Th1 与 Th2 免疫偏倚对感染 SARS-CoV-2 变异株的人 ACE2 敲入小鼠病毒、病理和免疫动力学的影响。
Influence of Th1 versus Th2 immune bias on viral, pathological, and immunological dynamics in SARS-CoV-2 variant-infected human ACE2 knock-in mice.
机构信息
Center for Vaccine Innovation, La Jolla Institute for Immunology, La Jolla, CA, 92037, USA.
Synbal Inc., 1759 Yorktown Rd., San Mateo, CA, 94402, USA.
出版信息
EBioMedicine. 2024 Oct;108:105361. doi: 10.1016/j.ebiom.2024.105361. Epub 2024 Sep 30.
BACKGROUND
Mouse models that recapitulate key features of severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) infection are important tools for understanding complex interactions between host genetics, immune responses, and SARS-CoV-2 pathogenesis. Little is known about how predominantly cellular (Th1 type) versus humoral (Th2 type) immune responses influence SARS-CoV-2 dynamics, including infectivity and disease course.
METHODS
We generated knock-in (KI) mice expressing human ACE2 (hACE2) and/or human TMPRSS2 (hTMPRSS2) on Th1-biased (C57BL/6; B6) and Th2-biased (BALB/c) genetic backgrounds. Mice were infected intranasally with SARS-CoV-2 Delta (B.1.617.2) or Omicron BA.1 (B.1.1.529) variants, followed by assessment of disease course, respiratory tract infection, lung histopathology, and humoral and cellular immune responses.
FINDINGS
In both B6 and BALB/c mice, hACE2 expression was required for infection of the lungs with Delta, but not Omicron BA.1. Disease severity was greater in Omicron BA.1-infected hTMPRSS2-KI and double-KI BALB/c mice compared with B6 mice, and in Delta-infected double-KI B6 and BALB/c mice compared with hACE2-KI mice. hACE2-KI B6 mice developed more severe lung pathology and more robust SARS-CoV-2-specific splenic CD8 T cell responses compared with hACE2-KI BALB/c mice. There were no notable differences between the two genetic backgrounds in plasma cell, germinal center B cell, or antibody responses to SARS-CoV-2.
INTERPRETATION
SARS-CoV-2 Delta and Omicron BA.1 infection, disease course, and CD8 T cell response are influenced by the host genetic background. These humanized mice hold promise as important tools for investigating the mechanisms underlying the heterogeneity of SARS-CoV-2-induced pathogenesis and immune response.
FUNDING
This work was funded by NIH U19 AI142790-02S1, the GHR Foundation, the Arvin Gottleib Foundation, and the Overton family (to SS and EOS); Prebys Foundation (to SS); NIH R44 AI157900 (to KJ); and by an American Association of Immunologists Career Reentry Fellowship (FASB).
背景
能够重现严重急性呼吸综合征冠状病毒 2 型(SARS-CoV-2)感染关键特征的小鼠模型对于理解宿主遗传学、免疫反应和 SARS-CoV-2 发病机制之间的复杂相互作用非常重要。关于主要是细胞(Th1 型)与体液(Th2 型)免疫反应如何影响 SARS-CoV-2 的动态变化,包括传染性和疾病进程,人们知之甚少。
方法
我们构建了表达人血管紧张素转换酶 2(hACE2)和/或人 TMPRSS2(hTMPRSS2)的基因敲入(KI)小鼠,这些小鼠在 Th1 偏向(C57BL/6;B6)和 Th2 偏向(BALB/c)遗传背景下表达。用 SARS-CoV-2 Delta(B.1.617.2)或奥密克戎 BA.1(B.1.1.529)变异株经鼻腔感染小鼠,然后评估疾病进程、呼吸道感染、肺组织病理学、体液和细胞免疫反应。
发现
在 B6 和 BALB/c 小鼠中,hACE2 表达是肺部感染 Delta 的必要条件,但不是奥密克戎 BA.1 的必要条件。与 B6 小鼠相比,奥密克戎 BA.1 感染的 hTMPRSS2-KI 和双 KI BALB/c 小鼠,以及 Delta 感染的双 KI B6 和 BALB/c 小鼠中,疾病严重程度更高。与 hACE2-KI BALB/c 小鼠相比,hACE2-KI B6 小鼠的肺部病理更严重,SARS-CoV-2 特异性脾 CD8 T 细胞反应更强。在两种遗传背景下,浆细胞、生发中心 B 细胞或针对 SARS-CoV-2 的抗体反应没有明显差异。
解释
SARS-CoV-2 Delta 和奥密克戎 BA.1 的感染、疾病进程和 CD8 T 细胞反应受到宿主遗传背景的影响。这些人源化小鼠有望成为研究 SARS-CoV-2 诱导发病机制和免疫反应异质性的重要工具。
资金来源
本工作由 NIH U19 AI142790-02S1、GHR 基金会、Arvin Gottleib 基金会和 Overton 家族(资助 SS 和 EOS);Prebys 基金会(资助 SS);NIH R44 AI157900(资助 KJ);以及美国免疫学家协会职业重返奖学金(资助 FASB)。
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