TY - JOUR
T1 - Circulating capsid-antibody-complexes (CACs) drive intrahepatic complement deposition and inform subclinical liver inflammation in chronic hepatitis B
AU - Tang, Yijie
AU - Xu, Mingzhu
AU - Wang, Cong
AU - Wu, Min
AU - Hu, Lyuyin
AU - Li, Jin
AU - Lu, Wei
AU - Zheng, Ye
AU - Zhang, Min
AU - Jiang, Xizi
AU - Zhu, Chuanwu
AU - Audsley, Jennifer
AU - Tangkijvanich, Pisit
AU - Avihingsanon, Anchalee
AU - Song, Shu
AU - Liu, Shuangzhe
AU - Lewin, Sharon R.
AU - George, Jacob
AU - Douglas, Mark
AU - Ling, Yun
AU - Yuan, Zhenghong
AU - Zhu, Li
AU - Zhang, Zhanqing
AU - Zhang, Xiaonan
N1 - Funding Information:
This work is supported by the Australian Centre for HIV and Hepatitis Virology Research (XZ), Chinese National Natural Science Foundation grant 32070152 (XZ), The Social Development Program of Jiangsu Province, China, BE2022734 (LZ), The Science and Technology Project of Suzhou, SKY2022061(LZ), Science and Technology Project of Suzhou Municipal Health Commission, LCZX202117 (LZ), Robert W. Storr Bequest to the Sydney Medical Foundation (JG), National Health and Medical Research Council of Australia (NHMRC) Program Grant APP1053206, APP2001692, APP1107178, APP1108422, APP1196492 (JG), APP2002565, APP2021586 (MD), APP1149990, APP1135851, APP2026490 (SRL), Cancer Institute, NSW grant, ATRG2028 (JG).The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Xiaonan Zhang reports financial support was provided by Chinese National Natural Science Foundation. Xiaonan Zhang reports financial support was provided by Australian Centre for HIV and Hepatitis Virology Research. Jacob George reports a relationship with Novo from Nordisk, Astra Zeneca, Roche, BMS, Pfizer, Cincera, Pharmaxis, Boehringer Mannheim that includes: speaking and lecture fees. Mark Douglas reports a relationship with Gilead, Glaxo-Smith-Kline, Abbvie, BMS, Roche. That includes: speaking and lecture fees. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.
Funding Information:
This work is supported by the Australian Centre for HIV and Hepatitis Virology Research (XZ), Chinese National Natural Science Foundation grant 32070152 (ZX), The Social Development Program of Jiangsu Province, China, BE2022734 (LZ), The Science and Technology Project of Suzhou, SKY2022061(LZ), Science and Technology Project of Suzhou Municipal Health Commission, LCZX202117 (LZ), Robert W. Storr Bequest to the Sydney Medical Foundation (JG), National Health and Medical Research Council of Australia (NHMRC) Program Grant APP1053206, APP2001692, APP1107178, APP1108422, APP1196492 (JG), APP2002565, APP2021586 (MD), APP1149990, APP1135851, APP2026490 (SRL), Cancer Institute, NSW grant, ATRG2028 (JG)
Publisher Copyright:
© 2024
PY - 2024/11
Y1 - 2024/11
N2 - Chronic infection with Hepatitis B Virus (HBV) often results in a dysfunctional virus-specific T cell response hampering viral clearance. Paradoxically, intrahepatic inflammatory responses that contribute more to liver histopathology than to viral suppression are commonly observed, which are widely believed to be cell mediated. The involvement of humoral immunity in this process however is not well documented. To investigate the possible roles of HBV Capsid-Antibody Complexes (CACs) in eliciting chronic liver inflammation, we developed a novel microplate-based assay for the quantification of CACs in serum. The CACs assay showed high sensitivity and specificity with its readout closely correlating with the molecular features of CACs. A cross-sectional study on untreated chronic hepatitis B (CHB) patients showed a 77% positive rate for CACs with significant association with alanine transaminase (ALT), intrahepatic inflammation, and complement deposition, suggestive of its functional role in hepatic injury. Multiple staining of complement activation fragment C4d with major leukocyte and myofibroblast markers revealed an intertwined picture in periportal area with a morphology reminiscent of “piecemeal necrosis”. In a pooled cohort with ALT levels lower than 40 IU/ml, CACs alone revealed subclinical liver inflammation. We provide definitive evidence for a causative role for CACs in complement-mediated intrahepatic immunopathology, an additional mechanism contributing to liver damage in CHB. Assessment of CACs in serum complements current clinical markers for assessing CHB associated inflammation.
AB - Chronic infection with Hepatitis B Virus (HBV) often results in a dysfunctional virus-specific T cell response hampering viral clearance. Paradoxically, intrahepatic inflammatory responses that contribute more to liver histopathology than to viral suppression are commonly observed, which are widely believed to be cell mediated. The involvement of humoral immunity in this process however is not well documented. To investigate the possible roles of HBV Capsid-Antibody Complexes (CACs) in eliciting chronic liver inflammation, we developed a novel microplate-based assay for the quantification of CACs in serum. The CACs assay showed high sensitivity and specificity with its readout closely correlating with the molecular features of CACs. A cross-sectional study on untreated chronic hepatitis B (CHB) patients showed a 77% positive rate for CACs with significant association with alanine transaminase (ALT), intrahepatic inflammation, and complement deposition, suggestive of its functional role in hepatic injury. Multiple staining of complement activation fragment C4d with major leukocyte and myofibroblast markers revealed an intertwined picture in periportal area with a morphology reminiscent of “piecemeal necrosis”. In a pooled cohort with ALT levels lower than 40 IU/ml, CACs alone revealed subclinical liver inflammation. We provide definitive evidence for a causative role for CACs in complement-mediated intrahepatic immunopathology, an additional mechanism contributing to liver damage in CHB. Assessment of CACs in serum complements current clinical markers for assessing CHB associated inflammation.
KW - Complement
KW - HBV
KW - Immune complex
KW - Liver inflammation
UR - http://www.scopus.com/inward/record.url?scp=85206160730&partnerID=8YFLogxK
U2 - 10.1016/j.antiviral.2024.106017
DO - 10.1016/j.antiviral.2024.106017
M3 - Article
C2 - 39396554
AN - SCOPUS:85206160730
SN - 0166-3542
VL - 231
SP - 1
EP - 13
JO - Antiviral Research
JF - Antiviral Research
M1 - 106017
ER -