SLU-PP-332vsTB-500

SLU-PP-332 is a small molecule agonist of estrogen-related receptor alpha (ERRα), one of three orphan nuclear receptors in the ERR family. Despite its name, ERRα does not bind estrogen — it was named for its structural similarity to estrogen receptors. ERRα is constitutively active and functions as a master transcription factor for genes controlling mitochondrial biogenesis, oxidative phosphorylation, and fatty acid oxidation, particularly in metabolically active tissues like skeletal muscle, heart, and brown adipose tissue.

SLU-PP-332 enhances ERRα transcriptional activity by stabilizing its active conformation and promoting coactivator recruitment (particularly PGC-1α, which is both an ERRα target gene and an ERRα coactivator, creating a positive feed-forward loop). Activated ERRα binds to ERR response elements (ERREs) in the promoter regions of hundreds of metabolic genes, upregulating the entire oxidative metabolism gene program: mitochondrial electron transport chain subunits, fatty acid oxidation enzymes, TCA cycle enzymes, and mitochondrial transcription and replication factors.

The most striking effect in preclinical studies is the transformation of skeletal muscle fiber type composition. SLU-PP-332 treatment increases the proportion of slow-twitch (type I) and oxidative fast-twitch (type IIA) fibers while decreasing glycolytic fast-twitch (type IIB/IIX) fibers. Type I fibers are rich in mitochondria, capillaries, and myoglobin — they are the fibers that endurance athletes develop through years of training. By pharmacologically shifting this fiber type ratio, SLU-PP-332 produces endurance capacity gains similar to what would require months of aerobic training. In mouse studies published in 2023, treated animals ran significantly longer and farther on treadmill tests. This ERRα-mediated mechanism is distinct from and potentially complementary to AMPK-based exercise mimetics like AICAR, as it targets a different node in the mitochondrial biogenesis regulatory network.

TB-500 is the active fragment of Thymosin Beta-4 (Tβ4), a 43-amino-acid peptide present in virtually every nucleated cell in the body. Its central molecular function is the sequestration of G-actin monomers — the globular, unpolymerized form of actin. By binding G-actin at a 1:1 ratio, TB-500 maintains a reservoir of monomeric actin that can be rapidly mobilized for polymerization into F-actin filaments when cells need to migrate, change shape, or form new structures during tissue repair.

This actin-regulating role is fundamental to TB-500's healing effects. When tissue is damaged, cells at the wound margin must migrate into the injury site. Cell migration requires dynamic actin polymerization at the leading edge of the cell (forming lamellipodia and filopodia) and depolymerization at the trailing edge. TB-500 facilitates this process by providing a controlled supply of G-actin monomers. It promotes migration of keratinocytes (for skin wound closure), endothelial cells (for new blood vessel formation), and cardiac progenitor cells (for heart repair).

Beyond actin regulation, TB-500 has significant anti-inflammatory and gene-regulatory effects. It downregulates pro-inflammatory cytokines including IL-1β, IL-6, and TNF-α while upregulating anti-inflammatory mediators. It activates cell survival pathways, specifically Akt-mediated anti-apoptotic signaling, protecting damaged cells from programmed cell death. TB-500 also promotes angiogenesis by stimulating endothelial progenitor cell differentiation and new capillary formation. In cardiac tissue, it has demonstrated the ability to activate epicardial progenitor cells and promote cardiomyocyte survival following ischemic injury. The combination of cell migration, anti-inflammation, angiogenesis, and cell survival makes TB-500 one of the most broad-spectrum healing peptides available.