The potassium channel KCa3.1 constitutes a pharmacological target for neuroinflammation associated with ischemia/reperfusion stroke

Chen, Yi‐Je; Nguyen, Hai M.; Maezawa, Izumi; Grössinger, Eva M.; Garing, April Lourdes A; Köhler, Ralf; Jin, Lee‐Way; Wulff, Heike

doi:10.1177/0271678x15611434

Cited by 84 publications

(129 citation statements)

References 42 publications

(65 reference statements)

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“…Animals that met these inclusion criteria were assigned to treatment or vehicle groups based on a computer‐generated randomization scheme. Based on our previous work with the KCa3.1 blocker TRAM‐34 in MCAO,16, 25 sample size was powered to detect a reduction of 40% in mean percentage infarct area with 80% power. Starting 12 h after reperfusion animals received the vehicle miglyol 812 neutral oil (Neobee M5 ® , Spectrum Chemicals) or PAP‐1 at 10 or 40 mg/kg intraperitoneally every 12 h until sacrifice on day‐8.…”

Section: Methodsmentioning

confidence: 99%

“…CD11b + cells from the infarct area were isolated as previously described 16, 27. Briefly, mice were anesthetized with isoflurane 2, 5, and 8 days after reperfusion MCAO and killed by cervical dislocation.…”

Section: Methodsmentioning

confidence: 99%

“…NeuN (1:1000, A60, Millipore) staining to assess infarct area was performed as described 16. For the mouse brain IF images in Figure 1A, Kv1.3 was stained with a polyclonal anti‐Kv1.3 antibody (1:300, APC‐101, Alomone) and Iba1 with a monoclonal anti‐Iba1 antibody (1:1000, NCNP24, Wako Chemical).…”

Section: Methodsmentioning

confidence: 99%

“…Electrophysiological experiments on slices15 or acutely isolated microglia16 have further demonstrated Kv1.3 currents on activated microglia following MCAO. In humans, strong Kv1.3 staining has been reported on microglia in the frontal cortex of patients with Alzheimer's disease17 and on CD68 + cells in multiple sclerosis brain lesions 18.…”

Section: Introductionmentioning

confidence: 98%

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Inhibition of the potassium channel Kv1.3 reduces infarction and inflammation in ischemic stroke

Chen

Nguyen

Maezawa

et al. 2017

Ann Clin Transl Neurol

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ObjectiveInhibitors of the voltage‐gated K+ channel Kv1.3 are currently in development as immunomodulators for the treatment of autoimmune diseases. As Kv1.3 is also expressed on microglia and has been shown to be specifically up‐regulated on “M1‐like” microglia, we here tested the therapeutic hypothesis that the brain‐penetrant small‐molecule Kv1.3‐inhibitor PAP‐1 reduces secondary inflammatory damage after ischemia/reperfusion.MethodsWe studied microglial Kv1.3 expression using electrophysiology and immunohistochemistry, and evaluated PAP‐1 in hypoxia‐exposed organotypic hippocampal slices and in middle cerebral artery occlusion (MCAO) with 8 days of reperfusion in both adult male C57BL/6J mice (60 min MCAO) and adult male Wistar rats (90 min MCAO). In both models, PAP‐1 administration was started 12 h after reperfusion.ResultsWe observed Kv1.3 staining on activated microglia in ischemic infarcts in mice, rats, and humans and found higher Kv1.3 current densities in acutely isolated microglia from the infarcted hemisphere than in microglia isolated from the contralateral hemisphere of MCAO mice. PAP‐1 reduced microglia activation and increased neuronal survival in hypoxia‐exposed hippocampal slices as effectively as minocycline. In mouse MCAO, PAP‐1 dose‐dependently reduced infarct area, improved neurological deficit score, and reduced brain levels of IL‐1β and IFN‐γ without affecting IL‐10 and brain‐derived nerve growth factor (BDNF) levels or inhibiting ongoing phagocytosis. The beneficial effects on infarct area and neurological deficit score were reproduced in rats providing confirmation in a second species.InterpretationOur findings suggest that Kv1.3 constitutes a promising therapeutic target for preferentially inhibiting “M1‐like” inflammatory microglia/macrophage functions in ischemic stroke.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 98%

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Inhibition of the potassium channel Kv1.3 reduces infarction and inflammation in ischemic stroke

Chen

Nguyen

Maezawa

et al. 2017

Ann Clin Transl Neurol

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“…Similar to the related small-conductance Ca 21 -activated K 1 channel or KCa2 channels, KCa3.1 channels have fewer charges in their S4 segment than voltage-gated K 1 (Kv) channels (Wei et al, 2005); therefore, they do not respond to changes in membrane voltage but instead are activated by Ca 21 binding to calmodulin, which functions as their b-subunit and induces Ca 21 -dependent channel opening (Fanger et al, 1999 KCa3.1 is widely expressed in cells of the immune system such as T-and B-lymphocytes (Ghanshani et al, 2000;Wulff et al, 2004), mast cells (Shumilina et al, 2008), macrophages, and microglia (Chen et al, 2016), where it plays an important role in cellular activation, migration, and cytokine production (Feske et al, 2015). KCa3.1 is further important for volume regulation in erythrocytes (Vandorpe et al, 1998), which is why the channel is often referred to as the Gárdos channel after the Hungarian scientist, who first described a Ca 21 -activated K 1 efflux leading to erythrocyte dehydration (Gardos, 1958).…”

Section: Introductionmentioning

confidence: 99%

Structural Insights into the Atomistic Mechanisms of Action of Small Molecule Inhibitors Targeting the KCa3.1 Channel Pore

et al. 2017

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Repurposing the KCa3.1 inhibitor senicapoc for Alzheimer's disease

Jin

Lucente

Nguyen

et al. 2019

Ann Clin Transl Neurol

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Objective Microglia play a pivotal role in the initiation and progression of Alzheimer's disease ( AD ). We here tested the therapeutic hypothesis that the Ca 2+ ‐activated potassium channel KC a3.1 constitutes a potential target for treating AD by reducing neuroinflammation. Methods To determine if KC a3.1 is relevant to AD , we tested if treating cultured microglia or hippocampal slices with A β oligomer (A β O) activated KC a3.1 in microglia, and if microglial KC a3.1 was upregulated in 5x FAD mice and in human AD brains. The expression/activity of KC a3.1 was examined by qPCR , Western blotting, immunohistochemistry, and whole‐cell patch‐clamp. To investigate the role of KC a3.1 in AD pathology, we resynthesized senicapoc, a clinically tested KC a3.1 blocker, and determined its pharmacokinetic properties and its effect on microglial activation, A β deposition and hippocampal long‐term potentiation ( hLTP ) in 5x FAD mice. Results We found markedly enhanced microglial KC a3.1 expression/activity in brains of both 5x FAD mice and AD patients. In hippocampal slices, microglial KC a3.1 expression/activity was increased by A β O treatment, and its inhibition diminished the proinflammatory and hLTP ‐impairing activities of A β O. Senicapoc exhibited excellent brain penetrance and oral availability, and in 5x FAD mice, reduced neuroinflammation, decreased cerebral amyloid load, and enhanced hippocampal neuronal plasticity. Interpretation Our results prompt us to propose repurposing senicapoc for AD clinical trials, as senicapoc has excellent pharmacological properties and was safe and well‐tolerated in a prior phase‐3 clinical trial for sickle cell anemia. Such repurposing has the potential to expedite the urgently needed new drug discovery for AD .

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The potassium channel KCa3.1 constitutes a pharmacological target for neuroinflammation associated with ischemia/reperfusion stroke

Cited by 84 publications

References 42 publications

Inhibition of the potassium channel Kv1.3 reduces infarction and inflammation in ischemic stroke

Inhibition of the potassium channel Kv1.3 reduces infarction and inflammation in ischemic stroke

Structural Insights into the Atomistic Mechanisms of Action of Small Molecule Inhibitors Targeting the KCa3.1 Channel Pore

Repurposing the KCa3.1 inhibitor senicapoc for Alzheimer's disease

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