Research Comparison

ARA-290 vs KPV

In Short

ARA-290 is erythropoietin-derived 11-amino-acid peptide; selective innate repair receptor (epor/cd131 beta-common heteromer) agonist; non-erythropoietic tissue-protective peptide; KPV is tripeptide; c-terminal fragment of alpha-melanocyte-stimulating hormone (alpha-msh); anti-inflammatory melanocortin-derived peptide. Both are supplied as lyophilized powders for laboratory and in-vitro research use only. The table below compares their molecular data, half-life and research focus side by side.

	ARA-290	KPV
Classification	Erythropoietin-derived 11-amino-acid peptide; selective innate repair receptor (EPOR/CD131 beta-common heteromer) agonist; non-erythropoietic tissue-protective peptide	Tripeptide; C-terminal fragment of alpha-melanocyte-stimulating hormone (alpha-MSH); anti-inflammatory melanocortin-derived peptide
Molecular formula	C45H68N12O15	C17H32N6O4
Molecular weight	1009.1 g/mol	384.48 g/mol
CAS number	1208243-50-8	112965-21-6
Research half-life	Short; minutes-range plasma half-life reported for the parent non-erythropoietic EPO-derived peptides - not precisely characterized for ARA-290 in the public literature	Not well characterized in the published literature
Primary research focus	Innate repair receptor signaling research	Intestinal inflammation and IBD models
Form	Lyophilized powder	Lyophilized powder
Price from	$36.99	$49.97

ARA-290

ARA-290, also known as cibinetide, is a small peptide derived from the structure of erythropoietin that selectively engages the innate repair receptor (a heteromer of the EPO receptor and the CD131 beta-common receptor) without stimulating erythropoiesis. Research has explored its role in modulating inflammatory cascades, supporting neuronal and vascular tissue under stress, and influencing pain pathways associated with small-fiber neuropathy. Because it does not raise hematocrit, it has been investigated as a tool for studying tissue-protective EPO signaling in isolation. This compound is supplied as a lyophilized powder for in-vitro and laboratory research use only and is not intended for human or veterinary use.

Full ARA-290 research guide

KPV

KPV (Lysine-Proline-Valine) is a C-terminal tripeptide fragment of alpha-melanocyte-stimulating hormone (alpha-MSH), specifically positions 11-13. Despite being only three amino acids, KPV retains the potent anti-inflammatory activity of the full-length hormone while lacking melanotropic and steroidogenic effects. KPV suppresses inflammation by inhibiting NF-kB nuclear translocation and reducing pro-inflammatory cytokine production, including IL-1beta, IL-6, and TNF-alpha. It enters cells and interacts directly with inflammatory signaling cascades independently of melanocortin receptors. Research published in the Journal of Biological Chemistry by Brzoska et al. demonstrated that KPV inhibited NF-kB activation in human intestinal epithelial cells, reducing inflammatory gene expression by 60-80% at micromolar concentrations. Studies in murine colitis models published in Inflammatory Bowel Diseases showed that oral and intracolonic KPV use significantly reduced disease activity index scores, colonic inflammation, and histological damage. Dalmasso et al. (2008) in PLoS ONE confirmed that KPV-loaded nanoparticles effectively targeted inflamed colonic tissue and accelerated mucosal healing. Compared to full-length alpha-MSH, KPV offers the advantage of anti-inflammatory activity without pigmentation effects or hormonal side effects. Unlike conventional anti-inflammatory agents such as corticosteroids or NSAIDs, KPV targets intracellular NF-kB signaling rather than cyclooxygenase or glucocorticoid receptor pathways, representing a mechanistically distinct approach to inflammation modulation. Store lyophilized KPV at -20°C. Reconstitute with bacteriostatic water and refrigerate at 2-8°C, using within 4 weeks. KPV is researched by gastroenterologists studying inflammatory bowel disease, dermatologists investigating anti-inflammatory skin treatments, and immunologists examining NF-kB-dependent inflammatory pathways.

Full KPV research guide

Frequently Asked Questions

What is the main difference between ARA-290 and KPV?

ARA-290 is classified as erythropoietin-derived 11-amino-acid peptide; selective innate repair receptor (epor/cd131 beta-common heteromer) agonist; non-erythropoietic tissue-protective peptide, while KPV is tripeptide; c-terminal fragment of alpha-melanocyte-stimulating hormone (alpha-msh); anti-inflammatory melanocortin-derived peptide. They are distinct research compounds with different mechanisms — the comparison table above sets out the molecular and pharmacokinetic differences side by side.

Can ARA-290 and KPV be studied together?

Some research protocols evaluate related peptides in combination, and research blends exist. Combination study design depends entirely on the research question and model. Both compounds are supplied for laboratory and in-vitro research use only — not for human use.

Are ARA-290 and KPV legal to buy for research?

Both are sold in the United States as research chemicals for laboratory and in-vitro use only. Neither is FDA-approved for human use. Researchers are responsible for compliance with all applicable regulations.

Buy ARA-290

From $36.99 — ≥98% HPLC, COA included.

Buy KPV

From $49.97 — ≥98% HPLC, COA included.

Research Use Only. This comparison summarizes published research. It is not medical advice. Neither compound is for human consumption or FDA-approved.