The Synthetic Compound SLU-PP-332

Overview

orb1819063

Of estrogen receptor-related receptors (ERRs), SLU-PP-332 represents a synthetic agonist. In cellular energy regulation, ERRs are involved as nuclear receptors, serving as molecular targets for this compound studied in preclinical research.

Estrogen-Related Receptors (ERRs)

ERR Function

As transcription factors, ERRs function as orphan nuclear receptors, regulating genes involved in cellular energy homeostasis. Endogenous estrogens are not bound despite structural homology with estrogen receptors (ERs).
Three isoforms exist:

  • ERRα (NR3B1)
  • ERRβ (NR3B2)
  • ERRγ (NR3B3)

    These regulate:
  • Glucose metabolism pathways
  • Fatty acid oxidation
  • Mitochondrial biogenesis
  • Oxidative phosphorylation
41401 2015 Article BFaps2014121 Fig1 HTML 1

Isoform Distribution

  • In skeletal muscle, liver, heart, and brown adipose tissue, ERRα is highly expressed
  • In cardiac and skeletal muscle tissue, ERRγ is abundant
  • For embryonic stem cell pluripotency, ERRβ is important

Laboratory Effects Observed

Mitochondrial Function

In skeletal muscle cell lines, mitochondrial respiration is stimulated by SLU-PP-332. Pyruvate dehydrogenase kinase 4 (Pdk4) expression, a key ERR target gene, is promoted.
Linked to ATP synthesis pathways, increased mitochondrial respiration in C2C12 myocytes is demonstrated by studies.

Muscle Fiber Composition

In murine skeletal muscle, oxidative fiber proportion is increased by SLU-PP-332 administration, as shown by experimental studies. With alterations in endurance capacity measurements, this adaptation has been correlated.

Tissue Distribution

Beyond skeletal muscle, in cardiac tissue (affecting mitochondrial biogenesis) and neural tissue (involving neuronal energy homeostasis), ERR activity may be influenced by SLU-PP-332.

Preclinical Research Data

Compared to controls, alterations in body composition were shown by mice treated with SLU-PP-332, despite identical food consumption patterns, as reported by Billon et al.
To various physiological parameters in animal models, whether SLU-PP-332’s metabolic effects might relate is examined by research.

References:

  • Billon, C., et al. (2023). Synthetic ERR agonist in exercise models. ACS Chem Biol, 18, 756-771.
  • Billon, C., et al. (2024). ERR agonist in laboratory studies. J Pharmacol Exp Ther, 388(2), 232-240.
  • Wang, X. X., et al. (2023). Receptor agonism in laboratory models. Am J Pathol, 193, 1969-1987.

NOTICE REGARDING RESEARCH MATERIALS: All content and materials available on this website are for informational purposes only. The compounds supplied by this entity are provided exclusively for controlled, in vitro scientific inquiry and laboratory use. These compounds are not formulated or sold as drugs, dietary supplements, or cosmetic products and are not intended for any clinical application in humans or animals. Any use outside of a laboratory research setting is strictly prohibited.

BOOST YOUR RESEARCH NOW
$25 OFF YOUR FIRST ORDER

ampetide

$25 Off

HAS BEEN APPLIED

TO YOUR FIRST ORDER

SHOP PEPTIDES NOW