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Re-evaluation of hepatitis B virus clinical phases by systems biology identifies unappreciated roles for the innate immune response and B cells
Thomas Vanwolleghem1, Jun Hou1, Gertine van Oord1, Arno C. Andeweg2, A.D.M.E. Osterhaus2, Suzan D. Pas2, Harry L.A. Janssen1,3,† andAndre Boonstra1,†,*
Article first published online: 27 APR 2015
DOI: 10.1002/hep.27805
© 2015 by the American Association for the Study of Liver Diseases
I
Hepatology
Volume 62, Issue 1, pages 87–100, July 2015
Article has an altmetric score of 7
1 Department of Gastroenterology and Hepatology, Erasmus University Medical Center, Rotterdam, The Netherlands
2 Department of Viroscience, Erasmus University Medical Center, Rotterdam, The Netherlands
3 Liver Clinic, University Health Network, Toronto, Ontario, Canada
† These authors contributed equally.
*Address reprint requests to: Andre Boonstra, Ph.D., Department of Gastroenterology and Hepatology, Na10-11, Erasmus MC, University Hospital Rotterdam, 3000 CA Rotterdam, The Netherlands. E-mail: [email protected]; fax: +31-10-7044762.
Potential conflict of interest: Prof. Janssen consults for and received grants from AbbVie, Bristol-Myers Squibb, Gilead, Innogenetics, Janssen, Medimmune, Medtronic, Merck, Novartis, and Roche. He consults for ISIS and Tekmira. Dr. Boonstra consults for and received grants from Bristol-Myers Squibb. He received grants from Gilead, Roche, and Janssen. Dr. Vanwolleghem received grants from Gilead and Bristol-Myers Squibb. Prof. Osterhaus consults for Viroclinics Biosciences.
This study was supported by the Virgo Consortium, funded by the Dutch government (project no.: FES0908) and the Netherlands Genomics Initiative (project no.: 050-060-452). T.V. is the recipient of an Erasmus MC Fellowship 2011.
To identify immunological mechanisms that govern distinct clinical phases of a chronic hepatitis B virus (HBV) infection—immune tolerant (IT), immune active (IA), inactive carrier (IC), and hepatitis B e antigen (HBeAg)-negative (ENEG) hepatitis phases—we performed a systems biology study. Serum samples from untreated chronic HBV patients (n = 71) were used for multiplex cytokine measurements, quantitative hepatitis B surface antigen (HBsAg), HBeAg levels, HBV genotype, and mutant analysis. Leukocytes were phenotyped using multicolor flow cytometry, and whole-blood transcriptome profiles were generated. The latter were compared with liver biopsy transcriptomes from IA (n = 16) and IT (n = 3) patients. HBV viral load as well as HBeAg and HBsAg levels (P < 0.001), but not leukocyte composition, differed significantly between distinct phases. Serum macrophage chemotactic protein 1, interleukin-12p40, interferon (IFN)-gamma-inducible protein 10, and macrophage inflammatory protein 1 beta levels were different between two or more clinical phases (P < 0.05). Comparison of blood transcriptomes identified 64 differentially expressed genes. The gene signature distinguishing IA from IT and IC patients was predominantly composed of highly up-regulated immunoglobulin-encoding genes. Modular repertoire analysis using gene sets clustered according to similar expression patterns corroborated the abundant expression of B-cell function-related genes in IA patients and pointed toward increased (ISG) transcript levels in IT patients, compared to subsequent phases. Natural killer cell activities were clustered in clinical phases with biochemical liver damage (IA and ENEG phases), whereas T-cell activities were higher in all phases, compared to IT patients. B-cell-related transcripts proved to be higher in biopsies from IA versus IT patients. Conclusion: HBV clinical phases are characterized by distinct blood gene signatures. Innate IFN and B-cell responses are highly active during the IT and IA phases, respectively. This suggests that the presumed immune tolerance in chronic HBV infections needs to be redefined. (Hepatology 2015;62:87-100)
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发表于 2015-6-28 12:57
