Cat #: 25-336

PeptiGrowth PG-008-10 Wnt3a Alternative Peptide, beta-catenin Pathway Agonist, 10 µg/vial

Cat #: 25-336

PeptiGrowth PG-008-10 Wnt3a Alternative Peptide, beta-catenin Pathway Agonist, 10 µg/vial


beta-catenin Pathway Agonist

10 µg/vial

Brand: PeptiGrowth

  • Totally synthetic, cyclic peptide containing non-natural amino acids
  • More stable than conventional growth factors
  • Animal-component free
  • Superior activity compared to recombinant Wnt3a in the TCF/LEF reporter assay, achieving the same level of activation at 1/70th mass concentration.
  • 1 nM of PG-008 has the same level of efficiency as 3 µM of CHIR99021 in differentiation of iPSCs into definitive endoderm
  • Work extracellularly unlike CHIR99021 and exhibit no cytotoxicity up to 10 uM, which is the highest concentration tested

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beta-catenin Pathway Agonist

10 µg/vial

Brand: PeptiGrowth

  • Totally synthetic, cyclic peptide containing non-natural amino acids
  • More stable than conventional growth factors
  • Animal-component free
  • Superior activity compared to recombinant Wnt3a in the TCF/LEF reporter assay, achieving the same level of activation at 1/70th mass concentration.
  • 1 nM of PG-008 has the same level of efficiency as 3 µM of CHIR99021 in differentiation of iPSCs into definitive endoderm
  • Work extracellularly unlike CHIR99021 and exhibit no cytotoxicity up to 10 uM, which is the highest concentration tested

PG-008, a fully chemically synthesized peptide, comprises a heterodimer of two cyclic peptides with selective binding affinity for Frizzled and LRP5/6. Unlike Wnt3a, PG-008 lacks lipid moieties, making it highly soluble and eliminating handling difficulties. It exhibits superior activity to Wnt3a in the agonistic activation of ?-catenin pathway.

During the differentiation of iPSCs into definitive endoderm, PG-008 was compared with CHIR99021 and recombinant Wnt3a in terms of differentiation induction efficiency. The results showed that when recombinant Wnt3a (50 ng/mL: approximately 1.3 nM) was used, the efficiency reached around 60%. In contrast, when PG-008 or CHIR99021 was used, the efficiency exceeded 98%. Notably, 1 nM of PG-008 exhibited a differentiation induction efficiency equivalent to that achieved with 3 µM of CHIR99021. PG-008 demonstrated no cytotoxicity up to 10 µM, the highest concentration tested, making it a safer alternative to CHIR99021.

Molecular weight 5099.63 (acetate)
Purity >95%
Storage Temp. -20°C

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