Long-term outcomes of thymosin-alpha 1 and interferon alpha-2b combination therapy in patients with hepatitis B e antigen (HBeAg) negative chronic hepatitis B.
Saruc. Murat M; Ozden. Nuri N; Turkel. Nurten N; Ayhan. Semin S; Hock. Lynette M LM; Tuzcuoglu. Isil I; Yuceyar. Hakan H
Key Findings
- Thymosin‑alpha‑1 plus interferon‑alpha‑2b achieved a 74% sustained response after 78 weeks, higher than interferon alone (40%) or interferon + lamivudine (53%).
- At 12 months post‑treatment, 70% of the combination group maintained virologic and biochemical response versus 20%–27% in the other groups.
- The benefit persisted at 18 months post‑treatment, with 71% of the combination group still responding versus 10%–20% in comparators.
Practical Outcomes
- For people with chronic hepatitis B, adding thymosin‑alpha‑1 to interferon therapy may boost long‑term viral control. The regimen used 1.6 mg subcutaneously twice weekly alongside standard interferon dosing. However, interferon has notable side effects, so this approach is best considered under medical supervision rather than DIY use.
Summary
A study in chronic hepatitis B patients found that adding the peptide thymosin‑alpha‑1 (1.6 mg under the skin twice a week) to standard interferon‑alpha‑2b therapy gave better long‑term virus suppression and liver‑enzyme improvements than interferon alone or interferon with the antiviral drug lamivudine.
Abstract
Hepatitis B e antibody (HbeAb) and hepatitis B virus (HBV) DNA positive chronic hepatitis is a clinical entity, distinct from classical hepatitis B e antigen (HbeAg) positive chronic hepatitis B. Our aim was to evaluate the long-term therapeutic efficacy of the combination of interferon alpha-2b and thymosin-alpha1 compared with lamivudine plus interferon alpha-2b and interferon alpha-2b alone. Fifty-two patients with HbeAg-negative chronic hepatitis B were assigned to three different groups in a nonrandomized manner. Group 1 (n = 27) received thymosin-alpha1 [1.6 mg subcutaneously (sc), twice a week] and interferon alpha-2b (10 MIU sc, three times per week) for 26 weeks, subsequently followed by interferon alpha-2b monotherapy at the same dosage for an additional 26 weeks. Group 2 (n = 10) received interferon alpha-2b (10 MIU sc, three times per week) for 52 weeks. Group 3 (n = 15) received interferon alpha-2b (10 MIU sc, three times per week) and lamivudine [100 mg orally (po), q.d.] for 52 weeks, followed by continuous lamivudine (100 mg po, q.d.) therapy. By the end of 78 weeks, a sustained response (SR-6 mo) was seen in 74% (20/27) of the patients within Group 1. On the contrary, Groups 2 and 3 had sustained response rates of 40 (4/10) and 53.3% (8/15), respectively (p = 0.13). At the end of 12 months post-treatment in Group 1, a virological and biochemical response rate was seen in 70.3% of patients (19/27); in contrast, Groups 2 and 3 had response rates of 20 (2/10) and 26.6% (4/15), respectively (p = 0036). At the end of the 18-month post-treatment follow-up period, 71.4% (19/27) of patients in Group 1, 10% of patients in Group 2 (1/10), and 20% of patients in Group 3(3/15) preserved their sustained response (p = 0.0003). Interferon alpha-2b and thymosin-alpha1 combination therapy results in significant virological and biochemical response rates compared with standard therapeutic regimens and is well tolerated.
Study Information
pubmed
2003
10.1002/jps.10401