Kollath Daniel R, Grill Francisca J, Itogawa Ashley N, Fabio-Braga Ana, Morales Matthew M, Shepardson Kelly M, Bryant Mitchell L, Yi Jinhee, Ramsey Marieke L, Luberto Emily T, Celona Kimberly R, Keim Paul S, Settles Erik W, Lake Douglas, Barker Bridget M
The Pathogen and Microbiome Institute, Northern Arizona University, Flagstaff, AZ, USA.
School of Life Sciences at Arizona State University, Tempe, AZ, USA.
Commun Med (Lond). 2024 Sep 30;4(1):186. doi: 10.1038/s43856-024-00610-y.
Early reports showed that patients with COVID-19 had recrudescence of previously resolved coccidioidomycosis (Valley fever, VF), and there were indications that coinfection had more severe outcomes. We therefore investigated serial infection of Coccidioides posadasii and SARS-CoV-2 in a K18-hACE2 mouse model to assess disease outcomes.
In our model, we challenged K18-hACE2 mice sequentially with a sub-lethal dose of SARS-CoV-2 and 24 hours later with low virulence strain of Coccidioides posadasii, and vice versa, compared to mice that only received a single infection challenge. We performed survival and pathogenesis mouse studies as well as looked at the systemic immune response differences between treatment groups.
Here we show that co-infected groups have a more severe disease progression as well as a decrease in survival. Importantly, results differ depending on the SARS-CoV-2 variant (WA-1, Delta, or Omicron) and infection timing (SARS-CoV-2 first, C. posadasii second or vice versa). We find that groups that are infected with the virus first had a decrease in survival, increased morbidity and weight loss, increased fungal and viral burdens, differences in immune responses, and the amount and size of fungal spherules. We also find that groups coinfected with C. posadasii first have a decrease fungal burden and inflammatory responses.
This is the first in vivo model investigation of a coinfection of SARS-CoV-2 and Coccidioides. Because of the potential for increased severity of disease in a coinfection, we suggest populations that live in areas of high coccidioidomycosis endemicity may experience higher incidence of complicated disease progression with COVID-19.
早期报告显示,2019冠状病毒病(COVID-19)患者先前已治愈的球孢子菌病(山谷热,VF)出现复发,且有迹象表明合并感染会导致更严重的后果。因此,我们在K18-hACE2小鼠模型中研究了波萨达斯球孢子菌和严重急性呼吸综合征冠状病毒2(SARS-CoV-2)的连续感染情况,以评估疾病结局。
在我们的模型中,我们先用亚致死剂量的SARS-CoV-2对K18-hACE2小鼠进行攻击,24小时后再用低毒力的波萨达斯球孢子菌菌株进行攻击,反之亦然,并与仅接受单次感染攻击的小鼠进行比较。我们进行了小鼠生存和发病机制研究,并观察了治疗组之间的全身免疫反应差异。
我们发现,合并感染组的疾病进展更严重,生存率降低。重要的是,结果因SARS-CoV-2变体(WA-1、德尔塔或奥密克戎)和感染时间(先感染SARS-CoV-2,后感染波萨达斯球孢子菌或反之)而异。我们发现,先感染病毒的组生存率降低、发病率和体重减轻增加、真菌和病毒载量增加、免疫反应存在差异,以及真菌球的数量和大小存在差异。我们还发现,先感染波萨达斯球孢子菌的合并感染组真菌载量和炎症反应降低。
这是首次对SARS-CoV-2和球孢子菌合并感染进行的体内模型研究。由于合并感染可能会增加疾病的严重程度,我们建议生活在球孢子菌病高流行地区的人群感染COVID-19后可能会出现更高的复杂疾病进展发生率。
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