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Thymosin-alpha-1

Thymalfasin, Zadaxin, Thymosin α1

Quick Stats
Studies 759
Trials 63
Score 2
1999 pubmed

Thymosin-alpha1 stimulates maturation of CD34+ stem cells into CD3+4+ cells in an in vitro thymic epithelia organ coculture model.

Knutsen. A P AP; Freeman. J J JJ; Mueller. K R KR; Roodman. S T ST; Bouhasin. J D JD

Key Findings

  • Thymosin‑alpha1 increased the total number of mononuclear cells in the culture after 2‑4 weeks.
  • It raised the proportion of CD3+ T‑cells, especially single‑positive CD4+ cells, at 3‑4 weeks.
  • Thymosin‑alpha1 tended to increase IL‑7 production, a cytokine that supports thymocyte maturation.

Practical Outcomes

  • The result hints that thymosin‑alpha1 might help strengthen the immune system by promoting T‑cell growth, but because the work is only in vitro, there’s no clear dosage or safety guidance for human use. Biohackers could consider this as mechanistic support for immune‑focused experiments, but should wait for animal or clinical studies before applying it to themselves.

Summary

In a lab test, adding the peptide thymosin‑alpha1 to human stem cells grown with thymus tissue helped the cells multiply and turn into mature CD4+ T‑cells, which are important for immune function. The study was done entirely in a dish, so it doesn’t tell us how to use the peptide in people, but it shows the peptide can boost T‑cell development under these conditions.

Abstract

The effect of thymosin-alpha1 on thymopoiesis is largely unknown. Thymosin is found in the cortical and medullary thymic epithelia, as well as in nurse cells; thus, it is hypothesized that thymosin may affect both early and late stage of thymocyte maturation. In this study, the effect of thymosin-alpha1 on thymopoiesis was determined by coculturing in vitro CD34+ stem cells (SC) with allogeneic cultured thymic epithelia fragments (CTEF) for 1-4 weeks and analyzing T-cell maturation by flow cytometry. Thymosin-alpha1 significantly enhanced the cell number (e.g., proliferation) of mononuclear cells obtained at 2 and 4 weeks of the SC-CTEF cocultures (P < 0.01 and < 0.05, respectively). In particular, thymosin-alpha1 stimulated expression of CD3+ cells at 3 and 4 weeks (P < 0.05). The predominant subpopulation increased by thymosin stimulation was single positive mature CD4+ cells, which was confirmed to occur within the SC-CTEF thymic organ tissue by laser confocal immunofluorescence microscopy. Thymosin stimulation tended to enhance IL-7 synthesis, critical cytokine in the maturation of thymocytes. In summary, this is the first study to demonstrate that thymosin-alpha1 enhanced thymopoiesis of CD34+ stem cells in humans using an in vitro model of differentiation using stem cells and cultured thymic epithelial fragments cocultures. Furthermore, the thymosin significantly increased expression of CD3+4+ T cells.

Study Information

Provider

pubmed

Year

1999

DOI

10.1016/s0192-0561(98)00060-5