必需的。这里提供的数据表明,联合使用两种针对不同靶点的治疗方式(这是 HIV 治疗中的常见策略)在亚毒性浓度下具有很强的附加效果。我们的数据为未来 COVID-19 临床试验中组合方案的研究奠定了基础。
