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Med Hypotheses. 2020 Nov;144:110027. doi: 10.1016/j.mehy.2020.110027. Epub 2020 Jun 26.
There currently is no specific antiviral drug or a vaccine for SARS-CoV-2/COVID-19 infections; now exceeding 10,300,000 infections worldwide. In the absence of animal models to test drugs, we need to find molecular explanations for any unforeseen peculiarities in clinical data, especially the recent reports describing an unexpected asthma paradox. Asthma is considered a high medical risk factor for susceptibility to SARS-CoV-2/COVID-19 infection, yet asthma is not on the list of top 10 chronic health problems suffered by people who died from SARS-CoV-2/COVID-19. Resolving this paradox requires looking beyond the binary model of a viral receptor-binding domain (RBD) attaching to the ACE-2 receptor. A NCBI pBlast analysis revealed that the SARS-CoV-2 surface spike protein contains key two calcium-dependent fusion domains that are almost identical to those that were recently discovered SARS-CoV-1. These viral calcium-dependent binding domains can facilitate membrane fusion only after cleavage by the host surface protease TMPRSS2. Importantly, TMPRSS2 also requires calcium for its SRCR (scavenger receptor cysteine-rich) domain and itsLDLRA(LDL receptor class A) domain. Thus, the presence of EDTA excipients in nebulized β-agonist medicines can disrupt SARS-CoV-2/COVID-19 infection and can explain the asthma paradox. This model validates repurposing EDTA in nebulizer solutions from a passive excipient to an active drug for treating COVID-19 infections. Repurposed EDTA delivery to respiratory tissues at an initial target dose of 2.4 mg per aerosol treatment is readily achievable with standard nebulizer and mechanical ventilator equipment. EDTA warrants further investigation as a potential treatment for SARS-CoV-2/COVID-19 in consideration of the new calcium requirements for virus infection and the regular presence of EDTA excipients in common asthma medications such as Metaproterenol. Finally, the natural history of Coronavirus diseases and further analysis of the fusion loop homologies between the Betacorona SARS-CoV-2 virus and the less pathogenic Alphacorona HC0V-229E virus suggest how to engineer a hybrid virus suitable for an attenuated alpha-beta SARS-CoV-2/COVID-19 vaccine. Thus, replacing SARS-CoV-2 fusion loops (amino acids 816-855) with the less pathogenic HCoV-229E fusion loop (amino acids 923-982) may provide antigenicity of COVID-19, but limit the pathogenicity to the level of HCoV-229E.
目前尚无针对 SARS-CoV-2/COVID-19 感染的特效抗病毒药物或疫苗;目前全球感染人数已超过 1030 万。由于缺乏可用于药物测试的动物模型,我们需要从分子角度解释临床数据中出现的任何意外特征,尤其是最近有报告描述了一种出乎意料的哮喘悖论。哮喘被认为是易感染 SARS-CoV-2/COVID-19 的高医疗风险因素,但在因 SARS-CoV-2/COVID-19 而死亡的人群中所患的十大慢性健康问题中并未将哮喘列入其中。要解决这一悖论,就不能仅局限于病毒受体结合域(RBD)与 ACE-2 受体结合的二元模型。NCBI pBlast 分析显示,SARS-CoV-2 表面刺突蛋白含有两个关键的钙依赖性融合结构域,与最近发现的 SARS-CoV-1 几乎相同。这些病毒的钙依赖性结合结构域只有在宿主表面蛋白酶 TMPRSS2 切割后才能促进膜融合。重要的是,TMPRSS2 也需要钙离子才能激活其 SRCR(清道夫受体富含半胱氨酸)结构域和 LDLRA(LDL 受体 A 类)结构域。因此,在雾化β-激动剂药物中使用 EDTA 赋形剂可能会破坏 SARS-CoV-2/COVID-19 的感染,从而可以解释哮喘悖论。该模型验证了将 EDTA 从雾化器溶液中的赋形剂重新用于 COVID-19 感染的治疗,成为一种活性药物。通过标准雾化器和机械呼吸机设备,以初始目标剂量 2.4mg 对呼吸道组织进行 EDTA 输送是可以实现的。鉴于病毒感染对钙的新需求以及 Metaproterenol 等常见哮喘药物中普遍存在 EDTA 赋形剂,EDTA 值得进一步研究,以作为 SARS-CoV-2/COVID-19 的潜在治疗方法。最后,冠状病毒疾病的自然史以及对贝塔冠状病毒 SARS-CoV-2 病毒和致病性较低的阿尔法冠状病毒 HC0V-229E 病毒融合环同源性的进一步分析表明,如何构建一种适合减毒 SARS-CoV-2/COVID-19 疫苗的杂交病毒。因此,用致病性较低的 HCoV-229E 融合环(氨基酸 923-982)替换 SARS-CoV-2 融合环(氨基酸 816-855)可能提供 COVID-19 的抗原性,但将其致病性限制在 HCoV-229E 水平。
