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- 2022-12-28
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Reduction of HBV replication prolongs the early immunological response to IFNa therapy
Anthony T. Tan 1,�, Long Truong Hoang 2,�, Daniel Chin 3, Erik Rasmussen 3, Uri Lopatin 3,��,
Stefan Hart 3, Hans Bitter 3, Tom Chu 3, Lore Gruenbaum 3, Palani Ravindran 3, Hua Zhong 3,
Ed Gane 4, Seng Gee Lim 5, Wan Cheng Chow 6, Pei-Jer Chen 7, Rosemary Petric 3,
Antonio Bertoletti 1,8,⇑,�, Martin Lloyd Hibberd 2,�
1 Singapore Institute for Clinical Sciences, A⁄STAR, Singapore;
2 Genome Institute of Singapore, A⁄STAR, Singapore;
3 Hoffmann-La Roche,
Switzerland;
4 Auckland City Hospital, Auckland, New Zealand;
5 National University Hospital, Singapore;
6 Singapore General Hospital, Singapore;
7 National Taiwan University Hospital, Taipei, Taiwan;
8 Program in Emerging Infectious Disease, Duke-NUS Graduate Medical School, Singapore
Background & Aims: The interaction between HBV replication
and immune modulatory effects mediated by IFNa therapy is
not well understood. We characterized the impact of HBV DNA
replication on the early IFNa-induced immunomodulatory
mechanisms.
Methods:We interrogated the transcriptional, serum cytokine/
chemokine and cellular immune profiles of 28 patients with
HBeAg+ chronic HBV infection (CHB) randomly assigned to one
of 4 treatment cohorts (untreated n = 5, weekly dosing of
360 lg Pegasys� [PegIFNa] n = 11, daily dose of 300 mg Viread�
[tenofovir disoproxil fumarate, TDF] n = 6, or a combination of
both n = 6). Samples were characterized at multiple early time
points through day 14 of therapy, after which all patients were
given standard of care (180 lg Pegasys� injected subcutaneously,
weekly).
Results: PegIFNa induced a distinct and rapid up-regulation of
IFN signaling pathway that coincided with increase detection of
distinct serum cytokines/chemokines (IL-15, IL-6, and CXCL-10)
and the up-regulation of the frequency of proliferating NK and
activated total CD8+ T cells. IFNa treatment alone did not result
in rapid decay of HBV replication and was not able to restore
the defective HBV-specific T cell response present in CHB
patients. In addition, the IFNa immune-stimulatory effects
diminished after the first dose, but this refractory effect was
reduced in patients where HBV replication was simultaneously
inhibited with TDF.
Conclusions:We present here the first comprehensive description
of the early effects of IFNa treatment on immune and viral
biomarkers in HBeAg+ CHB patients. Our results show that
PegIFNa-induced innate immune activation directly benefits
from the suppression of HBV replication.
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发表于 2013-12-15 13:40