Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions

PURPOSE: We present a case of voltage-gated potassium channel (VGKC) complex antibody-positive limbic encephalitis (LE) harboring autoantibodies against Kv1.2. Since the patient responded well to immunotherapy, the autoantibodies were regarded as pathogenic. We aimed to characterize the pathophysiol...

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Autores principales: Kirschstein, Timo, Sadkiewicz, Erika, Hund-Göschel, Gerda, Becker, Juliane, Guli, Xiati, Müller, Steffen, Rohde, Marco, Hübner, Dora-Charlotte, Brehme, Hannes, Kolbaske, Stephan, Porath, Katrin, Sellmann, Tina, Großmann, Annette, Wittstock, Matthias, Syrbe, Steffen, Storch, Alexander, Köhling, Rüdiger
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Neuroscience
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7110982/
https://www.ncbi.nlm.nih.gov/pubmed/32269520
http://dx.doi.org/10.3389/fnsyn.2020.00013
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author Kirschstein, Timo
Sadkiewicz, Erika
Hund-Göschel, Gerda
Becker, Juliane
Guli, Xiati
Müller, Steffen
Rohde, Marco
Hübner, Dora-Charlotte
Brehme, Hannes
Kolbaske, Stephan
Porath, Katrin
Sellmann, Tina
Großmann, Annette
Wittstock, Matthias
Syrbe, Steffen
Storch, Alexander
Köhling, Rüdiger
author_facet Kirschstein, Timo
Sadkiewicz, Erika
Hund-Göschel, Gerda
Becker, Juliane
Guli, Xiati
Müller, Steffen
Rohde, Marco
Hübner, Dora-Charlotte
Brehme, Hannes
Kolbaske, Stephan
Porath, Katrin
Sellmann, Tina
Großmann, Annette
Wittstock, Matthias
Syrbe, Steffen
Storch, Alexander
Köhling, Rüdiger
author_sort Kirschstein, Timo
collection PubMed
description PURPOSE: We present a case of voltage-gated potassium channel (VGKC) complex antibody-positive limbic encephalitis (LE) harboring autoantibodies against Kv1.2. Since the patient responded well to immunotherapy, the autoantibodies were regarded as pathogenic. We aimed to characterize the pathophysiological role of this antibody in comparison to an antibody against the VGKC-associated protein contactin-associated protein-2 (CASPR2). METHODS: Stereotactic injection of patient sera (anti-Kv1.2-associated LE or anti-CASPR2 encephalopathy) and a control subject was performed into the hippocampus of the anesthetized rat in vivo, and hippocampal slices were prepared for electrophysiological purposes. Using extra- and intracellular techniques, synaptic transmission, long-term potentiation (LTP) and vulnerability to pro-epileptic conditions were analyzed. RESULTS: We observed that the slope of the field excitatory postsynaptic potential (fEPSP) was significantly increased at Schaffer collateral-CA1 synapses in anti-Kv1.2-treated and anti-CASPR2-treated rats, but not at medial perforant path-dentate gyrus synapses. The increase of the fEPSP slope in CA1 was accompanied by a decrease of the paired-pulse ratio in anti-Kv1.2, but not in anti-CASPR2 tissue, indicating presynaptic site of anti-Kv1.2. In addition, anti-Kv1.2 tissue showed enhanced LTP in CA1, but dentate gyrus LTP remained unaltered. Importantly, LTP in slices from anti-CASPR2-treated animals did not differ from control values. Intracellular recordings from CA1 neurons revealed that the resting membrane potential and a single action potential were not different between anti-Kv1.2 and control tissue. However, when the depolarization was prolonged, the number of action potentials elicited was reduced in anti-Kv1.2-treated tissue compared to both control and anti-CASPR2 tissue. In contrast, polyspike discharges induced by removal of Mg(2+) occurred earlier and more frequently in both patient sera compared to control. CONCLUSION: Patient serum containing anti-Kv1.2 facilitates presynaptic transmitter release as well as postsynaptic depolarization at the Schaffer-collateral-CA1 synapse, but not in the dentate gyrus. As a consequence, both synaptic transmission and LTP in CA1 are facilitated and action potential firing is altered. In contrast, anti-CASPR2 leads to increased postsynaptic potentials, but without changing LTP or firing properties suggesting that anti-Kv1.2 and anti-CASPR2 differ in their cellular effects. Both patient sera alter susceptibility to epileptic conditions, but presumably by different mechanisms.
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spelling pubmed-71109822020-04-08 Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions Kirschstein, Timo Sadkiewicz, Erika Hund-Göschel, Gerda Becker, Juliane Guli, Xiati Müller, Steffen Rohde, Marco Hübner, Dora-Charlotte Brehme, Hannes Kolbaske, Stephan Porath, Katrin Sellmann, Tina Großmann, Annette Wittstock, Matthias Syrbe, Steffen Storch, Alexander Köhling, Rüdiger Front Synaptic Neurosci Neuroscience PURPOSE: We present a case of voltage-gated potassium channel (VGKC) complex antibody-positive limbic encephalitis (LE) harboring autoantibodies against Kv1.2. Since the patient responded well to immunotherapy, the autoantibodies were regarded as pathogenic. We aimed to characterize the pathophysiological role of this antibody in comparison to an antibody against the VGKC-associated protein contactin-associated protein-2 (CASPR2). METHODS: Stereotactic injection of patient sera (anti-Kv1.2-associated LE or anti-CASPR2 encephalopathy) and a control subject was performed into the hippocampus of the anesthetized rat in vivo, and hippocampal slices were prepared for electrophysiological purposes. Using extra- and intracellular techniques, synaptic transmission, long-term potentiation (LTP) and vulnerability to pro-epileptic conditions were analyzed. RESULTS: We observed that the slope of the field excitatory postsynaptic potential (fEPSP) was significantly increased at Schaffer collateral-CA1 synapses in anti-Kv1.2-treated and anti-CASPR2-treated rats, but not at medial perforant path-dentate gyrus synapses. The increase of the fEPSP slope in CA1 was accompanied by a decrease of the paired-pulse ratio in anti-Kv1.2, but not in anti-CASPR2 tissue, indicating presynaptic site of anti-Kv1.2. In addition, anti-Kv1.2 tissue showed enhanced LTP in CA1, but dentate gyrus LTP remained unaltered. Importantly, LTP in slices from anti-CASPR2-treated animals did not differ from control values. Intracellular recordings from CA1 neurons revealed that the resting membrane potential and a single action potential were not different between anti-Kv1.2 and control tissue. However, when the depolarization was prolonged, the number of action potentials elicited was reduced in anti-Kv1.2-treated tissue compared to both control and anti-CASPR2 tissue. In contrast, polyspike discharges induced by removal of Mg(2+) occurred earlier and more frequently in both patient sera compared to control. CONCLUSION: Patient serum containing anti-Kv1.2 facilitates presynaptic transmitter release as well as postsynaptic depolarization at the Schaffer-collateral-CA1 synapse, but not in the dentate gyrus. As a consequence, both synaptic transmission and LTP in CA1 are facilitated and action potential firing is altered. In contrast, anti-CASPR2 leads to increased postsynaptic potentials, but without changing LTP or firing properties suggesting that anti-Kv1.2 and anti-CASPR2 differ in their cellular effects. Both patient sera alter susceptibility to epileptic conditions, but presumably by different mechanisms. Frontiers Media S.A. 2020-03-25 /pmc/articles/PMC7110982/ /pubmed/32269520 http://dx.doi.org/10.3389/fnsyn.2020.00013 Text en Copyright © 2020 Kirschstein, Sadkiewicz, Hund-Göschel, Becker, Guli, Müller, Rohde, Hübner, Brehme, Kolbaske, Porath, Sellmann, Großmann, Wittstock, Syrbe, Storch and Köhling. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Neuroscience
Kirschstein, Timo
Sadkiewicz, Erika
Hund-Göschel, Gerda
Becker, Juliane
Guli, Xiati
Müller, Steffen
Rohde, Marco
Hübner, Dora-Charlotte
Brehme, Hannes
Kolbaske, Stephan
Porath, Katrin
Sellmann, Tina
Großmann, Annette
Wittstock, Matthias
Syrbe, Steffen
Storch, Alexander
Köhling, Rüdiger
Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions
title Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions
title_full Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions
title_fullStr Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions
title_full_unstemmed Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions
title_short Stereotactically Injected Kv1.2 and CASPR2 Antisera Cause Differential Effects on CA1 Synaptic and Cellular Excitability, but Both Enhance the Vulnerability to Pro-epileptic Conditions
title_sort stereotactically injected kv1.2 and caspr2 antisera cause differential effects on ca1 synaptic and cellular excitability, but both enhance the vulnerability to pro-epileptic conditions
topic Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7110982/
https://www.ncbi.nlm.nih.gov/pubmed/32269520
http://dx.doi.org/10.3389/fnsyn.2020.00013
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