Intracellular inactivation of the hepatitis B virus by cytotoxic T lymphocytes

Luca G. Guidotti; Tetsuya Ishikawa; Monte V. Hobbs; Brent Matzke; Robert Schreiber; Francis V. Chisari

doi:10.1016/S1074-7613(00)80295-2

Intracellular inactivation of the hepatitis B virus by cytotoxic T lymphocytes

Luca G. Guidotti, Tetsuya Ishikawa, Monte V. Hobbs, Brent Matzke, Robert Schreiber, Francis V. Chisari

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

928 Scopus citations

Abstract

It is widely believed that viral clearance is mediated principally by the destruction of infected cells by CTLs. In this report, we use a transgenic mouse model of HBV replication to demonstrate that this assumption may not be true for all viruses. We find that adoptively transferred virus-specific CTLs can abolish HBV gene expression and replication in the liver without killing the hepatocytes. This antiviral function is mediated by IFNγ and TNFα secreted by the CTL or by the antigen-nonspecific macrophages and T cells that they activate following antigen recognition. These cytokines activate two independent virocidal pathways: the first pathway eliminates HBV nucleocapsid particles and their cargo of replicating viral genomes, while the second pathway destabilizes the viral RNA. Intracellular viral inactivation mechanisms such as these could greatly amplify the protective effects of the immune response, while failure of such mechanisms could lead to viral persistence or to the death of the host.

Original language	English
Pages (from-to)	25-36
Number of pages	12
Journal	Immunity
Volume	4
Issue number	1
DOIs	https://doi.org/10.1016/S1074-7613(00)80295-2
State	Published - Jan 1996

Access to Document

10.1016/S1074-7613(00)80295-2

Cite this

@article{8e41ca3f06c84d668a1c8993e2c019a9,

title = "Intracellular inactivation of the hepatitis B virus by cytotoxic T lymphocytes",

abstract = "It is widely believed that viral clearance is mediated principally by the destruction of infected cells by CTLs. In this report, we use a transgenic mouse model of HBV replication to demonstrate that this assumption may not be true for all viruses. We find that adoptively transferred virus-specific CTLs can abolish HBV gene expression and replication in the liver without killing the hepatocytes. This antiviral function is mediated by IFNγ and TNFα secreted by the CTL or by the antigen-nonspecific macrophages and T cells that they activate following antigen recognition. These cytokines activate two independent virocidal pathways: the first pathway eliminates HBV nucleocapsid particles and their cargo of replicating viral genomes, while the second pathway destabilizes the viral RNA. Intracellular viral inactivation mechanisms such as these could greatly amplify the protective effects of the immune response, while failure of such mechanisms could lead to viral persistence or to the death of the host.",

author = "Guidotti, {Luca G.} and Tetsuya Ishikawa and Hobbs, {Monte V.} and Brent Matzke and Robert Schreiber and Chisari, {Francis V.}",

note = "Funding Information: The authors thank Drs. H.-J. Schlicht and J. Kock for performing polymerase chain reaction–based detection of HBV cccDNA; Drs. D. K{\"a}gi, H. Hengartner, and R. Zinkernagel for providing HBV-primed cells from their perforin knockout mice; Drs. R. H. Costa and U. Samadani for performing RNAse protection assays for HNF3α, HNF3β, and transthyretin in CTL-injected animals; Dr. D. Bylund and Mr. D. Duncan and the Scripps Immunology Reference Laboratory for performing serum HBV DNA quantitation; Dr. R. Hyman for providing the mCD8α (DM) subclone; J. Price and the Scripps Transgenic Mouse Facility for embryo microinjections; Ms. M. Pagels for preparation and staining of tissue sections; Mr. R. Koch and Ms. J. Chung for excellent technical assistance; and Ms. B. Weier for help with manuscript preparation. This work was supported by grants R37CA40489 and AG09822 from the National Insitutes of Health. This is manuscript number 9463-MEM from the Scripps Research Institute. ",

year = "1996",

month = jan,

doi = "10.1016/S1074-7613(00)80295-2",

language = "English",

volume = "4",

pages = "25--36",

journal = "Immunity",

issn = "1074-7613",

number = "1",

}

TY - JOUR

T1 - Intracellular inactivation of the hepatitis B virus by cytotoxic T lymphocytes

AU - Guidotti, Luca G.

AU - Ishikawa, Tetsuya

AU - Hobbs, Monte V.

AU - Matzke, Brent

AU - Schreiber, Robert

AU - Chisari, Francis V.

N1 - Funding Information: The authors thank Drs. H.-J. Schlicht and J. Kock for performing polymerase chain reaction–based detection of HBV cccDNA; Drs. D. Kägi, H. Hengartner, and R. Zinkernagel for providing HBV-primed cells from their perforin knockout mice; Drs. R. H. Costa and U. Samadani for performing RNAse protection assays for HNF3α, HNF3β, and transthyretin in CTL-injected animals; Dr. D. Bylund and Mr. D. Duncan and the Scripps Immunology Reference Laboratory for performing serum HBV DNA quantitation; Dr. R. Hyman for providing the mCD8α (DM) subclone; J. Price and the Scripps Transgenic Mouse Facility for embryo microinjections; Ms. M. Pagels for preparation and staining of tissue sections; Mr. R. Koch and Ms. J. Chung for excellent technical assistance; and Ms. B. Weier for help with manuscript preparation. This work was supported by grants R37CA40489 and AG09822 from the National Insitutes of Health. This is manuscript number 9463-MEM from the Scripps Research Institute.

PY - 1996/1

Y1 - 1996/1

N2 - It is widely believed that viral clearance is mediated principally by the destruction of infected cells by CTLs. In this report, we use a transgenic mouse model of HBV replication to demonstrate that this assumption may not be true for all viruses. We find that adoptively transferred virus-specific CTLs can abolish HBV gene expression and replication in the liver without killing the hepatocytes. This antiviral function is mediated by IFNγ and TNFα secreted by the CTL or by the antigen-nonspecific macrophages and T cells that they activate following antigen recognition. These cytokines activate two independent virocidal pathways: the first pathway eliminates HBV nucleocapsid particles and their cargo of replicating viral genomes, while the second pathway destabilizes the viral RNA. Intracellular viral inactivation mechanisms such as these could greatly amplify the protective effects of the immune response, while failure of such mechanisms could lead to viral persistence or to the death of the host.

AB - It is widely believed that viral clearance is mediated principally by the destruction of infected cells by CTLs. In this report, we use a transgenic mouse model of HBV replication to demonstrate that this assumption may not be true for all viruses. We find that adoptively transferred virus-specific CTLs can abolish HBV gene expression and replication in the liver without killing the hepatocytes. This antiviral function is mediated by IFNγ and TNFα secreted by the CTL or by the antigen-nonspecific macrophages and T cells that they activate following antigen recognition. These cytokines activate two independent virocidal pathways: the first pathway eliminates HBV nucleocapsid particles and their cargo of replicating viral genomes, while the second pathway destabilizes the viral RNA. Intracellular viral inactivation mechanisms such as these could greatly amplify the protective effects of the immune response, while failure of such mechanisms could lead to viral persistence or to the death of the host.

UR - http://www.scopus.com/inward/record.url?scp=0030021968&partnerID=8YFLogxK

U2 - 10.1016/S1074-7613(00)80295-2

DO - 10.1016/S1074-7613(00)80295-2

M3 - Article

C2 - 8574849

AN - SCOPUS:0030021968

SN - 1074-7613

VL - 4

SP - 25

EP - 36

JO - Immunity

JF - Immunity

IS - 1

ER -

Intracellular inactivation of the hepatitis B virus by cytotoxic T lymphocytes

Abstract

Access to Document

Other files and links

Fingerprint

Cite this