| Literature DB >> 26115521 |
Quan Yuan1, Liu-Wei Song1, Daniela Cavallone2, Francesco Moriconi2, Beatrice Cherubini2, Piero Colombatto2, Filippo Oliveri2, Barbara Agata Coco2, Gabriele Ricco2, Ferruccio Bonino3, James Wai Kuo Shih1, Ning-Shao Xia1, Maurizia Rossana Brunetto2.
Abstract
Non invasive immunologic markers of virus-induced liver disease are unmet needs. We tested the clinical significance of quantitative total and IgM-anti-HBc in well characterized chronic-HBsAg-carriers. Sera (212) were obtained from 111 HBsAg-carriers followed-up for 52 months (28-216) during different phases of chronic-HBV-genotype-D-infection: 10 HBeAg-positive, 25 inactive-carriers (HBV-DNA≤2000IU/ml, ALT<30U/L), 66 HBeAg-negative-CHB-patients and 10 with HDV-super-infection. In 35 patients treated with Peg-IFN±nucleos(t)ide-analogues (NUCs) sera were obtained at baseline, end-of-therapy and week-24-off-therapy and in 22 treated with NUCs (for 60 months, 42-134m) at baseline and end-of-follow-up. HBsAg and IgM-anti-HBc were measured by Architect-assays (Abbott, USA); total-anti-HBc by double-antigen-sandwich-immune-assay (Wantai, China); HBV-DNA by COBAS-TaqMan (Roche, Germany). Total-anti-HBc were detectable in all sera with lower levels in HBsAg-carriers without CHB (immune-tolerant, inactive and HDV-superinfected, median 3.26, range 2.26-4.49 Log10 IU/ml) versus untreated-CHB (median 4.68, range 2.76-5.54 Log10 IU/ml), p<0.0001. IgM-anti-HBc positive using the chronic-hepatitis-cut-off" (0.130-S/CO) were positive in 102 of 212 sera (48.1%). Overall total-anti-HBc and IgM-anti-HBc correlated significantly (p<0.001, r=0.417). Total-anti-HBc declined significantly in CHB patients with response to Peg-IFN (p<0.001) and in NUC-treated patients (p<0.001); the lowest levels (median 2.68, range 2.12-3.08 Log10 IU/ml) were found in long-term responders who cleared HBsAg subsequently. During spontaneous and therapy-induced fluctuations of CHB (remissions and reactivations) total- and IgM-anti-HBc correlated with ALT (p<0.001, r=0.351 and p=0.008, r=0.185 respectively). Total-anti-HBc qualifies as a useful marker of HBV-induced-liver-disease that might help to discriminate major phases of chronic HBV infection and to predict sustained response to antivirals.Entities:
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Year: 2015 PMID: 26115521 PMCID: PMC4482637 DOI: 10.1371/journal.pone.0130209
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Characteristics of HBsAg Carriers.
| HBsAgCarriers | N.ofcases | N.ofsera | Age median(range) | Male/Female | ALTU/Lmedian(range) | HBsAgLog10 IU/mlmedian(range) | HBV-DNALog10 IU/mlmedian(range) |
|---|---|---|---|---|---|---|---|
| A: HBeAg-positive | 10 | 10 | 38.92(21.45–71.04) | 8/2 | 77.5(26–346) | 4.99(3.71–5.46) | 7.83(0–8.26) |
| B: HBeAg-negative, inactive | 25 | 25 | 53.78(31.15–79.41) | 17/8 | 18.0(10–60) | 1.72(-1.7–3.22) | 1.82(0–3.21) |
| C: HBeAg-negative, with HDV superinfection | 10 | 10 | 34.03(13.65–59.86) | 9/1 | 104.5(70–207) | 4.17(4.07–4.53) | 1.58(0–1.98) |
| D: HBeAg-negative, chronic hepatitis B | 66 | 167 | 54.18(32.62–83.52) | 45/21 | 73.0(7–1243) | 3.51(-0.38–4.7) | 5.08(0–8.13) |
A) 10 HBeAg-positive HBsAg-carriers: 9 HBeAg-positive-CHB patients and 1 in the "immune tolerance" phase;
B) 25 inactive-carriers [IC, HBV-DNA levels persistently ≤ 2000 IU/ml and normal ALT (<30 U/L)];
C) 10 HBeAg-negative/anti-HBe positive/anti-HDV-positive carriers with chronic-Delta-hepatitis (CDH);
D) 66 active carriers, HBeAg-negative/anti-HBe-positive CHB with fluctuating HBV-DNA above 20000 IU/mL and elevated ALT.
Fig 1Box Plot analysis.
Serum levels of total-anti-HBc (a) and anti-HBc-IgM (b) in 4 groups: a) inactive HBsAg-carriers; b) untreated HBeAg-negative-CHB patients, baseline; c) HBeAg-negative-CHB patients with SVR to Peg-IFN±NUC (EOF); d) NUC-treated patients (EOF). The distribution of total-anti-HBc levels falls within the dynamic range of quantification of the assay in all the patients. On the contrary, this holds true for 52% only of the sera, even using the lower CHB cut-off of 0.130 S/CO.
Fig 2Receiver operating characteristic (ROC) curve analyses.
Total-anti-HBc (full line) and anti-HBc-IgM (dotted line). A. AUROCs of total-anti-HBc and IgM-anti-HBc to identify IC from CHB were 0.947 (95% CI 0.86–0.97, p<0.0001) and 0.915 (95% CI 0.91–0.99, p<0.0001) respectively. B. AUROCs of total-anti-HBc and IgM-anti-HBc to identify HBeAg-negative-CHB with SVR from untreated HBeAg-negative-CHB were 0.928 (95% CI 0.89–0.97, p<0.0001) and 0.871 (95% CI 0.81–0.93, p<0.0001). The discriminative capacity of the 2 assays was comparable, even if total-anti-HBc performed better than IgM-anti-HBc (p = 0.212 and p = 0.062 for ROC analysis a and b respectively). We identified 2 cut-off-values for total-anti-HBc: the former (12489IU/ml) to distinguish IC from HBeAg-negative-CHB with 81.8%-sensitivity, 94.4%-specificity, 76.1%-PPV, 96.4%-NPVs and 87.3%-DA, the latter (10804IU/ml) to distinguish HBeAg-negative-CHB with SVR from untreated patients with 83.3%-sensitivity, 88.6%-specificity,84.9%-PPV, 87.3%-NPV and 86.0%-DA.
Fig 3Kinetics of HBV markers in patients treated with Peg-IFN.
Kinetics of median values of HBV markers between baseline (BL), end of therapy (EOT) and end of follow-up (EOF) in 35 patients treated with Peg-IFN: 6 NR, 10 REL and 19 SVR. Patients who did not respond to IFN (NR and REL) were subsequently switched to NUC. P values: a) HBsAg: BL vs EOT 0.27 for NR, 0.50 for REL and <0.001 for SVR; b) HBV-DNA: BL vs EOT 0.59 for NR, 0.014 for REL and <0.001 for SVR; c) Anti-HBc-IgM: BL vs EOT 0.24 for NR, 0.01 for REL and 0.17 for SVR; d) Total Anti-HBc: BL vs EOT 0.39 for NR, <0.001 for REL and <0.001 for SVR.
Fig 4Kinetics of ALT and HBV markers between between remission and reactivation phases of CHB.
A. untreated HBeAg-negative CHB patients at spontaneous disease remissions and flare-ups (5 cases): total-anti-HBc mean 4.23, median 4.56, and mean 4.88, median 4.93-Log10IU/ml, p = 0.054; IgM-anti-HBc mean 0.24, median 0.25, and mean 1.35, median 1.0S/CO, p = 0.054; HBV-DNA mean 3.78, median 3.76, and mean 5.86, median 5.89-Log10IU/ml, p = 0.058; HBsAg mean 3.18, median 3.4, and mean 3.21, median 3.52-Log10IU/ml, p = 0.91and ALT mean 23, median 23, and mean 244.6, median 201UI/L, p = 0.046. B. CHB patients treated with PEG-IFN (REL) at the time of temporary disease remission during therapy and hepatitis reactivation after relapse (9 cases): total-anti-HBc mean 4.04, median 4.01, and mean 4.79, median-4.93-Log10IU/ml, p = 0.002; IgM-anti-HBc mean 0.39, median 0.14, and mean 1.16, median 0.81S/CO, p = 0.03; HBV-DNA mean 3.34, median 1.74, and mean 7.18, median 7.27-Log10IU/ml, p = 0.004; HBsAg mean 3.61, median 3.54, and mean 3.55, median 3.65-Log10IU/ml, p = 0.73 and ALT mean 43, median 29, and mean 413, median 311 UI/L, p = 0.007.