AI Article Synopsis

  • Lamivudine therapy can temporarily boost antiviral T cell responses in chronic hepatitis B patients, but this increase isn't long-lasting.
  • A study involving 12 patients monitored their HBV-specific CD4 and CD8 T cells over time, revealing an initial rise in their activity followed by a decline after about 5-6 months of treatment.
  • Findings suggest that early therapeutic targeting of T cell responses is important, as the temporary nature of the immune boost could lead to virus reactivation once treatment ends.

Article Abstract

Background/aims: Lamivudine therapy in patients with chronic hepatitis B can induce the recovery of antiviral T cell responses. It is unknown whether the recovery of T cell responsiveness is long-lasting and persists throughout the treatment and whether the elevation of viremia which follows therapy withdrawal can restore a condition of T cell unresponsiveness.

Methods: Frequency and function of circulating hepatitis B virus (HBV)-specific CD4 and CD8 cells from 12 hepatitis e surface antigen + patients with chronic hepatitis B were studied longitudinally before, during and after lamivudine therapy by intracellular cytokine staining, proliferation and cytotoxicity assays against HBV proteins and peptides. CD4-mediated responses were analyzed in all patients, whereas CD8 cells were studied in 6 HLA-A2+ patients.

Results: HBV-specific CD4 and CD8 reactivity showed a bi-phasic behavior under lamivudine therapy with an early enhancement of T cell frequency and intensity of responses followed by a persistent decline starting from the 5th to 6th month of treatment.

Conclusions: Since restoration of HBV-specific T cell reactivity is only transient, our study indicates that therapeutic stimulation of HBV-specific T cell responses to complement lamivudine treatment should be done early after the initiation of lamivudine. Moreover, the transient nature of the immune reconstitution may represent a favorable condition for virus reactivation once lamivudine therapy is withdrawn.

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Source
http://dx.doi.org/10.1016/s0168-8278(03)00292-7DOI Listing

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