Department of Metabolic Medicine, Graduate School of Medicine, Osaka University, Suita, Osaka, Japan; Department of Diabetes Care Medicine, Graduate School of Medicine, Osaka University, Suita, Osaka, Japan.
Department of Metabolic Medicine, Graduate School of Medicine, Osaka University, Suita, Osaka, Japan.
Metabolism. 2022 Aug;133:155236. doi: 10.1016/j.metabol.2022.155236. Epub 2022 Jun 8.
COVID-19 can cause multiple organ damages as well as metabolic abnormalities such as hyperglycemia, insulin resistance, and new onset of diabetes. The insulin/IGF signaling pathway plays an important role in regulating energy metabolism and cell survival, but little is known about the impact of SARS-CoV-2 infection. The aim of this work was to investigate whether SARS-CoV-2 infection impairs the insulin/IGF signaling pathway in the host cell/tissue, and if so, the potential mechanism and association with COVID-19 pathology.
To determine the impact of SARS-CoV-2 on insulin/IGF signaling pathway, we utilized transcriptome datasets of SARS-CoV-2 infected cells and tissues from public repositories for a wide range of high-throughput gene expression data: autopsy lungs from COVID-19 patients compared to the control from non-COVID-19 patients; lungs from a human ACE2 transgenic mouse infected with SARS-CoV-2 compared to the control infected with mock; human pluripotent stem cell (hPSC)-derived liver organoids infected with SARS-CoV-2; adipose tissues from a mouse model of COVID-19 overexpressing human ACE2 via adeno-associated virus serotype 9 (AAV9) compared to the control GFP after SARS-CoV-2 infection; iPS-derived human pancreatic cells infected with SARS-CoV-2 compared to the mock control. Gain and loss of IRF1 function models were established in HEK293T and/or Calu3 cells to evaluate the impact on insulin signaling. To understand the mechanistic regulation and relevance with COVID-19 risk factors, such as older age, male sex, obesity, and diabetes, several transcriptomes of human respiratory, metabolic, and endocrine cells and tissue were analyzed. To estimate the association with COVID-19 severity, whole blood transcriptomes of critical patients with COVID-19 compared to those of hospitalized noncritical patients with COVID-19.
We found that SARS-CoV-2 infection impaired insulin/IGF signaling pathway genes, such as IRS, PI3K, AKT, mTOR, and MAPK, in the host lung, liver, adipose tissue, and pancreatic cells. The impairments were attributed to interferon regulatory factor 1 (IRF1), and its gene expression was highly relevant to risk factors for severe COVID-19; increased with aging in the lung, specifically in men; augmented by obese and diabetic conditions in liver, adipose tissue, and pancreatic islets. IRF1 activation was significantly associated with the impaired insulin signaling in human cells. IRF1 intron variant rs17622656-A, which was previously reported to be associated with COVID-19 prevalence, increased the IRF1 gene expression in human tissue and was frequently found in American and European population. Critical patients with COVID-19 exhibited higher IRF1 and lower insulin/IGF signaling pathway genes in the whole blood compared to hospitalized noncritical patients. Hormonal interventions, such as dihydrotestosterone and dexamethasone, ameliorated the pathological traits in SARS-CoV-2 infectable cells and tissues.
The present study provides the first scientific evidence that SARS-CoV-2 infection impairs the insulin/IGF signaling pathway in respiratory, metabolic, and endocrine cells and tissues. This feature likely contributes to COVID-19 severity with cell/tissue damage and metabolic abnormalities, which may be exacerbated in older, male, obese, or diabetic patients.
COVID-19 可导致多种器官损伤以及代谢异常,如高血糖、胰岛素抵抗和新发糖尿病。胰岛素/IGF 信号通路在调节能量代谢和细胞存活方面起着重要作用,但关于 SARS-CoV-2 感染的影响知之甚少。本研究旨在探讨 SARS-CoV-2 感染是否会损害宿主细胞/组织中的胰岛素/IGF 信号通路,如果是,其潜在机制以及与 COVID-19 病理学的关联。
为了确定 SARS-CoV-2 对胰岛素/IGF 信号通路的影响,我们利用了公共存储库中 SARS-CoV-2 感染细胞和组织的转录组数据集,这些数据集涵盖了广泛的高通量基因表达数据:与非 COVID-19 患者的对照相比,COVID-19 患者的尸检肺;与模拟感染的对照相比,感染 SARS-CoV-2 的人类 ACE2 转基因小鼠的肺;与模拟感染的对照相比,感染 SARS-CoV-2 的人多能干细胞(hPSC)衍生的肝类器官;与 SARS-CoV-2 感染后的对照 GFP 相比,通过腺相关病毒血清型 9(AAV9)过表达人 ACE2 的 COVID-19 小鼠模型的脂肪组织;与模拟感染的对照相比,感染 SARS-CoV-2 的 iPS 衍生的人胰腺细胞。在 HEK293T 和/或 Calu3 细胞中建立了 IRF1 功能获得和丧失模型,以评估其对胰岛素信号的影响。为了了解与 COVID-19 风险因素(如年龄较大、男性、肥胖和糖尿病)的机制调节和相关性,分析了人类呼吸、代谢和内分泌细胞和组织的多个转录组。为了评估与 COVID-19 严重程度的关联,将 COVID-19 重症患者的全血转录组与住院非重症 COVID-19 患者的全血转录组进行了比较。
我们发现,SARS-CoV-2 感染会损害宿主肺、肝、脂肪组织和胰腺细胞中的胰岛素/IGF 信号通路基因,如 IRS、PI3K、AKT、mTOR 和 MAPK。这种损伤归因于干扰素调节因子 1(IRF1),其基因表达与 COVID-19 严重程度的风险因素高度相关;在肺部,特别是在男性中,随着年龄的增长而增加;在肥胖和糖尿病患者的肝脏、脂肪组织和胰腺胰岛中增加。IRF1 激活与人类细胞中胰岛素信号的受损显著相关。先前报道与 COVID-19 患病率相关的 IRF1 内含子变体 rs17622656-A 增加了人组织中的 IRF1 基因表达,并且在美洲和欧洲人群中经常发现。与住院非重症 COVID-19 患者相比,COVID-19 重症患者的全血中 IRF1 和胰岛素/IGF 信号通路基因表达水平更高。激素干预,如二氢睾酮和地塞米松,可改善 SARS-CoV-2 感染细胞和组织的病理特征。
本研究首次提供了科学证据,表明 SARS-CoV-2 感染可损害呼吸、代谢和内分泌细胞和组织中的胰岛素/IGF 信号通路。这一特征可能导致 COVID-19 严重程度与细胞/组织损伤和代谢异常有关,在年龄较大、男性、肥胖或糖尿病患者中可能更为严重。
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