Characterization of CD8 super(+) cytotoxic T-lymphocyte responses after genetic immunization with retrovirus vectors expressing different forms of the hepatitis B virus core and e antigens

Characterization of CD8 super(+) cytotoxic T-lymphocyte responses after genetic immunization with retrovirus vectors expressing different forms of the hepatitis B virus core and e antigens

Cytotoxic T-lymphocyte (CTL) activity appears to play an important role in resolving hepatitis B virus (HBV) infection, and the ability to induce such responses remains an important goal for developing effective immunotherapeutics. A panel of recombinant retrovirus vectors expressing different forms...

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Veröffentlicht in:Journal of virology 1997-05, Vol.71 (5), p.3365-3374
Hauptverfasser: Townsend, K, Saellberg, M, O'Dea, J, Banks, T, Driver, D, Sauter, S, Chang, S M, Jolly, D J, Mento, S J, Milich, DR, Lee, WTL
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container_end_page 3374
container_issue 5
container_start_page 3365
container_title Journal of virology
container_volume 71
creator Townsend, K
Saellberg, M
O'Dea, J
Banks, T
Driver, D
Sauter, S
Chang, S M
Jolly, D J
Mento, S J
Milich, DR
Lee, WTL
description Cytotoxic T-lymphocyte (CTL) activity appears to play an important role in resolving hepatitis B virus (HBV) infection, and the ability to induce such responses remains an important goal for developing effective immunotherapeutics. A panel of recombinant retrovirus vectors expressing different forms of the HBV core antigen (HBcAg) or e antigen (eAg) were found to induce antigen-specific major histocompatibility complex-restricted CTL responses in both mice and macaques. In addition, a novel retrovirus vector expressing an HBcAg-neomycin phosphotransferase II (HBc-Neo) fusion protein [LHBc-NEO(6A3)], which allows the measurement of the anti-Neo antibody response as a means of directly tracking biological activity of the vector, was generated. Doses greater than 10 super(7) CFU were necessary to induce CTL responses in H-2 super(k) mice. Intramuscular injections with 10 super(8) CFU of the LHBc-NEO(6A3) retrovirus vector into rhesus monkeys induced HBc /eAg-specific antibody production and CD8 super(+) CTLs. The CTL response from one of the two responder rhesus monkeys was directed against a 9-residue peptide, GELMTLATW, at positions 63 to 71 of the HBc/eAg sequence. The CTL response is long lived, being detectable as late as 16 weeks after immunization, and can be boosted upon reimmunization. The potent ability of recombinant retrovirus vectors to induce HBcAg- and eAg-specific CTL responses may prove beneficial as a therapeutic treatment for chronic hepatitis B infection.
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title Characterization of CD8 super(+) cytotoxic T-lymphocyte responses after genetic immunization with retrovirus vectors expressing different forms of the hepatitis B virus core and e antigens
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