HGH 191AAvsThymulin

Human Growth Hormone is a 191-amino-acid single-chain polypeptide secreted by somatotroph cells of the anterior pituitary gland. It exerts its effects through two distinct pathways: direct action via GH receptors and indirect action through insulin-like growth factor 1 (IGF-1). When HGH binds to the GH receptor (a type I cytokine receptor), it induces receptor dimerization and activates the JAK2/STAT5 signaling cascade, which directly stimulates gene transcription for protein synthesis, cell proliferation, and lipolysis.

The indirect pathway is equally important. GH receptor activation in hepatocytes stimulates the production and secretion of IGF-1, a 70-amino-acid peptide that circulates bound to IGF binding proteins (primarily IGFBP-3 and the acid-labile subunit). Circulating IGF-1 acts on virtually every tissue in the body — promoting amino acid uptake and protein synthesis in skeletal muscle, stimulating chondrocyte proliferation in growth plates, enhancing osteoblast activity for bone formation, and supporting neuronal survival and myelination.

GH also has profound effects on metabolism independent of IGF-1. It directly stimulates lipolysis in adipocytes by activating hormone-sensitive lipase, mobilizing stored fat as free fatty acids for energy. It antagonizes insulin action in peripheral tissues (hence the diabetogenic risk), shifting the body's fuel preference from glucose to fatty acids. In muscle, GH promotes nitrogen retention and positive protein balance. The pulsatile pattern of natural GH secretion — with the largest pulse during deep sleep — is important for its physiological effects, which is why exogenous GH protocols often try to mimic this pattern.

Thymulin (also known as facteur thymique sérique, FTS) is a nonapeptide (Glu-Ala-Lys-Ser-Gln-Gly-Gly-Ser-Asn) that is unique among thymic hormones in requiring a zinc ion for biological activity. The zinc ion is coordinated by the asparagine (position 9), serine (position 4), and the N-terminal glutamic acid, creating a metallopeptide complex where the zinc is essential for the correct three-dimensional conformation needed for receptor binding. Without zinc, thymulin is biologically inactive — this zinc dependency has important implications for immune function in zinc-deficient individuals.

Thymulin is produced exclusively by thymic epithelial cells and is the only thymic hormone that is truly thymus-specific — its serum levels become undetectable after thymectomy (surgical thymus removal). It binds to high-affinity receptors on T-cell precursors (thymocytes) and mature T cells, promoting several key aspects of T-cell biology. It induces the expression of T-cell differentiation markers (CD2, CD3, CD4, CD8), driving immature thymocytes through the stages of T-cell maturation. It enhances the cytotoxic function of CD8+ T cells and the helper function of CD4+ T cells. It modulates the balance between T-helper and T-suppressor (regulatory) cell populations, promoting appropriate immune regulation.

Thymulin also modulates cytokine production — it promotes IL-2 secretion (essential for T-cell proliferation and the generation of effector T cells), enhances IFN-γ production (important for Th1 cellular immunity), and influences the balance of pro-inflammatory versus anti-inflammatory cytokines. Serum thymulin levels peak around puberty and decline progressively with age, becoming virtually undetectable by age 60 — mirroring the age-related involution of the thymus gland. This decline correlates closely with immunosenescence markers: reduced naive T-cell output, skewed CD4/CD8 ratios, impaired vaccine responses, and increased susceptibility to infections and cancer. Zinc supplementation alone can partially restore thymulin activity in zinc-deficient elderly individuals, highlighting the clinical importance of the zinc-thymulin interaction.