| Literature DB >> 30192392 |
Reina Sasaki1,2, Keith Meyer2, Mitsuhiko Moriyama3, Naoya Kato4, Osamu Yokosuka4, Ratna B Ray1,2, Rajeev Aurora5, Ranjit Ray2,5, Tatsuo Kanda3,4.
Abstract
Altered immune parameters associated with hepatitis C virus (HCV) genotype 1b infection and their correlation with virus eradication in direct-acting antivirals (DAA)-treated patients were examined. Thirty-one HCV-infected patients were treated with DAAs for 12 weeks. Pre-DAA-treatment and post-DAA-treatment sera were analyzed for cytokines/chemokines using MILLIPLEX MAP. Serum complement level and antibody neutralization activity were measured separately. Sera from 11 spontaneously cleared HCV subjects were included for comparison. Rapid virological responders (RVR) or end-of-treatment responders (EOTR) were defined as patients with HCV RNA negative at week 4 or positive at week 4 and negative at week 12, respectively. HCV RNA eradication and a decrease in liver fibrosis-related cytokines after treatment were observed when compared with pretreatment sera from RVR and EOTR. In pretreatment sera, interferons and T-helper 1 or 2 cell-associated cytokines/chemokines were significantly higher among RVR as compared with EOTR. Furthermore, serum complement and virus neutralizing antibody levels were higher in pretreatment RVR sera. Eradication of HCV RNA by DAA decreased liver fibrosis-related cytokines. Pretreatment sera from RVR displayed an enhanced cytokine/chemokine, complement and virus neutralizing antibody response as compared with EOTR sera. Our results suggested that enhanced host immune status may play an additive role on HCV RNA clearance by DAA.Entities:
Keywords: cytokines; direct-acting antivirals; helper T cells; hepatitis C virus; interferon
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Year: 2018 PMID: 30192392 DOI: 10.1002/jmv.25310
Source DB: PubMed Journal: J Med Virol ISSN: 0146-6615 Impact factor: 2.327