International Journal of Molecular Sciences (Apr 2022)

Role of Polyamine-Induced Dimerization of Antizyme in Its Cellular Functions

  • Mervi T. Hyvönen,
  • Olga A. Smirnova,
  • Vladimir A. Mitkevich,
  • Vera L. Tunitskaya,
  • Maxim Khomutov,
  • Dmitry S. Karpov,
  • Sergey P. Korolev,
  • Merja R. Häkkinen,
  • Marko Pietilä,
  • Marina B. Gottikh,
  • Jouko Vepsäläinen,
  • Leena Alhonen,
  • Alexander A. Makarov,
  • Sergey N. Kochetkov,
  • Heather M. Wallace,
  • Tuomo A. Keinänen,
  • Alex R. Khomutov

DOI
https://doi.org/10.3390/ijms23094614
Journal volume & issue
Vol. 23, no. 9
p. 4614

Abstract

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The polyamines, spermine (Spm) and spermidine (Spd), are important for cell growth and function. Their homeostasis is strictly controlled, and a key downregulator of the polyamine pool is the polyamine-inducible protein, antizyme 1 (OAZ1). OAZ1 inhibits polyamine uptake and targets ornithine decarboxylase (ODC), the rate-limiting enzyme of polyamine biosynthesis, for proteasomal degradation. Here we report, for the first time, that polyamines induce dimerization of mouse recombinant full-length OAZ1, forming an (OAZ1)2-Polyamine complex. Dimerization could be modulated by functionally active C-methylated spermidine mimetics (MeSpds) by changing the position of the methyl group along the Spd backbone—2-MeSpd was a poor inducer as opposed to 1-MeSpd, 3-MeSpd, and Spd, which were good inducers. Importantly, the ability of compounds to inhibit polyamine uptake correlated with the efficiency of the (OAZ1)2-Polyamine complex formation. Thus, the (OAZ1)2-Polyamine complex may be needed to inhibit polyamine uptake. The efficiency of polyamine-induced ribosomal +1 frameshifting of OAZ1 mRNA could also be differentially modulated by MeSpds—2-MeSpd was a poor inducer of OAZ1 biosynthesis and hence a poor downregulator of ODC activity unlike the other MeSpds. These findings offer new insight into the OAZ1-mediated regulation of polyamine homeostasis and provide the chemical tools to study it.

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