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. 2024 Jan 1;79(1):167-182.
doi: 10.1097/HEP.0000000000000524. Epub 2023 Jun 27.

Single-cell RNA sequencing reveals the immunoregulatory roles of PegIFN-α in patients with chronic hepatitis B

Penglei Jiang  1   2   3 Hongyu Jia  4 Xinyue Qian  1   2   3 Tian Tang  1   2   3 Yingli Han  1   2   3 Zhaoru Zhang  1   2   3 Lingli Jiang  1   2   3 Zebin Yu  1   2   3 Lin Zheng  4 Guodong Yu  4 Huan Cai  4 Shanyan Zhang  4 Xiaoli Zhang  4 Jueqing Gu  4 Chanyuan Ye  4 Lisha Yang  4 Yingfeng Lu  4 Heng Liu  4 Xiaoqing Lu  4 Ciliang Jin  4 Yue Ren  5 Miaomiao Lu  5 Lingling Xu  5   6 Jiong Yu  4 Xi Jin  5 Yida Yang  4 Pengxu Qian  1   2   3
Affiliations

Single-cell RNA sequencing reveals the immunoregulatory roles of PegIFN-α in patients with chronic hepatitis B

Penglei Jiang et al. Hepatology. .

Abstract

Background and aims: Chronic hepatitis B (CHB) is caused by HBV infection and affects the lives of millions of people worldwide by causing liver inflammation, cirrhosis, and liver cancer. Interferon-alpha (IFN-α) therapy is a conventional immunotherapy that has been widely used in CHB treatment and achieved promising therapeutic outcomes by activating viral sensors and interferon-stimulated genes (ISGs) suppressed by HBV. However, the longitudinal landscape of immune cells of CHB patients and the effect of IFN-α on the immune system are not fully understood.

Approach and results: Here, we applied single-cell RNA sequencing (scRNA-seq) to delineate the transcriptomic landscape of peripheral immune cells in CHB patients before and after PegIFN-α therapy. Notably, we identified three CHB-specific cell subsets, pro-inflammatory (Pro-infla) CD14+ monocytes, Pro-infla CD16+ monocytes and IFNG+ CX3CR1- NK cells, which highly expressed proinflammatory genes and positively correlated with HBsAg. Furthermore, PegIFN-α treatment attenuated percentages of hyperactivated monocytes, increased ratios of long-lived naive/memory T cells and enhanced effector T cell cytotoxicity. Finally, PegIFN-α treatment switched the transcriptional profiles of entire immune cells from TNF-driven to IFN-α-driven pattern and enhanced innate antiviral response, including virus sensing and antigen presentation.

Conclusions: Collectively, our study expands the understanding of the pathological characteristics of CHB and the immunoregulatory roles of PegIFN-α, which provides a new powerful reference for the clinical diagnosis and treatment of CHB.

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