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Thymosin-alpha-1

Thymalfasin, Zadaxin, Thymosin α1

Quick Stats
Studies 759
Trials 63
Score 1
2004 pubmed

Past, present, and future hepatitis C treatments.

Foster. Graham R GR

Key Findings

  • Standard interferon alone gives low cure rates for hepatitis C.
  • Adding ribavirin improves cure rates but causes more side effects.
  • Pegylated interferon is more effective and can be taken weekly, improving quality of life.
  • Thymosin‑alpha‑1 is mentioned as a potential immunomodulatory adjunct, but no efficacy or dosing data are provided.

Practical Outcomes

  • For biohackers, there is currently no actionable protocol for using thymosin‑alpha‑1 in hepatitis C or for general health optimization. The peptide remains experimental in this context, so any use would be off‑label and unsupported by solid evidence. Focus on well‑studied interventions rather than this unproven adjunct.

Summary

The abstract talks about how hepatitis C has been treated with interferon drugs, sometimes combined with ribavirin, and mentions newer versions like pegylated interferon that work better and are easier to take. It also says that a peptide called thymosin‑alpha‑1 (thymalfasin) is being studied as an extra immune‑boosting add‑on, but there are no details on how well it works or how to use it.

Abstract

Conventional interferon (IFN) alfa has been used for many years in the treatment of chronic hepatitis C. However, few patients achieve sustained virological responses with IFN. Combining IFN with ribavirin improves efficacy considerably, but at the expense of diminished tolerability attributable to ribavirin. Pegylated interferons have improved pharmacokinetic profiles, may be administered once weekly, and are more effective than IFN is alone or in combination with ribavirin. In addition to enhanced efficacy, pegylated interferon alfa-2a (40 kD) also improves health-related quality of life during therapy compared with IFN-based therapy. New adjuvant agents have the potential to further improve sustained response rates and tolerability; however, pegylated interferons will likely remain the backbone of therapy in the foreseeable future. Therapies under development and evaluation for patients with HCV infection include adjunctive use of the antiviral agent amantadine and the immunomodulatory agent thymalfasin. Novel small molecules include the ribavirin analogues, viramidine and levovirin, and BILN 2061, an inhibitor of HCV serine protease. Other therapeutic strategies that have reached the clinic include antisense oligonucleotides (ISIS 14803), nuclease-resistant ribozymes targeting HCV RNA (Heptazyme), human monoclonal antibodie, and human antibody fragments directed at HCV helicase.

Study Information

Provider

pubmed

Year

2004

Date

2004-05-01T00:00:00.000Z

DOI

10.1055/s-2004-832934

References

66