Heme oxygenase inhibition in cancers: possible tools and targets
Article 2018 pl
Authors
PP
Paulina Podkalicka
OM
Olga Mucha
AJ
Alicja Józkowicz
Abstract
1 min read
Heme oxygenase-1 (HO-1, encoded by <i>HMOX1</i>) through degradation of pro-oxidant heme into carbon monoxide (CO), ferrous ions (Fe<sup>2+</sup>) and biliverdin, exhibits cytoprotective, anti-apoptotic and anti-inflammatory properties. All of these potentially beneficial functions of HO-1 may play an important role in tumors' development and progression. Moreover, HO-1 is very often upregulated in tumors in comparison to healthy tissues, and its expression is further induced upon chemo-, radio- and photodynamic therapy, what results in decreased effectiveness of the treatment. Consequently, HO-1 can be proposed as a therapeutic target for anticancer treatment in many types of tumors. Nonetheless, possibilities of specific inhibition of HO-1 are strongly limited. Metalloporphyrins are widely used in <i>in vitro</i> studies, however, they are unselective and may exert serious side effects including an increase in <i>HMOX1</i> mRNA level. On the other hand, detailed information about pharmacokinetics and biodistribution of imidazole-dioxolane derivatives, other potential inhibitors, is lacking. The genetic inhibition of HO-1 by RNA interference (RNAi) or CRISPR/Cas9 approaches provides the possibility to specifically target HO-1; however, the potential therapeutic application of those methods are distant at best. In summary, HO-1 inhibition might be the valuable anticancer approach, however, the ideal strategy for HO-1 targeting requires further studies.
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