Ischemia-induced cell depolarization: does the hyperpolarization-activated cation channel HCN2 affect the outcome after stroke in mice?

Petra Ehling; Eva Göb; Stefan Bittner; Thomas Budde; Andreas Ludwig; Christoph Kleinschnitz; Sven G Meuth

doi:10.1186/2040-7378-5-16

Ischemia-induced cell depolarization: does the hyperpolarization-activated cation channel HCN2 affect the outcome after stroke in mice?

Exp Transl Stroke Med. 2013 Dec 27;5(1):16. doi: 10.1186/2040-7378-5-16.

Authors

Petra Ehling^#^{1

2}, Eva Göb^#³, Stefan Bittner⁴, Thomas Budde⁵, Andreas Ludwig⁶, Christoph Kleinschnitz³, Sven G Meuth^{1

4}

Affiliations

¹ Department of Neurology, and Institute of Physiology, Neuropathophysiology, Albert-Schweitzer-Campus 1, Westfälische Wilhelms University, 48149 Münster, Germany.
² Department of Neurology, ICB, Mendelstr. 7, 48149 Münster, Germany.
³ Department of Neurology, University Clinic Würzburg, Josef-Schneider-Str. 11, Würzburg, Germany.
⁴ Department of Neurology, Albert-Schweitzer-Campus 1, Westfälische Wilhelms University, Münster, Germany.
⁵ Institute of Physiology I, Westfälische Wilhelms University, Robert-Koch-Str. 27a, Münster, Germany.
⁶ Institute of Experimental and Clinical Pharmacology and Toxicology, Friedrich-Alexander Universität Erlangen-Nürnberg, Fahrstr. 17, Erlangen, Germany.

^# Contributed equally.

Abstract

Background: Brain ischemia is known to include neuronal cell death and persisting neurological deficits. A lack of oxygen and glucose are considered to be key mediators of ischemic neurodegeneration while the exact mechanisms are yet unclear. In former studies the expression of two different two-pore domain potassium (K2P) channels (TASK1, TREK1) were shown to ameliorate neuronal damage due to cerebral ischemia. In neurons, TASK channels carrying hyperpolarizing K+ leak currents, and the pacemaker channel HCN2, carrying depolarizing Ih, stabilize the membrane potential by a mutual functional interaction. It is assumed that this ionic interplay between TASK and HCN2 channels enhances the resistance of neurons to insults accompanied by extracellular pH shifts.

Methods: In C57Bl/6 (wildtype, WT), hcn2+/+ and hcn2-/- mice we used an in vivo model of cerebral ischemia (transient middle cerebral artery occlusion (tMCAO)) to depict a functional impact of HCN2 in stroke formation. Subsequent analyses comprise behavioural tests and hcn2 gene expression assays.

Results: After 60 min of tMCAO induction in WT mice, we collected tissue samples at 6, 12, and 24 h after reperfusion. In the infarcted neocortex, hcn2 expression analyses revealed a nominal peak of hcn2 expression 6 h after reperfusion with a tendency towards lower expression levels with longer reperfusion times. Hcn2 gene expression levels in infarcted basal ganglia did not change after 6 h and 12 h. Only at 24 h after reperfusion, hcn2 expression significantly decreases by ~55%. However, 30 min of tMCAO in hcn2-/- as well as hcn2+/+ littermates induced similar infarct volumes. Behavioural tests for global neurological function (Bederson score) and motor function/coordination (grip test) were performed at day 1 after surgery. Again, we found no differences between the groups.

Conclusions: Here, we hypothesized that the absence of HCN2, an important functional counter player of TASK channels, affects neuronal survival during stroke-induced tissue damage. However, together with a former study on TASK3 these results implicate that both TASK3 and HCN2 which were supposed to be neuroprotective due to their pH-dependency, do not influence ischemic neurodegeneration during stroke in the tMCAO model.