High frequency of functional anti-YMDD and -mutant cytotoxic T lymphocytes after in vitro expansion correlates with successful response to lamivudine therapy for chronic hepatitis B

Lin, Chun-Yao; Tsai, S-L; Lee, Tzong-Hsien; Chien, Rong‐Nan; Sk, Liao; Yf, Liaw

doi:10.1136/gut.2003.032920

Cited by 21 publications

(20 citation statements)

References 52 publications

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“…Likewise, Figure 1b shows the prediction of 15-mer peptides of continuous amino acid sequences on HBcAg 1-30 using the SYFPEITHI scoring system on DRB1*0401 molecule correlates proliferation assays of CD4 + CD25 + T reg cells from DRB1*0401 patients in terms of [H 3 ] thymidine incorporation. The proliferation in response to peptide P16 (HBcAg [16][17][18][19][20][21][22][23][24][25][26][27][28][29][30] , with an SYFPEITHI score = 20 on DRB1*0401 molecule) was comparable to that of rHBcAg, thus this peptide (as P2 in Supplementary Table 1) was selected for the construction of DRB1*0401 tetramer in this study. These data of proliferation are consistent with reports that MHC class II tetramers may identify peptide-specific human CD4 + T cells proliferating to viral antigens [27,34], and with that T reg cell population could be induced and expanded by foreign antigen [35].…”

Section: Resultsmentioning

confidence: 99%

“…Amino acids that are regarded as having a negative effect on the binding ability are given values between )1 and )3. The 17 peptides with 15-mer amino acids used in this study were arbitrarily designed (their SYFPEITHI scores not shown, Supplementary Table 1), of which, P2, LSFLPSDFFP SVRDL (HBcAg [16][17][18][19][20][21][22][23][24][25][26][27][28][29][30] ) and P13, PPAYRPPNAPILSTL (HBcAg 129-143 ) had the highest SYFPEITHI scores, i.e., 20 and 28, for DRB1*0401 and DRB1*0101 molecules, respectively. They were used for the construction of each of MHC class II tetramers.…”

Section: Study Subjectsmentioning

confidence: 99%

“…Preparation of HLA-A2-HBcAg 18-27 tetrameric complexes HLA-A2-restricted epitope peptide HBcAg [18][19][20][21][22][23][24][25][26][27] FLPSDFFPSV, an immunodominant cytotoxic T lymphocyte (CTL) epitope on HBcAg, is currently the most widely used epitope for assaying CTL activities in HBV patients [2,[17][18][19][20][21]. We used HLA-A2-HBcAg 18-27 tetrameric complexes in this study to monitor CTL activities for the correlation with T reg f during AEs in HLA-A2 patients.…”

Section: Study Subjectsmentioning

confidence: 99%

“…The culture procedures using the 15-mer peptide P2 or P13 combined with recombinant HBcAg (rHBcAg) to stimulate LITs were carried out as described [20,22]. Generally, the CRI-p culture method gives 5-to 15-fold increase in total T reg cell numbers compared to that obtained directly from fresh LITs or PBMCs ex vivo [20,22].…”

Section: Study Subjectsmentioning

confidence: 99%

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HBcAg-specific CD4+CD25+regulatory T cells modulate immune tolerance and acute exacerbation on the natural history of chronic hepatitis B virus infection

et al. 2006

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Acute exacerbations (AEs) of chronic hepatitis B (CH-B) are accompanied by increased T cell responses to hepatitis B core and e antigens (HBcAg/HBeAg). Why patients are immunotolerant (IT) to the virus and why AEs occur spontaneously on the immunoactive phase remain unclear. The role of HBcAg-specific CD4(+)CD25(+) regulatory T (T(reg)) cells in AE and IT phases was investigated in this study. The SYFPEITHI scoring system was employed to predict MHC class II-restricted epitope peptides on HBcAg overlapping with HBeAg that were used for T(reg)-cell cloning and for the construction of MHC class II tetramers to measure T(reg) cell frequencies (T(reg) f). The results showed that HBcAg-specific T(reg) f declined during AE accompanied by increased HBcAg peptide-specific cytotoxic T lymphocyte frequencies. Predominant Foxp3-expressing T(reg) cell clones were generated from patients on the immune tolerance phase, while the majority of Th1 clones were obtained from patients on the immunoactive phase. T(reg) cells from liver and peripheral blood of CH-B patients express CD152 and PD1 antigens that exhibit suppression on PBMCs proliferation to HBcAg. These data suggest that HBcAg peptide-specific T(reg) cells modulate the IT phase, and that their decline may account for the spontaneous AEs on the natural history of chronic hepatitis B virus infection.

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Section: Resultsmentioning

confidence: 99%

Section: Study Subjectsmentioning

confidence: 99%

Section: Study Subjectsmentioning

confidence: 99%

Section: Study Subjectsmentioning

confidence: 99%

See 2 more Smart Citations

HBcAg-specific CD4+CD25+regulatory T cells modulate immune tolerance and acute exacerbation on the natural history of chronic hepatitis B virus infection

et al. 2006

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“…This difference from our study may suggest that our patients were predominately Genotype C, in contrast to the European study, which mainly involved those of Genotype A or D. Another possibility may be the presence of fewer substitutions in the rt region at commencement of therapy, either alone or with emergence of YMDD mutant, as discussed below. A recent report showed that sustained lamivudine responders with HLA-A2 elicited more potent cytotoxic Tlymphocyte (CTL) immunity against YMDD and its mutant (YIDD and YVDD) [Lin et al, 2005]. Although we do not have HLA type data for the patients in our study, anti-mutant CTLs such as those described above may contribute in suppressing the elevation of mutant virus loads.…”

Section: Discussionmentioning

confidence: 77%

Clinical and virological features of non-breakthrough and severe exacerbation due to lamivudine-resistant hepatitis B virus mutants

et al. 2006

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Patients who develop YMDD mutant during lamivudine therapy for hepatitis B virus (HBV) infection exhibit various clinical courses. Some patients show normal ALT levels, whereas others develop severe hepatitis exacerbations (SHEs) due to YMDD mutants. We studied 136 patients with YMDD mutant among 362 Japanese adult patients on lamivudine therapy. Clinical and virological features of patients without elevated HBV DNA after emergence of YMDD mutant (non-elevated group) were investigated. Moreover, virological analysis was also performed in patients with SHE due to YMDD mutants. Patients in the non-elevated group were characterized by HBeAg-negative pretreatment, HBeAg loss during therapy, a longer duration from commencement of therapy until emergence of YMDD mutant, and no mixed-type YMDD mutants. Patients with SHE had more substitutions in the reverse transcriptase (rt) region within the polymerase gene at the time of exacerbation than those without SHE, although no specific substitutions were noted. Sequence analysis of full-length HBV genome showed more substitutions in X, rt, and surface proteins in patients with SHE than in those without elevated HBV DNA level. In conclusion, negativity for HBeAg at commencement of therapy or before emergence of YMDD mutant was an important factor among non-elevated group. More substitutions in the rt region and the other proteins may be related to the emergence of severe hepatitis caused by lamivudine-resistant virus.

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Characteristics of lamivudine‐resistant hepatitis B virus (HBV) strains with and without breakthrough hepatitis in patients with chronic hepatitis B evaluated by serial HBV full‐genome sequences

Horiike

Dương

Michitaka

et al. 2007

Journal of Medical Virology

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Lamivudine therapy often causes breakthrough of hepatitis B virus (HBV) DNA and breakthrough hepatitis. The aim of this study was to determine the viral factors that relate to HBV-DNA breakthrough with and without breakthrough hepatitis. Among 82 patients with chronic hepatitis B (CHB) who received lamivudine at a dose of 100 mg daily for more than 24 months, 23 patients had HBV-DNA breakthrough induced by a lamivudine-resistant mutant. Of these 23 patients, 16 had breakthrough hepatitis and 7 had only HBV-DNA breakthrough. Serial HBV-DNA full-genome sequences during therapy were examined in 10 (7 had breakthrough hepatitis and 3 did not) of these 23 patients by direct sequencing. Mutations in the S region were examined by cloning in representative patients. There were no significant differences in the baseline clinical backgrounds and virus marker between patients with and without breakthrough hepatitis. The HBV amino acid substitutions at breakthrough hepatitis were identical to those at HBV-DNA breakthrough. Cloning analysis revealed that monoclonal mutational strain appeared at breakthrough and no such mutations existed at baseline. Regarding HBV amino acid substitutions in the polymerase region, S region, X region, and precore-core region with breakthrough compared to baseline, there was no significant differences of the numbers of amino acid substitution between breakthrough hepatitis and non-breakthrough hepatitis. There were no common amino acid changes in patients with breakthrough hepatitis. Although monoclonal lamivudine-resistant strain emerged at HBV-DNA breakthrough in patients with CHB, there were no common amino acid changes, suggesting viral factor may have insignificant role in breakthrough hepatitis.

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High frequency of functional anti-YMDD and -mutant cytotoxic T lymphocytes after in vitro expansion correlates with successful response to lamivudine therapy for chronic hepatitis B

Cited by 21 publications

References 52 publications

HBcAg-specific CD4+CD25+regulatory T cells modulate immune tolerance and acute exacerbation on the natural history of chronic hepatitis B virus infection

HBcAg-specific CD4+CD25+regulatory T cells modulate immune tolerance and acute exacerbation on the natural history of chronic hepatitis B virus infection

Clinical and virological features of non-breakthrough and severe exacerbation due to lamivudine-resistant hepatitis B virus mutants

Characteristics of lamivudine‐resistant hepatitis B virus (HBV) strains with and without breakthrough hepatitis in patients with chronic hepatitis B evaluated by serial HBV full‐genome sequences

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