Single-cell landscape of functionally cured chronic hepatitis B patients reveals activation of innate and altered CD4-CTL-driven adaptive immunity

Balakrishnan Chakrapani Narmada; Atefeh Khakpoor; Niranjan Shirgaonkar; Sriram Narayanan; Pauline Poh Kim Aw; Malay Singh; Kok Haur Ong; Collins Oduor Owino; Jane Wei Ting Ng; Hui Chuing Yew; Nu Soibah Binte Mohamed Nasir; Veonice Bijin Au; Reina Sng; Nivashini Kaliaperumal; Htet Htet Toe Wai Khine; Francesca Casuscelli di Tocco; Otsuka Masayuki; Shamita Naikar; Hui Xin Ng; Su Li Chia; Cindy Xin Yi Seah; Myra Hj Alnawaz; Chris Lee Yoon Wai; Amy Yuh Ling Tay; Kamarjit Singh Mangat; Valerie Chew; Weimiao Yu; John Edward Connolly; Giridharan Periyasamy; Marie-Laure Plissonnier; Massimo Levrero; Seng Gee Lim; Ramanuj DasGupta

doi:10.1016/j.jhep.2024.02.017

Single-cell landscape of functionally cured chronic hepatitis B patients reveals activation of innate and altered CD4-CTL-driven adaptive immunity

J Hepatol. 2024 Feb 28:S0168-8278(24)00137-5. doi: 10.1016/j.jhep.2024.02.017. Online ahead of print.

Authors

Balakrishnan Chakrapani Narmada¹, Atefeh Khakpoor², Niranjan Shirgaonkar³, Sriram Narayanan⁴, Pauline Poh Kim Aw³, Malay Singh⁵, Kok Haur Ong⁵, Collins Oduor Owino⁶, Jane Wei Ting Ng², Hui Chuing Yew², Nu Soibah Binte Mohamed Nasir², Veonice Bijin Au⁴, Reina Sng⁴, Nivashini Kaliaperumal⁴, Htet Htet Toe Wai Khine², Francesca Casuscelli di Tocco⁷, Otsuka Masayuki⁸, Shamita Naikar⁸, Hui Xin Ng², Su Li Chia², Cindy Xin Yi Seah⁹, Myra Hj Alnawaz⁹, Chris Lee Yoon Wai², Amy Yuh Ling Tay², Kamarjit Singh Mangat², Valerie Chew⁸, Weimiao Yu¹⁰, John Edward Connolly¹¹, Giridharan Periyasamy¹², Marie-Laure Plissonnier⁷, Massimo Levrero¹³, Seng Gee Lim¹⁴, Ramanuj DasGupta¹⁵

Affiliations

¹ Laboratory of Precision Medicine and Cancer Evolution, Genome Institute of Singapore, Agency for Science, Technology and Research (A∗STAR), 60 Biopolis St., #02-01 Genome, Singapore 138672; Experimental Drug Development Centre, A∗STAR, 10 Biopolis Way, Chromos, Singapore 138670, Singapore.
² Department of Medicine, Yong Loo Lin School of Medicine, National University of Singapore, Singapore.
³ Laboratory of Precision Medicine and Cancer Evolution, Genome Institute of Singapore, Agency for Science, Technology and Research (A∗STAR), 60 Biopolis St., #02-01 Genome, Singapore 138672.
⁴ Institute of Molecular and Cell Biology, A∗STAR, 61 Biopolis Drive, Proteos, Singapore, 138673, Singapore.
⁵ Bioinformatics Institute, A∗STAR, 30 Biopolis Street, Matrix, Singapore 138671, Singapore.
⁶ Laboratory of Precision Medicine and Cancer Evolution, Genome Institute of Singapore, Agency for Science, Technology and Research (A∗STAR), 60 Biopolis St., #02-01 Genome, Singapore 138672; Department of Microbiology and Immunology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore.
⁷ Cancer Research Center of Lyon (CRCL), INSERM U1052, CNRS UMR5286, Lyon, France.
⁸ Translational Immunology Institute (TII), SingHealth-DukeNUS Academic Medical Centre, Singapore 169856, Singapore.
⁹ Department of Medicine, National University Hospital, Singapore.
¹⁰ Institute of Molecular and Cell Biology, A∗STAR, 61 Biopolis Drive, Proteos, Singapore, 138673, Singapore; Bioinformatics Institute, A∗STAR, 30 Biopolis Street, Matrix, Singapore 138671, Singapore.
¹¹ Institute of Molecular and Cell Biology, A∗STAR, 61 Biopolis Drive, Proteos, Singapore, 138673, Singapore; Department of Microbiology and Immunology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore; Institute of Biomedical Studies, Baylor University, Waco, TX, USA; Parker Institute for Cancer Immunotherapy, San Francisco, CA, USA.
¹² Experimental Drug Development Centre, A∗STAR, 10 Biopolis Way, Chromos, Singapore 138670, Singapore.
¹³ Cancer Research Center of Lyon (CRCL), INSERM U1052, CNRS UMR5286, Lyon, France; Department of Hepatology, Hôpital Croix-Rousse, Hospices Civils de Lyon, Lyon, France; University of Lyon Claude Bernard 1 (UCLB1), Lyon, France; Department of Medicine SCIAC and the Italian Institute of Technology (IIT) Center for Life Nanosciences (CLNS), University of Rome La Sapienza, Rome, Italy.
¹⁴ Institute of Molecular and Cell Biology, A∗STAR, 61 Biopolis Drive, Proteos, Singapore, 138673, Singapore; Department of Medicine, National University Hospital, Singapore; Division of Gastroenterology and Hepatology, National University Hospital, National University Health System, Singapore. Electronic address: mdclimsg@nus.edu.sg.
¹⁵ Laboratory of Precision Medicine and Cancer Evolution, Genome Institute of Singapore, Agency for Science, Technology and Research (A∗STAR), 60 Biopolis St., #02-01 Genome, Singapore 138672. Electronic address: dasguptar@gis.a-star.edu.sg.

PMID: 38423478
DOI: 10.1016/j.jhep.2024.02.017

Abstract

Background & aims: Hepatitis B surface antigen (HBsAg) loss or functional cure (FC) is considered the optimal therapeutic outcome for patients with chronic hepatitis B (CHB). However, the immune-pathological biomarkers and underlying mechanisms of FC remain unclear. In this study we comprehensively interrogate disease-associated cell states identified within intrahepatic tissue and matched PBMCs from patients with CHB or after FC, at the resolution of single cells, to provide novel insights into putative mechanisms underlying FC.

Methods: We combined single-cell transcriptomics (single-cell RNA sequencing) with multiparametric flow cytometry-based immune phenotyping, and multiplexed immunofluorescence to elucidate the immunopathological cell states associated with CHB vs. FC.

Results: We found that the intrahepatic environment in CHB and FC displays specific cell identities and molecular signatures that are distinct from those found in matched PBMCs. FC is associated with the emergence of an altered adaptive immune response marked by CD4 cytotoxic T lymphocytes, and an activated innate response represented by liver-resident natural killer cells, specific Kupffer cell subtypes and marginated neutrophils. Surprisingly, we found MHC class II-expressing hepatocytes in patients achieving FC, as well as low but persistent levels of covalently closed circular DNA and pregenomic RNA, which may play an important role in FC.

Conclusions: Our study provides conceptually novel insights into the immuno-pathological control of HBV cure, and opens exciting new avenues for clinical management, biomarker discovery and therapeutic development. We believe that the discoveries from this study, as it relates to the activation of an innate and altered immune response that may facilitate sustained, low-grade inflammation, may have broader implications in the resolution of chronic viral hepatitis.

Impact and implications: This study dissects the immuno-pathological cell states associated with functionally cured chronic hepatitis B (defined by the loss of HBV surface antigen or HBsAg). We identified the sustained presence of very low viral load, accessory antigen-presenting hepatocytes, adaptive-memory-like natural killer cells, and the emergence of helper CD4 T cells with cytotoxic or effector-like signatures associated with functional cure, suggesting previously unsuspected alterations in the adaptive immune response, as well as a key role for the innate immune response in achieving or maintaining functional cure. Overall, the insights generated from this study may provide new avenues for the development of alternative therapies as well as patient surveillance for better clinical management of chronic hepatitis B.

Keywords: CD4-CTL; HBV; HBsAg; accessory APC; immune; liver; neutrophils; single cell RNA-seq; viral hepatitis.