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Thymosin-alpha-1

Thymalfasin, Zadaxin, Thymosin α1

Quick Stats
Studies 759
Trials 63
2007 pubmed 6 citations

Solid-phase synthesis of a peptide derivative of thymosin alpha1 and initial studies on its (99m)Tc-radiolabelling.

Klimentzou. Persefoni P; Beck. Alexander A; Varvarigou. Alexandra A; Tsitsilonis. Ourania O; Voelter. Wolfgang W; Pirmettis. Ioannis I; Papadopoulos. Minas M; Livaniou. Evangelia E; Zikos. Christos C

Key Findings

  • A new thymosin‑alpha‑1 derivative was designed to include a chelating group for technetium‑99m.
  • The peptide was synthesized using solid‑phase methods with about 35% overall yield and >95% purity.
  • The derivative was successfully radiolabelled with technetium‑99m, representing the first reported Tc‑99m‑labelled thymosin‑alpha‑1.

Practical Outcomes

  • This study is primarily a technical tool for researchers to track the peptide in lab or animal experiments. It does not offer actionable protocols, dosage recommendations, or direct health benefits for biohackers or self‑experimenters.

Summary

Scientists created a modified version of the immune‑boosting peptide thymosin‑alpha‑1 that can be attached to a radioactive tag (technetium‑99m) for imaging studies. The work shows how to make and label the peptide, but it doesn’t provide any guidance on dosing, safety, or health benefits for everyday use.

Abstract

A derivative (1) of the immunopotentiating 28-peptide thymosin alpha1 has been especially designed, so that it can be (99m)Tc-radiolabelled, and synthesized following the Fmoc solid-phase peptide synthesis approach. Derivative 1 contains the N-terminal fragment Talpha1[1-14] as a bioactive segment, at the C-terminus of which a (99m)Tc-chelating moiety consisting of N(alpha),N(alpha)-dimethylglycine, serine and cysteine is linked through the N(epsilon)-amino group of a 'bifunctional' lysine residue; the latter is indirectly anchored on the solid-phase peptide synthesis resin through 6-aminocaproic acid (dmGSCK{N(epsilon)-Talpha1[1-14]}Aca). Synthetic derivative 1 was obtained at high overall yield (approximately 35%) and purity (>95%) and shown to be efficiently radiolabelled with (99m)Tc, thus resulting in the first, to our knowledge, so far reported (99m)Tc-radiolabelled derivative of thymosin alpha1, which may be eventually used as a specific molecular tool for the in vitro/in vivo study of the mode of action of the parent bioactive peptide.

Study Information

Provider

pubmed

Year

2007

Date

2007-07-01T00:00:00.000Z

DOI

10.1111/j.1747-0285.2007.00529.x

Citations

6

References

36