Chronic Hepatitis C Pathogenesis: Immune Response in the Liver Microenvironment and Peripheral Compartment

Daniela Alejandra Rios; Paola Cecilia Casciato; María Soledad Caldirola; María Isabel Gaillard; Cecilia Giadans; Beatriz Ameigeiras; Elena Noemí De Matteo; María Victoria Preciado; Pamela Valva

doi:10.3389/fcimb.2021.712105

Chronic Hepatitis C Pathogenesis: Immune Response in the Liver Microenvironment and Peripheral Compartment

Front Cell Infect Microbiol. 2021 Aug 3:11:712105. doi: 10.3389/fcimb.2021.712105. eCollection 2021.

Authors

Daniela Alejandra Rios¹, Paola Cecilia Casciato², María Soledad Caldirola³, María Isabel Gaillard³, Cecilia Giadans¹, Beatriz Ameigeiras⁴, Elena Noemí De Matteo¹, María Victoria Preciado¹, Pamela Valva¹

Affiliations

¹ Laboratory of Molecular Biology, Multidisciplinary Institute for Investigation in Pediatric Pathologies (IMIPP), CONICET-GCBA, Pathology Division, Ricardo Gutiérrez Children's Hospital, Buenos Aires, Argentina.
² Liver Unit, Italian's Hospital of Buenos Aires, Buenos Aires, Argentina.
³ Immunology Unit, Multidisciplinary Institute for Investigation in Pediatric Pathologies (IMIPP), CONICET-GCBA, Ricardo Gutiérrez Children's Hospital, Buenos Aires, Argentina.
⁴ Liver Unit, Ramos Mejía Hospital, Buenos Aires, Argentina.

Abstract

Chronic hepatitis C (CHC) pathogenic mechanisms as well as the participation of the immune response in the generation of liver damage are still a topic of interest. Here, we evaluated immune cell populations and cytokines in the liver and peripheral blood (PB) to elucidate their role in CHC pathogenesis. B, CTL, Th, Treg, Th1, Th17, and NK cell localization and frequency were evaluated on liver biopsies by immunohistochemistry, while frequency, differentiation, and functional status on PB were evaluated by flow cytometry. TNF-α, IL-23, IFN-γ, IL-1β, IL-6, IL-8, IL-17A, IL-21, IL-10, and TGF-β expression levels were quantified in fresh liver biopsy by RT-qPCR and in plasma by CBA/ELISA. Liver CTL and Th1 at the lobular area inversely correlated with viral load (r = -0.469, p =0.003 and r = -0.384, p = 0.040). Treg correlated with CTL and Th1 at the lobular area (r = 0.784, p < 0.0001; r = 0.436, p = 0.013). Th17 correlated with hepatic IL-8 (r = 0.52, p < 0.05), and both were higher in advanced fibrosis cases (Th17 p = 0.0312, IL-8 p = 0.009). Hepatic cytokines were higher in severe hepatitis cases (IL-1β p = 0.026, IL-23 p = 0.031, IL-8 p = 0.002, TGF-β, p= 0.037). Peripheral NK (p = 0.008) and NK dim (p = 0.018) were diminished, while NK bright (p = 0.025) was elevated in patients vs. donors. Naïve Th (p = 0.011) and CTL (p = 0.0007) were decreased, while activated Th (p = 0.0007) and CTL (p = 0.0003) were increased. IFN-γ production and degranulation activity in NK and CTL were normal. Peripheral cytokines showed an altered profile vs. donors, particularly elevated IL-6 (p = 0.008) and TGF-β (p = 0.041). Total hepatic CTLs favored damage. Treg could not prevent fibrogenesis triggered by Th17 and IL-8. Peripheral T-lymphocyte differentiation stage shift, elevated cytokine levels and NK-cell count decrease would contribute to global disease.

Keywords: HCV: Hepatitis C virus; Th17; Treg: regulatory T lymphocytes; chronic liver disease; immunopathogenesis; inflammatory liver infiltrate; peripheral blood.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Hepatitis C, Chronic*
Humans
Immunity
T-Lymphocytes, Regulatory
Th17 Cells