Journal of Enzyme Inhibition and Medicinal Chemistry (Jan 2019)

Exploring the activity of polyamine analogues on polyamine and spermine oxidase: methoctramine, a potent and selective inhibitor of polyamine oxidase

  • Maria Luisa Di Paolo,
  • Manuela Cervelli,
  • Paolo Mariottini,
  • Alessia Leonetti,
  • Fabio Polticelli,
  • Michela Rosini,
  • Andrea Milelli,
  • Filippo Basagni,
  • Rina Venerando,
  • Enzo Agostinelli,
  • Anna Minarini

DOI
https://doi.org/10.1080/14756366.2019.1584620
Journal volume & issue
Vol. 34, no. 1
pp. 740 – 752

Abstract

Read online

Fourteen polyamine analogues, asymmetric or symmetric substituted spermine (1–9) or methoctramine (10–14) analogues, were evaluated as potential inhibitors or substrates of two enzymes of the polyamine catabolic pathway, spermine oxidase (SMOX) and acetylpolyamine oxidase (PAOX). Compound 2 turned out to be the best substrate for PAOX, having the highest affinity and catalytic efficiency with respect to its physiological substrates. Methoctramine (10), a well-known muscarinic M2 receptor antagonist, emerged as the most potent competitive PAOX inhibitor known so far (Ki = 10 nM), endowed with very good selectivity compared with SMOX (Ki=1.2 μM vs SMOX). The efficacy of methoctramine in inhibiting PAOX activity was confirmed in the HT22 cell line. Methoctramine is a very promising tool in the design of drugs targeting the polyamine catabolism pathway, both to understand the physio-pathological role of PAOX vs SMOX and for pharmacological applications, being the polyamine pathway involved in various pathologies.

Keywords