Newly developed oral bioavailable EHMT2 inhibitor as a potential epigenetic therapy for Prader-Willi syndrome

Mol Ther. 2024 Aug 7;32(8):2662-2675. doi: 10.1016/j.ymthe.2024.05.034. Epub 2024 May 24.

Abstract

Prader-Willi syndrome (PWS) is the prototypic genomic disorder resulting from deficiency of paternally expressed genes in the human chromosome 15q11-q13 region. The unique molecular mechanism involving epigenetic modifications renders PWS as the most attractive candidate to explore a proof-of-concept of epigenetic therapy in humans. The premise is that epigenetic modulations could reactivate the repressed PWS candidate genes from the maternal chromosome and offer therapeutic benefit. Our prior study identifies an EHMT2/G9a inhibitor, UNC0642, that reactivates the expression of PWS genes via reduction of H3K9me2. However, low brain permeability and poor oral bioavailability of UNC0642 preclude its advancement into translational studies in humans. In this study, a newly developed inhibitor, MS152, modified from the structure of UNC0642, has better brain penetration and greater potency and selectivity against EHMT2/G9a. MS152 reactivated maternally silenced PWS genes in PWS patient fibroblasts and in brain and liver tissues of PWS mouse models. Importantly, the molecular efficacy of oral administration is comparable with the intraperitoneal route. MS152 treatment in newborns ameliorates the perinatal lethality and poor growth, maintaining reactivation in a PWS mouse model at postnatal 90 days. Our findings provide strong support for MS152 as a first-in-class inhibitor to advance the epigenetic therapy of PWS in humans.

Keywords: EHMT2; H3K9 methyl transferase; H3K9me1/2; Histone modification; Prader-willi syndrome; Snord116; Snrpn; epigenetic therapy; imrpinting disorder; pharmacological intervention.

MeSH terms

  • Administration, Oral
  • Animals
  • Brain / drug effects
  • Brain / metabolism
  • Disease Models, Animal*
  • Epigenesis, Genetic* / drug effects
  • Histocompatibility Antigens / genetics
  • Histocompatibility Antigens / metabolism
  • Histone-Lysine N-Methyltransferase
  • Humans
  • Mice
  • Prader-Willi Syndrome* / drug therapy
  • Prader-Willi Syndrome* / genetics

Substances

  • EHMT2 protein, human
  • Histocompatibility Antigens
  • Histone-Lysine N-Methyltransferase