MGF (Mechano Growth Factor / IGF-1Ec splice variant)

MGF refers both to the IGF-1Ec splice variant produced by stretched muscle and to synthetic peptides corresponding to the unique E-domain region used in research and the peptide marketplace.

The mechano growth factor concept was developed primarily by Geoffrey Goldspink and colleagues, who showed that mechanical stretch of skeletal muscle induces alternative splicing of the IGF-1 gene to produce a splice variant (IGF-1Ec in humans) with a distinct E-domain. The hypothesis: this splice variant has a separate regenerative role in response to mechanical loading.^[1]

The Goldspink-group hypothesis is that the E-domain peptide acts on satellite cells (muscle stem cells) to promote their activation and proliferation in response to mechanical loading or injury, complementing the effects of mature IGF-1 itself.^[1]

Native MGF peptides are highly unstable in plasma. PEGylated MGF analogs (PEG-MGF) extend the half-life but remain investigational.

The peer-reviewed literature on MGF is summarized below across two tiers: human research (the highest standard), and preclinical / emerging research (animal models and early-stage human work).

This table summarizes commonly discussed claims and how the published evidence weighs in. The aim is clarity — supported claims, claims that look promising but need more data, and claims that outrun the science.

User communities describe subcutaneous and intramuscular use of synthetic MGF or PEG-MGF; no FDA-approved formulations exist.

The native MGF / IGF-1Ec biology is genuinely interesting — a clean illustration of tissue-specific alternative splicing in response to mechanical loading. Synthetic MGF peptide use is a different proposition: built on extrapolation from that biology, with limited controlled human evidence and significant marketplace heterogeneity. The two should not be conflated in evaluating claims.