Hepatitis C Virus Persistence after Spontaneous or Treatment-Induced Resolution of Hepatitis C

doi:10.1128/JVI.78.11.5867-5874.2004

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Hepatitis C Virus Persistence after Spontaneous or Treatment-Induced Resolution of Hepatitis C

Tram N. Q. Pham,¹ Sonya A. MacParland,¹ Patricia M. Mulrooney,¹ Helen Cooksley,² Nikolai V. Naoumov,² and Tomasz I. Michalak¹^,3^*

Molecular Virology and Hepatology Research, Division of Basic Medical Science,¹ Division of Pathology, Faculty of Medicine, Memorial University, St. John's, Newfoundland, Canada,³ Institute of Hepatology, University College London, London, England²

Received 10 December 2003/ Accepted 3 February 2004

It is presumed that resolution of hepatitis C, as evidencedby normalization of liver function tests and disappearance ofhepatitis C virus (HCV) RNA from serum, as determined by conventionallaboratory assays, reflects virus eradication. In this study,we examined the expression of the HCV genome in the sera, peripheralblood mononuclear cells (PBMC), and, on some occasions, monocyte-deriveddendritic cells (DC) long after resolution of hepatitis C byusing a highly sensitive reverse transcription (RT)-PCR-nucleicacid hybridization (RT-PCR-NAH) assay. The samples obtainedfrom 16 randomly selected patients (5 with spontaneous and 11with treatment-induced resolution), monitored for up to 5 years,were studied by qualitative and semiquantitative RT-PCR-NAHand by real-time RT-PCR to detect the HCV RNA positive strand.The replicative HCV RNA negative strand was examined in PBMCafter culture with a T-cell proliferation stimulating mitogen.The findings show that HCV RNA was carried in the convalescent-phasesera and/or PBMC in all 16 individuals investigated. Also, DCfrom six of seven patients were reactive for the HCV genome.Importantly, traces of the HCV RNA negative strand, suggestingprogressing virus replication, were detected in the majorityof mitogen-stimulated PBMC, including four samples collected5 years after recovery. Sequencing of the HCV 5' untranslatedregion fragment revealed genotype 1b in four of nine individualsexamined and genotypes 1a and 2a in three and two patients,respectively. These results imply that HCV RNA can persist atvery low levels in the serum and peripheral lymphoid cells andthat an intermediate replicative form of the HCV genome canpersist in PBMC for many years after apparently complete spontaneousor antiviral therapy-induced resolution of chronic hepatitisC.

* Corresponding author. Mailing address: Molecular Virology and Hepatology Research, Faculty of Medicine, Health Science Centre, Memorial University, St. John's, Newfoundland, Canada A1B 3V6. Phone: (709) 777-7301. Fax: (709) 777-8279. E-mail: timich{at}mun.ca.

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