Product details

Regulatory note: PEG conjugate with variable architecture across suppliers. Confirm PEG molecular weight, attachment site, and PEG-to-peptide ratio per batch COA. Pharmacokinetic comparability across supplier sources cannot be assumed.

FAQ

Why is PEG architecture (MW and attachment chemistry) so critical for PEG-MGF?

The PEG component on PEG-MGF is not a passive shield, it actively determines the molecule's pharmacokinetics. PEG polymer MW affects hydrodynamic radius (which sets renal-clearance threshold) and the overall molecular weight, both of which set the in vivo half-life. PEG attachment chemistry (site-specific vs random) affects both the consistency of the product (random conjugation produces isomer mixtures) and the residual MGF biological activity (some attachment sites preserve activity better than others). Two PEG-MGF preparations from different suppliers can have the same nominal name but differ by 5-10× in functional half-life due to PEG-architecture differences, buyers must compare PEG MW, attachment site, and PEG-to-peptide ratio across suppliers, not just label.

When should I order PEG-MGF instead of unmodified MGF?

PEG-MGF is the right choice for in vivo research workflows where the very short native MGF half-life (minutes) would require impractical dosing frequency. The PEGylation extends functional half-life by 10-100× depending on the PEG architecture, supporting once-daily or less-frequent dosing protocols. Unmodified MGF is the right choice for cell-culture and biochemical-assay work where the dose is added directly to a defined system and stability across hours rather than days is sufficient. Many published cell-culture studies use unmodified MGF; published in vivo studies are split between PEG-MGF and similar long-acting analogs.

Certificate of Analysis (COA)