HCV-Specific T-Cell Response in Relation to Viral Kinetics and Treatment Outcome (DITTO-HCV Project)

Massimo Pilli; Alessandro Zerbini; Amalia Penna; Alessandra Orlandini; Esther Lukasiewicz; Jean Michel Pawlotsky; Stefan Zeuzem; Solko W. Schalm; Michael von Wagner; Georgios Germanidis; Yoav Lurie; Juan I. Esteban; Bart L. Haagmans; Christophe Hezode; Martin Lagging; Francesco Negro; Yonit Homburger; Avidan U. Neumann; Carlo Ferrari; Gabriele Missale

doi:10.1053/j.gastro.2007.06.059

HCV-Specific T-Cell Response in Relation to Viral Kinetics and Treatment Outcome (DITTO-HCV Project)

Massimo Pilli, Alessandro Zerbini, Amalia Penna, Alessandra Orlandini, Esther Lukasiewicz, Jean Michel Pawlotsky, Stefan Zeuzem, Solko W. Schalm, Michael von Wagner, Georgios Germanidis, Yoav Lurie, Juan I. Esteban, Bart L. Haagmans, Christophe Hezode, Martin Lagging, Francesco Negro, Yonit Homburger, Avidan U. Neumann, Carlo Ferrari, Gabriele Missale

The Mina and Everard Goodman Faculty of Life Sciences - at Bar-Ilan University

Research output: Contribution to journal › Article › peer-review

56 Scopus citations

Abstract

Background & Aims: The second slope of viral decline induced by interferon treatment has been suggested to be influenced mainly by the hepatitis C virus (HCV)-specific T-cell response; however, this hypothesis needs to be validated by results derived from experimental studies. Methods: To address this issue, the HCV-specific T-cell response of 32 genotype-1-infected patients of the 270 patients enrolled in the dynamically individualized treatment of hepatitis C infection and correlates of viral/host dynamics phase III, open-label, randomized, multicenter trial was studied in relation to viral kinetics and treatment outcome. Results: Greater proliferative responses by HCV-specific CD8 cells were found before treatment in patients with a fast viral decline and with a sustained viral response. However, no significant improvement of HCV-specific CD8 responses was observed in the first weeks of therapy in both rapid viral responder and non-rapid viral responder patients. A mild enhancement of proliferative T-cell responses and a partial restoration of the cytotoxic T-cell potential was expressed only late during treatment, likely favored by HCV clearance. Conclusions: Early restoration of an efficient T-cell response does not seem to be an essential requirement for a rapid viral decline in the first weeks of treatment. However, patients presenting a better HCV-specific CD8 cell proliferative potential at baseline are more likely to present a rapid and sustained viral response. Therefore, future treatment protocols should consider the development of strategies aimed at improving HCV-specific T-cell responses.

Original language	English
Pages (from-to)	1132-1143
Number of pages	12
Journal	Gastroenterology
Volume	133
Issue number	4
DOIs	https://doi.org/10.1053/j.gastro.2007.06.059
State	Published - Oct 2007

Bibliographical note

Funding Information:
Supported by the European Community (QLK2-2000-00836), Hoffmann La-Roche, and Maxim Pharmaceuticals. J–M.P. has received research grants from Roche and is an advisor of Roche; S.Z. is a consultant for Roche and Schering-Plough; S.W.S. has received research grants from Roche and Schering-Plough. A.N. is a consultant for Roche, Schering-Plough, and Human Genome Sciences and has received research grants from Roche and Human Genome Sciences.

Funding

Supported by the European Community (QLK2-2000-00836), Hoffmann La-Roche, and Maxim Pharmaceuticals. J–M.P. has received research grants from Roche and is an advisor of Roche; S.Z. is a consultant for Roche and Schering-Plough; S.W.S. has received research grants from Roche and Schering-Plough. A.N. is a consultant for Roche, Schering-Plough, and Human Genome Sciences and has received research grants from Roche and Human Genome Sciences.

Funders	Funder number
Hoffmann La-Roche
Maxim Pharmaceuticals
European Commission	QLK2-2000-00836

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1053/j.gastro.2007.06.059

Cite this

Pilli, M., Zerbini, A., Penna, A., Orlandini, A., Lukasiewicz, E., Pawlotsky, J. M., Zeuzem, S., Schalm, S. W., von Wagner, M., Germanidis, G., Lurie, Y., Esteban, J. I., Haagmans, B. L., Hezode, C., Lagging, M., Negro, F., Homburger, Y., Neumann, A. U., Ferrari, C., & Missale, G. (2007). HCV-Specific T-Cell Response in Relation to Viral Kinetics and Treatment Outcome (DITTO-HCV Project). Gastroenterology, 133(4), 1132-1143. https://doi.org/10.1053/j.gastro.2007.06.059

@article{561fc9d9296e4a2d86797016b2c8e2a2,

title = "HCV-Specific T-Cell Response in Relation to Viral Kinetics and Treatment Outcome (DITTO-HCV Project)",

abstract = "Background \& Aims: The second slope of viral decline induced by interferon treatment has been suggested to be influenced mainly by the hepatitis C virus (HCV)-specific T-cell response; however, this hypothesis needs to be validated by results derived from experimental studies. Methods: To address this issue, the HCV-specific T-cell response of 32 genotype-1-infected patients of the 270 patients enrolled in the dynamically individualized treatment of hepatitis C infection and correlates of viral/host dynamics phase III, open-label, randomized, multicenter trial was studied in relation to viral kinetics and treatment outcome. Results: Greater proliferative responses by HCV-specific CD8 cells were found before treatment in patients with a fast viral decline and with a sustained viral response. However, no significant improvement of HCV-specific CD8 responses was observed in the first weeks of therapy in both rapid viral responder and non-rapid viral responder patients. A mild enhancement of proliferative T-cell responses and a partial restoration of the cytotoxic T-cell potential was expressed only late during treatment, likely favored by HCV clearance. Conclusions: Early restoration of an efficient T-cell response does not seem to be an essential requirement for a rapid viral decline in the first weeks of treatment. However, patients presenting a better HCV-specific CD8 cell proliferative potential at baseline are more likely to present a rapid and sustained viral response. Therefore, future treatment protocols should consider the development of strategies aimed at improving HCV-specific T-cell responses.",

author = "Massimo Pilli and Alessandro Zerbini and Amalia Penna and Alessandra Orlandini and Esther Lukasiewicz and Pawlotsky, \{Jean Michel\} and Stefan Zeuzem and Schalm, \{Solko W.\} and \{von Wagner\}, Michael and Georgios Germanidis and Yoav Lurie and Esteban, \{Juan I.\} and Haagmans, \{Bart L.\} and Christophe Hezode and Martin Lagging and Francesco Negro and Yonit Homburger and Neumann, \{Avidan U.\} and Carlo Ferrari and Gabriele Missale",

note = "Funding Information: Supported by the European Community (QLK2-2000-00836), Hoffmann La-Roche, and Maxim Pharmaceuticals. J–M.P. has received research grants from Roche and is an advisor of Roche; S.Z. is a consultant for Roche and Schering-Plough; S.W.S. has received research grants from Roche and Schering-Plough. A.N. is a consultant for Roche, Schering-Plough, and Human Genome Sciences and has received research grants from Roche and Human Genome Sciences. ",

year = "2007",

month = oct,

doi = "10.1053/j.gastro.2007.06.059",

language = "אנגלית",

volume = "133",

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Pilli, M, Zerbini, A, Penna, A, Orlandini, A, Lukasiewicz, E, Pawlotsky, JM, Zeuzem, S, Schalm, SW, von Wagner, M, Germanidis, G, Lurie, Y, Esteban, JI, Haagmans, BL, Hezode, C, Lagging, M, Negro, F, Homburger, Y, Neumann, AU, Ferrari, C & Missale, G 2007, 'HCV-Specific T-Cell Response in Relation to Viral Kinetics and Treatment Outcome (DITTO-HCV Project)', Gastroenterology, vol. 133, no. 4, pp. 1132-1143. https://doi.org/10.1053/j.gastro.2007.06.059

TY - JOUR

T1 - HCV-Specific T-Cell Response in Relation to Viral Kinetics and Treatment Outcome (DITTO-HCV Project)

AU - Pilli, Massimo

AU - Zerbini, Alessandro

AU - Penna, Amalia

AU - Orlandini, Alessandra

AU - Lukasiewicz, Esther

AU - Pawlotsky, Jean Michel

AU - Zeuzem, Stefan

AU - Schalm, Solko W.

AU - von Wagner, Michael

AU - Germanidis, Georgios

AU - Lurie, Yoav

AU - Esteban, Juan I.

AU - Haagmans, Bart L.

AU - Hezode, Christophe

AU - Lagging, Martin

AU - Negro, Francesco

AU - Homburger, Yonit

AU - Neumann, Avidan U.

AU - Ferrari, Carlo

AU - Missale, Gabriele

N1 - Funding Information: Supported by the European Community (QLK2-2000-00836), Hoffmann La-Roche, and Maxim Pharmaceuticals. J–M.P. has received research grants from Roche and is an advisor of Roche; S.Z. is a consultant for Roche and Schering-Plough; S.W.S. has received research grants from Roche and Schering-Plough. A.N. is a consultant for Roche, Schering-Plough, and Human Genome Sciences and has received research grants from Roche and Human Genome Sciences.

PY - 2007/10

Y1 - 2007/10

N2 - Background & Aims: The second slope of viral decline induced by interferon treatment has been suggested to be influenced mainly by the hepatitis C virus (HCV)-specific T-cell response; however, this hypothesis needs to be validated by results derived from experimental studies. Methods: To address this issue, the HCV-specific T-cell response of 32 genotype-1-infected patients of the 270 patients enrolled in the dynamically individualized treatment of hepatitis C infection and correlates of viral/host dynamics phase III, open-label, randomized, multicenter trial was studied in relation to viral kinetics and treatment outcome. Results: Greater proliferative responses by HCV-specific CD8 cells were found before treatment in patients with a fast viral decline and with a sustained viral response. However, no significant improvement of HCV-specific CD8 responses was observed in the first weeks of therapy in both rapid viral responder and non-rapid viral responder patients. A mild enhancement of proliferative T-cell responses and a partial restoration of the cytotoxic T-cell potential was expressed only late during treatment, likely favored by HCV clearance. Conclusions: Early restoration of an efficient T-cell response does not seem to be an essential requirement for a rapid viral decline in the first weeks of treatment. However, patients presenting a better HCV-specific CD8 cell proliferative potential at baseline are more likely to present a rapid and sustained viral response. Therefore, future treatment protocols should consider the development of strategies aimed at improving HCV-specific T-cell responses.

AB - Background & Aims: The second slope of viral decline induced by interferon treatment has been suggested to be influenced mainly by the hepatitis C virus (HCV)-specific T-cell response; however, this hypothesis needs to be validated by results derived from experimental studies. Methods: To address this issue, the HCV-specific T-cell response of 32 genotype-1-infected patients of the 270 patients enrolled in the dynamically individualized treatment of hepatitis C infection and correlates of viral/host dynamics phase III, open-label, randomized, multicenter trial was studied in relation to viral kinetics and treatment outcome. Results: Greater proliferative responses by HCV-specific CD8 cells were found before treatment in patients with a fast viral decline and with a sustained viral response. However, no significant improvement of HCV-specific CD8 responses was observed in the first weeks of therapy in both rapid viral responder and non-rapid viral responder patients. A mild enhancement of proliferative T-cell responses and a partial restoration of the cytotoxic T-cell potential was expressed only late during treatment, likely favored by HCV clearance. Conclusions: Early restoration of an efficient T-cell response does not seem to be an essential requirement for a rapid viral decline in the first weeks of treatment. However, patients presenting a better HCV-specific CD8 cell proliferative potential at baseline are more likely to present a rapid and sustained viral response. Therefore, future treatment protocols should consider the development of strategies aimed at improving HCV-specific T-cell responses.

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HCV-Specific T-Cell Response in Relation to Viral Kinetics and Treatment Outcome (DITTO-HCV Project)

Abstract

Bibliographical note

Funding

UN SDGs

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