Peripheral blood correlates of virologic relapse after Sofosbuvir and Ribavirin treatment of Genotype-1 HCV infection

Cody Orr; Wenjie Xu; Henry Masur; Shyam Kottilil; Eric G. Meissner

doi:10.1186/s12879-020-05657-5

BMC Infectious Diseases (Dec 2020)

Peripheral blood correlates of virologic relapse after Sofosbuvir and Ribavirin treatment of Genotype-1 HCV infection

Cody Orr,
Wenjie Xu,
Henry Masur,
Shyam Kottilil,
Eric G. Meissner

Affiliations

Cody Orr: Division of Infectious Diseases, Medical University of South Carolina
Wenjie Xu: Nanostring Technologies
Henry Masur: Critical Care Medicine Department, NIH Clinical Center, National Institutes of Health
Shyam Kottilil: Division of Clinical Care and Research, Institute of Human Virology, University of Maryland School of Medicine
Eric G. Meissner: Division of Infectious Diseases, Medical University of South Carolina

DOI: https://doi.org/10.1186/s12879-020-05657-5
Journal volume & issue: Vol. 20, no. 1
pp. 1 – 9

Abstract

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Abstract Background Treatment of chronic hepatitis C virus infection with direct acting antiviral therapy results in viral elimination in over 90% of cases. The duration of treatment required to achieve cure differs between individuals and relapse can occur. We asked whether cellular and transcriptional profiling of peripheral blood collected during treatment could identify biomarkers predictive of treatment outcome. Methods We analyzed peripheral blood collected during treatment of genotype 1 HCV with 24 weeks of sofosbuvir and weight-based or low dose ribavirin in a trial in which 29% of patients relapsed. Changes in host immunity during treatment were assessed by flow cytometry and whole blood gene expression profiling. Differences in expression of immune-relevant transcripts based on treatment outcome were analyzed using the Nanostring Human Immunology V2 panel. Results Multiple cellular populations changed during treatment, but pre-treatment neutrophil counts were lower and natural post-treatment killer cell counts were higher in patients who relapsed. Pre-treatment expression of genes associated with interferon-signaling, T-cell dysfunction, and T-cell co-stimulation differed by treatment outcome. We identified a pre- and post-treatment gene expression signature with high predictive capacity for distinguishing treatment outcome, but neither signature was sufficiently robust to suggest viability for clinical use. Conclusions Patients who relapse after hepatitis C virus therapy differ immunologically from non-relapsers based on expression of transcripts related to interferon signaling and T-cell dysfunction, as well as by peripheral neutrophil and NK-cell concentrations. These data provide insight into the host immunologic basis of relapse after DAA therapy for HCV and suggests mechanisms which may be relevant for understanding outcomes with currently approved regimens.

Published in BMC Infectious Diseases

ISSN: 1471-2334 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Infectious and parasitic diseases
Website: https://bmcinfectdis.biomedcentral.com

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