FOXO4-DRIvsIGF-1

FOXO4-DRI is a D-retro-inverso (DRI) peptide — a peptide composed entirely of D-amino acids (mirror image of natural L-amino acids) assembled in reverse sequence order. This DRI modification makes the peptide virtually invisible to cellular proteases (which have evolved to cleave L-amino acid peptide bonds), dramatically extending its biological half-life while preserving the spatial orientation of key amino acid side chains needed for target interaction.

The target is the FOXO4-p53 protein-protein interaction that keeps senescent cells alive. Cellular senescence is a state of permanent cell cycle arrest triggered by DNA damage, oncogene activation, or telomere shortening. Senescent cells would normally undergo p53-mediated apoptosis (programmed cell death), but they evade this fate through a survival mechanism: the transcription factor FOXO4 is selectively upregulated in senescent cells and physically binds to p53, sequestering it in PML (promyelocytic leukemia) nuclear bodies. This binding prevents p53 from activating its pro-apoptotic transcriptional program (PUMA, BAX, NOXA), keeping the damaged cell alive.

FOXO4-DRI competitively disrupts this interaction by mimicking the FOXO4 binding interface for p53 but without the nuclear body-localizing function. When FOXO4-DRI competes p53 away from endogenous FOXO4, liberated p53 can access its apoptotic target genes, triggering mitochondrial outer membrane permeabilization and caspase activation — selectively killing the senescent cell. Crucially, non-senescent cells do not depend on FOXO4-p53 interaction for survival (they have intact cell cycle regulation and don't upregulate FOXO4), so they are unaffected by FOXO4-DRI. This selectivity — killing only 'zombie' senescent cells while sparing healthy cells — makes FOXO4-DRI a true senolytic agent. In the original 2017 Cell publication by de Keizer et al., FOXO4-DRI treatment in aged mice reduced senescent cell burden and restored physical fitness, fur density, and renal function.

IGF-1 (Insulin-like Growth Factor 1) is a 70-amino-acid peptide hormone with approximately 50% structural homology to proinsulin. It is primarily produced by hepatocytes in response to growth hormone stimulation, though virtually all tissues produce IGF-1 locally for paracrine/autocrine signaling. Circulating IGF-1 is bound to six IGF binding proteins (IGFBP-1 through IGFBP-6), with approximately 80-90% bound to IGFBP-3 in a ternary complex with the acid-labile subunit (ALS). Only free, unbound IGF-1 (approximately 1-2% of total) can activate receptors.

IGF-1 binds to the IGF-1 receptor (IGF-1R), a heterotetrameric receptor tyrosine kinase structurally similar to the insulin receptor. Ligand binding triggers receptor autophosphorylation and recruitment of insulin receptor substrate (IRS) adaptor proteins, activating two major downstream cascades. The PI3K/Akt/mTOR pathway drives protein synthesis (through mTORC1 activation of S6K1 and inhibition of 4E-BP1), cell survival (through BAD phosphorylation and Bcl-2 family regulation), and glucose uptake (through GLUT4 translocation). The Ras/Raf/MEK/ERK pathway promotes cell proliferation, differentiation, and gene expression changes required for tissue growth.

In skeletal muscle, IGF-1's effects include both hypertrophy (enlargement of existing muscle fibers through increased protein synthesis) and hyperplasia (generation of new muscle cells through satellite cell activation and differentiation). Local muscle-derived IGF-1 isoforms (including the MGF splice variant) play a particularly important role in exercise-induced muscle adaptation. The very short half-life of free IGF-1 (10-20 minutes) means that therapeutic administration requires frequent dosing or modified forms (such as IGF-1 LR3 with its extended half-life). Native IGF-1 also binds the insulin receptor (with lower affinity), which contributes to its hypoglycemic effects — a significant clinical risk that requires careful glucose monitoring and administration with food.