Ara-290vsLL-37

Ara-290 is an 11-amino-acid peptide designed to selectively activate the innate repair receptor (IRR), a heteromeric receptor complex composed of the erythropoietin receptor (EPOR) and the beta common receptor (CD131/βcR). This receptor is distinct from the classical homodimeric EPOR that mediates erythropoiesis, which is why Ara-290 can deliver tissue-protective effects without stimulating red blood cell production or the thrombotic risks associated with EPO.

The IRR is expressed on tissues subjected to metabolic stress, inflammation, or injury — including neurons, Schwann cells, cardiomyocytes, renal tubular cells, and endothelial cells. When Ara-290 activates the IRR, it triggers a cascade of protective signaling pathways: JAK2/STAT5 activation promotes anti-apoptotic gene expression (Bcl-2, Bcl-xL); PI3K/Akt signaling provides cell survival signals; NF-κB modulation shifts the inflammatory balance from pro-inflammatory to pro-resolution. The net effect is protection of viable cells from death, reduction of inflammation, and activation of repair processes.

Ara-290's most clinically advanced application is in peripheral neuropathy, particularly diabetic small fiber neuropathy. Schwann cells — the myelinating glial cells of the peripheral nervous system — express the IRR, and Ara-290 stimulates their survival and regenerative capacity. In clinical trials, subcutaneous Ara-290 administration improved corneal nerve fiber density (a measure of small fiber regeneration) and reduced neuropathic symptoms. Despite its extremely short plasma half-life (approximately 2 minutes), the tissue-protective effects persist for days because the cellular signaling cascades activated by IRR engagement have sustained downstream effects that outlast the peptide's presence in circulation.

LL-37 is the only cathelicidin-derived antimicrobial peptide in humans, cleaved from the precursor protein hCAP-18 by proteinase 3 in neutrophil granules. It functions as a critical component of the innate immune system's first line of defense, with both direct antimicrobial activity and sophisticated immunomodulatory signaling.

The direct antimicrobial mechanism relies on LL-37's amphipathic alpha-helical structure — one face is positively charged (cationic) while the other is hydrophobic. The cationic face electrostatically attracts the negatively charged phospholipid headgroups of bacterial membranes (which differ from mammalian membranes in their lipid composition and charge distribution). Once bound, the hydrophobic face inserts into the lipid bilayer, creating pores or disrupting membrane integrity through a 'carpet' or 'toroidal pore' mechanism. This physical membrane disruption kills bacteria, fungi, and enveloped viruses rapidly and is difficult for microbes to develop resistance against, unlike conventional antibiotics that target specific enzymes.

The immunomodulatory functions are equally important. LL-37 acts as a chemoattractant for neutrophils, monocytes, and T cells through formyl peptide receptor-like 1 (FPRL1) activation, recruiting immune cells to infection sites. It promotes macrophage phagocytosis and enhances the killing capacity of neutrophil extracellular traps (NETs). Critically, LL-37 neutralizes bacterial lipopolysaccharide (LPS/endotoxin), preventing the cytokine storm that leads to sepsis. It also stimulates angiogenesis through VEGF upregulation and promotes wound re-epithelialization by activating epidermal growth factor receptor (EGFR) transactivation. LL-37 production is upregulated by vitamin D (which is why vitamin D status affects innate immunity), and its expression is found in skin, airways, the gastrointestinal tract, and virtually all epithelial barrier tissues.