Department of Nuclear Medicine, Shanghai Changhai Hospital, Shanghai, China.
School of Medicine, Shanghai University, Shanghai, China.
J Med Virol. 2022 Oct;94(10):4878-4889. doi: 10.1002/jmv.27958. Epub 2022 Jul 5.
A transocular infection has been proved as one of the main approaches that severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) invades the body, and angiotensin-converting enzyme 2 (ACE2) plays a key role in this procedure. Dynamic and quantitative details on virus distribution are lacking for virus prevention and drug design. In this study, a radiotraceable pseudovirus packed with an enhanced green fluorescent protein (EGFP) gene, I-CoV, was prepared and inoculated in the unilateral eye of humanized ACE2 (hACE2) mice or ACE2-knockout (ACE2-KO) mice. Single-photon emission computed tomography/computed tomography images were acquired at multiple time points to exhibit ACE2-dependent procedures from invasion to clearance. Positron emission tomography (PET) and western blot were performed to quantify ACE2 expression and verify the factors affecting transocular infection. For the transocular infection of coronavirus (CoV), the renin-angiotensin-aldosterone system (RAAS), lungs, intestines, and genital glands were the main targeted organs. Due to the specific anchor to ACE2-expressed host cells, virus concentrations in genital glands, liver, and lungs ranked the top three most and stabilized at 3.75 ± 0.55, 3.30 ± 0.25, and 2.10 ± 0.55% inoculated dose (ID)/mL at 48 h post treatment. Meanwhile, ACE2-KO mice had already completed the in vivo clearance. In consideration of organ volumes, lungs (14.50 ± 3.75%ID) and liver (10.94 ± 0.71%ID) were the main in-store reservoirs of CoV. However, the inoculated eye (5.52 ± 1.85%ID for hACE2, 5.24 ± 1.45%ID for ACE2-KO, p > 0.05) and the adjacent brain exhibited ACE2-independent virus infection at the end of 72 h observation, and absolute amount of virus played a key role in host cell infection. These observations on CoV infection were further manifested by infection-driven intracellular EGFP expression. ACE2 PET revealed an infection-related systematic upregulation of ACE2 expression in the organs involved in RAAS (e.g., brain, lung, heart, liver, and kidney) and the organ that was of own local renin-angiotensin system (e.g., eye). Transocular infection of CoV is ACE2-dependent and constitutes the cause of disturbed ACE2 expression in the host. The brain, genital glands, and intestines were of the highest unit uptake, potentially accounting for the sequelae. Lungs and liver were of the highest absolute amount, closely related to the respiratory diffusion and in vivo duplication. ACE2 expression was upregulated in the short term after infection with CoV. These visual and quantitative results are helpful to fully understanding the transocular path of SARS-CoV-2 and other CoVs.
眼内感染已被证实是严重急性呼吸综合征冠状病毒 2(SARS-CoV-2)入侵人体的主要途径之一,血管紧张素转换酶 2(ACE2)在此过程中起着关键作用。目前缺乏有关病毒分布的动态和定量细节,这对病毒预防和药物设计至关重要。在这项研究中,我们制备了一种携带增强型绿色荧光蛋白(EGFP)基因的放射性示踪假病毒 I-CoV,并将其接种到人源化 ACE2(hACE2)小鼠或 ACE2 敲除(ACE2-KO)小鼠的单侧眼睛中。在多个时间点采集单光子发射计算机断层扫描/计算机断层扫描图像,以展示从入侵到清除的 ACE2 依赖性过程。进行正电子发射断层扫描(PET)和蛋白质印迹以定量 ACE2 表达并验证影响眼内感染的因素。对于冠状病毒(CoV)的眼内感染,肾素-血管紧张素-醛固酮系统(RAAS)、肺部、肠道和生殖腺是主要的靶向器官。由于对 ACE2 表达的宿主细胞具有特异性锚定,生殖腺、肝脏和肺部中的病毒浓度排名前三,分别稳定在接种剂量(ID)/mL 的 3.75±0.55%、3.30±0.25%和 2.10±0.55%,在治疗后 48 小时。同时,ACE2-KO 小鼠已经完成了体内清除。考虑到器官体积,肺(14.50±3.75%ID)和肝(10.94±0.71%ID)是 CoV 的主要储存库。然而,接种眼(hACE2 为 5.52±1.85%ID,ACE2-KO 为 5.24±1.45%ID,p>0.05)和相邻大脑在 72 小时观察结束时表现出 ACE2 非依赖性病毒感染,病毒的绝对数量在宿主细胞感染中起着关键作用。CoV 感染的这些观察结果进一步通过感染驱动的细胞内 EGFP 表达得到证实。ACE2 PET 显示,与 RAAS 相关的器官(如大脑、肺、心脏、肝脏和肾脏)和自身局部肾素-血管紧张素系统(如眼睛)中 ACE2 表达的系统上调与感染有关。CoV 的眼内感染是 ACE2 依赖性的,构成了宿主中 ACE2 表达紊乱的原因。大脑、生殖腺和肠道的单位摄取率最高,可能是导致后遗症的原因。肺和肝脏的绝对数量最高,与呼吸扩散和体内复制密切相关。感染 CoV 后 ACE2 的表达在短期内上调。这些直观和定量的结果有助于全面了解 SARS-CoV-2 和其他 CoV 的眼内途径。
