Disease Models & Mechanisms (Aug 2016)

A chemical with proven clinical safety rescues Down-syndrome-related phenotypes in through DYRK1A inhibition

  • Hyeongki Kim,
  • Kyu-Sun Lee,
  • Ae-Kyeong Kim,
  • Miri Choi,
  • Kwangman Choi,
  • Mingu Kang,
  • Seung-Wook Chi,
  • Min-Sung Lee,
  • Jeong-Soo Lee,
  • So-Young Lee,
  • Woo-Joo Song,
  • Kweon Yu,
  • Sungchan Cho

DOI
https://doi.org/10.1242/dmm.025668
Journal volume & issue
Vol. 9, no. 8
pp. 839 – 848

Abstract

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DYRK1A is important in neuronal development and function, and its excessive activity is considered a significant pathogenic factor in Down syndrome and Alzheimer's disease. Thus, inhibition of DYRK1A has been suggested to be a new strategy to modify the disease. Very few compounds, however, have been reported to act as inhibitors, and their potential clinical uses require further evaluation. Here, we newly identify CX-4945, the safety of which has been already proven in the clinical setting, as a potent inhibitor of DYRK1A that acts in an ATP-competitive manner. The inhibitory potency of CX-4945 on DYRK1A (IC50=6.8 nM) in vitro was higher than that of harmine, INDY or proINDY, which are well-known potent inhibitors of DYRK1A. CX-4945 effectively reverses the aberrant phosphorylation of Tau, amyloid precursor protein (APP) and presenilin 1 (PS1) in mammalian cells. To our surprise, feeding with CX-4945 significantly restored the neurological and phenotypic defects induced by the overexpression of minibrain, an ortholog of human DYRK1A, in the Drosophila model. Moreover, oral administration of CX-4945 acutely suppressed Tau hyperphosphorylation in the hippocampus of DYRK1A-overexpressing mice. Our research results demonstrate that CX-4945 is a potent DYRK1A inhibitor and also suggest that it has therapeutic potential for DYRK1A-associated diseases.

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