IFNγ initiates TLR9-dependent autoimmune hepatitis in DNase II deficient mice

bioRxiv Pub Date : 2024-07-16 DOI:10.1101/2024.07.10.602775
Kaiyuan Hao, K. M. Gao, Melissa Strauss, Sharon Subramanian, Ann Marshak-Rothstein
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Abstract

Patients with biallelic hypomorphic mutation in DNASE2 develop systemic autoinflammation and early-onset liver fibrosis. Prior studies showed that Dnase2-/- Ifnar-/- double knockout (DKO) mice develop Type I IFN-independent liver inflammation, but immune mechanisms were unclear. We now show that DKO mice recapitulate many features of human autoimmune hepatitis (AIH), including periportal and interstitial inflammation and fibrosis and elevated ALT. Infiltrating cells include CD8+ tissue resident memory T cells, type I innate lymphoid cells, and inflammatory monocyte/macrophage cells that replace the Kupffer cell pool. Importantly, TLR9 expression by bone marrow-derived cells is required for the the development of AIH. TLR9 is highly expressed by inflammatory myeloid cells but not long-lived Kupffer cells. Furthermore, the initial recruitment of TLR9 expressing monocytes and subsequent activation of lymphocytes requires IFNγ signaling. These findings highlight a critical role of feed forward loop between TLR9 expressing monocyte-lineage cells and IFNg producing lymphocytes in autoimmune hepatitis.
IFNγ 在 DNase II 缺乏的小鼠体内引发 TLR9 依赖性自身免疫性肝炎
DNASE2双倍体低位突变患者会出现全身性自身炎症和早发性肝纤维化。之前的研究表明,Dnase2-/- Ifnar-/- 双基因敲除(DKO)小鼠会出现 I 型 IFN 依赖性肝脏炎症,但免疫机制尚不清楚。我们现在发现,DKO 小鼠再现了人类自身免疫性肝炎(AIH)的许多特征,包括门脉周围和间质炎症、纤维化和谷丙转氨酶升高。浸润细胞包括 CD8+ 组织常驻记忆 T 细胞、I 型先天性淋巴细胞和取代 Kupffer 细胞池的炎性单核细胞/巨噬细胞。重要的是,骨髓衍生细胞表达 TLR9 是 AIH 发病的必要条件。炎性髓系细胞高度表达 TLR9,但长效 Kupffer 细胞不表达 TLR9。此外,表达 TLR9 的单核细胞的初始招募和随后的淋巴细胞活化需要 IFNγ 信号。这些发现凸显了表达 TLR9 的单核细胞系细胞和产生 IFNg 的淋巴细胞之间的前馈循环在自身免疫性肝炎中的关键作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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