Buy Thymulin Peptide (10mg)

Name: Thymulin Peptide (10mg)
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Thymulin Product Description (Thymalin Peptide)

Thymulin is a nonapeptide hormone (nine amino acids) originally isolated from thymus tissue, studied for its role in immune system regulation and T-cell differentiation mechanisms. This research-grade compound is supplied as lyophilized powder with high purity standards verified through advanced analytical testing.

The molecular structure (Pyr-Ala-Lys-Ser-Gln-Gly-Gly-Ser-Asn-OH) enables investigation of thymic factor activity in immune cell development and cellular signaling pathways. Each batch undergoes rigorous chemical characterization to ensure consistent quality for laboratory applications.

Manufactured in USA GMP facilities with comprehensive documentation. This peptide compound is intended exclusively for in vitro research investigating immune function mechanisms.

Peptide Information

Property	Value
Peptide Sequence	Pyr-Ala-Lys-Ser-Gln-Gly-Gly-Ser-Asn-OH
Molecular Formula	C33H54N12O15
Molecular Weight	858.86 g/mol
CAS Number	63958-90-7
PubChem CID	3085284
Synonyms	Thymulin, Thymalin, Thymic Factor, Facteur Thymique Serique, Serum Thymic Factor, Nonathymulin, STF

Thymulin Research Overview

Thymulin is a nonapeptide (pyro-Glu-Ala-Lys-Ser-Gln-Gly-Gly-Ser-Asn) originally identified as facteur thymique sérique (FTS).

Molecular Identity and Zinc Dependence

The peptide requires zinc binding in a 1:1 ratio to achieve cellular activity.

NMR studies confirmed that zinc binding induces a specific three-dimensional conformation required for receptor binding. Thymic epithelial cells secrete the peptide in its active zinc-containing form.^[1]

Zinc deficiency models show that reduced thymulin activity directly correlates with declines in T-cell subpopulations and lymphokine production. Zinc repletion consistently restores thymulin bioactivity in laboratory investigations.^[2]

Immune Modulation

T-Cell Differentiation and Th1/Th2 Balance

Thymulin influences both intrathymic and extrathymic T-cell differentiation through specific receptor binding on T-cell lines.

Gene expression studies in murine asthma models demonstrated thymulin’s ability to shift immune balance away from Th2 dominance:^[3]

Increased IFN-γ expression, stimulating Th1 cells
Reduced IL-13 secretion (Th2-associated mediator)
Decreased eotaxin (eosinophil chemotactic factor)
Lower eosinophil, neutrophil, and mononuclear cell infiltration in bronchoalveolar lavage fluid

Zinc deficiency investigations show that reduced thymulin activity impairs Th1 cell proliferation while leaving Th2 function intact, resulting in measurable Th1/Th2 imbalance.^[4]

Anti-Inflammatory Mechanisms

Cytokine and Mediator Downregulation

A thymulin peptide analogue (PAT) demonstrated anti-inflammatory activity in endotoxin-induced inflammation models, downregulating multiple proinflammatory mediators simultaneously.^[5]

Mediator	Effect of PAT	Model
TNF-α	Abolished elevation	Localized (i.pl. ET)
IL-1β	Reduced levels	Localized and systemic
IL-6	Reduced to control levels	Localized and systemic
NGF	Reduced levels	Localized (i.pl. ET)
PGE₂	Reduced to control levels	Systemic (i.p. ET)

Mechanistic data indicate PAT inhibits NF-κB nuclear translocation, the transcription factor governing proinflammatory cytokine and COX-2 gene expression.

Separate mouse models showed thymulin prevented overproduction of proinflammatory cytokines and heat shock protein Hsp70 through the NF-κB pathway.^[6]

Anti-Fibrotic Signaling

Thymulin gene expression in asthma models reduced airway remodeling markers:^[3]

Decreased TGF-β and VEGF expression
Reduced collagen fiber deposition in airways
Attenuated smooth muscle hypertrophy in terminal bronchioles
Prevented subepithelial fibrosis and mucous cell hyperplasia

Earlier work showed thymulin reduced bleomycin-induced cytokine production and inhibited pulmonary fibrosis. In monocrotaline-induced pulmonary hypertension, thymulin suppressed the proinflammatory p38 MAPK pathway.

Neurological Research

Analgesic Properties

PAT exhibited analgesic potency comparable to dexamethasone and indomethacin in reversing endotoxin-induced mechanical and thermal hyperalgesia, but at lower molar concentrations. It outperformed anti-IL-1β peptides by approximately 10x in molar terms.^[5]

PAT reversed both hyperalgesia and fever in systemic inflammation models. Effects are attributed to suppression of COX-2-dependent PGE₂ formation and peripheral cytokine cascades.

Neuroprotection

Intracerebroventricular administration studies demonstrated thymulin’s neuroprotective role in experimentally induced brain inflammation, reversing inflammatory hyperalgesia and modulating proinflammatory cytokine concentrations.^[7]

Adenoviral vectors carrying synthetic thymulin genes achieved longer transgene expression in rat brain regions compared to other reporter genes. The proposed mechanism involves thymulin’s local anti-inflammatory activity protecting virus-transduced brain cells from immune-mediated destruction.

Neuroendocrine Regulation

Hypophysiotropic Activity

Thymulin acts as a hypophysiotropic peptide, regulating pituitary hormone release in dispersed rat pituitary cell studies:^[7]

Luteinizing hormone (LH) and follicle-stimulating hormone (FSH) release
Growth hormone (GH) and prolactin (PRL) secretion
Thyrotropin (TSH) release
Adrenocorticotropic hormone (ACTH) secretion via cAMP and cGMP accumulation

Thymulin also modulates GnRH stimulatory activity on gonadotropin release and influences gonadotropin-induced ovarian and testicular steroidogenesis.

Bidirectional Regulation

Thymulin production is regulated by the neuroendocrine system in a bidirectional loop. Growth hormone stimulates thymulin release from thymic epithelial cells via GH receptors.

Prolactin receptors on thymic epithelial cells allow direct stimulation of thymulin synthesis. Thyroid hormones (T₃/T₄) stimulate thymulin secretion, while hypothyroidism depresses circulating levels.

Metabolic Research

Athymic mouse models develop spontaneous hyperglycemia, impaired glucose tolerance, and peripheral insulin insensitivity after approximately one month. These mice show increased somatostatin-producing D-cell populations and elevated pancreatic somatostatin content.^[7]

Neonatal thymulin gene therapy completely prevented adult-onset hyperglycemia in 70-day-old nude mice. Additional documented metabolic effects include:

Reduction of serum cholesterol levels
Increased LDL catabolism
Inhibition of hepatic HMG-CoA reductase activity
Partial normalization of hepatic phospholipid fatty acid composition

These findings indicate thymulin’s modulatory role in both glucose and lipid metabolism pathways.

Aging and Thymic Involution

Age-related thymus involution results in progressive decline of thymulin secretion, contributing to immunosenescence in aging organisms. Thymic involution has been linked to cellular senescence driven by oxidative stress.^[8]

Several neuroendocrine interventions demonstrated partial restoration of declining thymulin levels in aged animal models. Bovine GH treatment in aged dogs partially restored low serum thymulin levels.

Ovine GH in old mice increased circulating thymulin and enhanced thymocyte proliferation and IL-6 production. Combined GH and T₄ treatment partially restored thymulin levels in old rats.

Extrathymic Production Under Cellular Stress

Studies show that thymulin is not exclusively of thymic origin. When non-thymic cells (RAW 264.7 macrophages and L929 fibroblasts) were exposed to oxidative stress, heat shock, or apoptosis-inducing agents, extracellular thymulin was detected in culture media within 2 hours.^[6]

SPATS2L as Putative Precursor

Western blot analysis revealed two bands (~60 kDa and ~10 kDa) interpreted as potential precursor and intermediate product. SPATS2L (Spermatogenesis-Associated Serine-Rich 2-Like), an intranucleolar stress-response protein, was identified as containing a thymulin-like sequence.

Key observations supporting SPATS2L as a thymulin precursor:

Strong Pearson correlation (r = 0.925, p < 0.01) between SPATS2L and 60 kDa thymulin-stained band
SPATS2L migrates from nucleolus to stress granules under oxidative stress
The 10 kDa intermediate correlates with caspase-3 activation
The 60 kDa precursor correlates with NF-κB pathway activation

This extrathymic production pathway suggests thymulin may function as a stress-responsive signal from damaged cells to local immune cells, potentially explaining how thymulin-mediated immune regulation persists after age-related thymic involution.

Summary of Signaling Pathways

Pathway / Target	Effect of Thymulin	Study Context
NF-κB	Inhibits nuclear translocation	LPS inflammation models
p38 MAPK	Suppresses activation	Pulmonary hypertension
Th1/Th2 balance	Shifts toward Th1 (↑IFN-γ)	Asthma, zinc deficiency
COX-2 / PGE₂	Reduces PGE₂ production	Systemic inflammation
TGF-β / VEGF	Downregulates expression	Airway remodeling
cAMP / cGMP	Mediates ACTH stimulation	Pituitary cells
HMG-CoA reductase	Inhibits activity	Cholesterol metabolism

Research Use Only: This compound is intended exclusively for in vitro laboratory research. Not for human consumption or therapeutic use.

References

Dardenne M, Pléau JM, Nabarra B, Lefrancier P, Derrien M, Choay J, et al. Contribution of zinc and other metals to the biological activity of the serum thymic factor. Proceedings of the National Academy of Sciences; 1982. https://doi.org/10.1073/pnas.79.17.5370
Prasad AS, Meftah S, Abdallah J, Kaplan J, Brewer GJ, Bach JF, et al. Serum thymulin in human zinc deficiency. American Society for Clinical Investigation; 1988. https://doi.org/10.1172/jci113717
da Silva AL, Martini SV, Abreu SC, Samary C dos S, Diaz BL, Fernezlian S, et al. DNA nanoparticle-mediated thymulin gene therapy prevents airway remodeling in experimental allergic asthma. Elsevier BV; 2014. https://doi.org/10.1016/j.jconrel.2014.02.010
Prasad AS. Lessons Learned from Experimental Human Model of Zinc Deficiency. Wiley; 2020. https://doi.org/10.1155/2020/9207279
Safieh‐Garabedian B, Dardenne M, Pléau JM, Saadé NE. Potent analgesic and anti‐inflammatory actions of a novel thymulin‐related peptide in the rat. Wiley; 2002. https://doi.org/10.1038/sj.bjp.0704793
Lunin SM, Khrenov MO, Glushkova OV, Vinogradova EV, Yashin VA, Fesenko EE, et al. Extrathymic production of thymulin induced by oxidative stress, heat shock, apoptosis, or necrosis. SAGE Publications; 2017. https://doi.org/10.1177/0394632017694625
Reggiani PC, Morel GR, Cónsole GM, Barbeito CG, Rodriguez SS, Brown OA, et al. The Thymus–Neuroendocrine Axis. Wiley; 2009. https://doi.org/10.1111/j.1749-6632.2008.03964.x
Barbouti A, Vasileiou PVS, Evangelou K, Vlasis KG, Papoudou-Bai A, Gorgoulis VG, et al. Implications of Oxidative Stress and Cellular Senescence in Age-Related Thymus Involution. Wiley; 2020. https://doi.org/10.1155/2020/7986071

Thymulin (260632)

Thymulin (260632) ×

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