AUTHOR=Houtman Marien J. C. , Friesacher Theres , Chen Xingyu , Zangerl-Plessl Eva-Maria , Heyden Marcel A. G. van der , Stary-Weinzinger Anna 

TITLE=Development of IKATP Ion Channel Blockers Targeting Sulfonylurea Resistant Mutant KIR6.2 Based Channels for Treating DEND Syndrome

JOURNAL=Frontiers in Pharmacology

VOLUME=12

YEAR=2022

URL=https://www.frontiersin.org/journals/pharmacology/articles/10.3389/fphar.2021.814066

DOI=10.3389/fphar.2021.814066

ISSN=1663-9812

ABSTRACT=<p><bold>Introduction:</bold> DEND syndrome is a rare channelopathy characterized by a combination of developmental delay, epilepsy and severe neonatal diabetes. Gain of function mutations in the <italic>KCNJ11</italic> gene, encoding the K<sub>IR</sub>6.2 subunit of the I<sub>KATP</sub> potassium channel, stand at the basis of most forms of DEND syndrome. In a previous search for existing drugs with the potential of targeting Cantú Syndrome, also resulting from increased I<sub>KATP</sub>, we found a set of candidate drugs that may also possess the potential to target DEND syndrome. In the current work, we combined Molecular Modelling including Molecular Dynamics simulations, with single cell patch clamp electrophysiology, in order to test the effect of selected drug candidates on the K<sub>IR</sub>6.2 WT and DEND mutant channels.</p><p><bold>Methods:</bold> Molecular dynamics simulations were performed to investigate potential drug binding sites. To conduct <italic>in vitro</italic> studies, K<sub>IR</sub>6.2 Q52R and L164P mutants were constructed. Inside/out patch clamp electrophysiology on transiently transfected HEK293T cells was performed for establishing drug-channel inhibition relationships.</p><p><bold>Results:</bold> Molecular Dynamics simulations provided insight in potential channel interaction and shed light on possible mechanisms of action of the tested drug candidates. Effective I<sub>KIR6.2/SUR2a</sub> inhibition was obtained with the pore-blocker betaxolol (IC<sub>50</sub> values 27–37 μM). Levobetaxolol effectively inhibited WT and L164P (IC<sub>50</sub> values 22 μM) and Q52R (IC<sub>50</sub> 55 μM) channels. Of the SUR binding prostaglandin series, travoprost was found to be the best blocker of WT and L164P channels (IC<sub>50</sub> 2–3 μM), while Q52R inhibition was 15–20% at 10 μM.</p><p><bold>Conclusion:</bold> Our combination of MD and inside-out electrophysiology provides the rationale for drug mediated I<sub>KATP</sub> inhibition, and will be the basis for 1) screening of additional existing drugs for repurposing to address DEND syndrome, and 2) rationalized medicinal chemistry to improve I<sub>KATP</sub> inhibitor efficacy and specificity.</p>