Time and dose dependent effects of oxidative stress induced by cumene hydroperoxide in neuronal excitability of rat motor cortex neurons

•CH depresses the excitability of pyramidal neurons in a time/dose dependent manner.•Reversibility of alterations by CH is inversely proportional to exposure time.•Ability to repetitively discharge action potentials was the most affected property.•Large neurons of the motor cortex are more sensitive...

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Veröffentlicht in:	Neurotoxicology (Park Forest South) 2016-03, Vol.53, p.201-214
Hauptverfasser:	Pardillo-Díaz, R., Carrascal, L., Muñoz, M.F., Ayala, A., Nunez-Abades, P.
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Sprache:	eng
Schlagworte:	Amyotrophic Lateral Sclerosis Analysis of Variance Animals Animals, Newborn Benzene Derivatives - pharmacology Biophysical Phenomena - drug effects Biophysics Cumene hydroperoxide Dose-Response Relationship, Drug Electric Stimulation In Vitro Techniques Lipid peroxidation Membrane Potentials - drug effects Motor Cortex - cytology Neuronal excitability Neurons - drug effects Oxidants - pharmacology Oxidative Stress - drug effects Patch clamp Patch-Clamp Techniques Pyramidal neurons Rats Rats, Wistar Time Factors
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description	•CH depresses the excitability of pyramidal neurons in a time/dose dependent manner.•Reversibility of alterations by CH is inversely proportional to exposure time.•Ability to repetitively discharge action potentials was the most affected property.•Large neurons of the motor cortex are more sensitive to the oxidant.•Melatonin prevented LPO and the physiological changes induced by CH. It has been claimed that oxidative stress and the production of reactive oxygen radicals can contribute to neuron degeneration and might be one factor in the development of different neurological diseases. In our study, we have attempted to clarify how oxidative damage induces dose dependent changes in functional membrane properties of neurons by means of whole cell patch clamp techniques in brain slices from young adult rats. Our research demonstrates physiological changes in membrane properties of pyramidal motor cortex neurons exposed to 3 concentrations of cumene hydroperoxide (CH; 1, 10 and 100μM) during 30min. Results show that oxidative stress induced by CH evokes important changes, in a concentration and time dependent manner, in the neuronal excitability of motor cortex neurons of the rat: (i) Low concentration of the drug (1μM) already blocks inward rectifications (sag) and decreases action potential amplitude and gain, a drug concentration which has no effects on other neuronal populations, (ii) 10μM of CH depresses the excitability of pyramidal motor cortex neurons by decreasing input resistance, amplitude of the action potential, and gain and maximum frequency of the repetitive firing discharge, and (iii) 100μM completely blocks the capability to produce repetitive discharge of action potentials in all cells. Both larger drug concentrations and/or longer times of exposure to CH narrow the current working range. This happens because of the increase in the rheobase, and the reduction of the cancelation current. The effects caused by oxidative stress, including those produced by the level of lipid peroxidation, are practically irreversible and, this, therefore, indicates that neuroprotective agents should be administered at the first symptoms of alterations to membrane properties. In fact, the pre-treatment with melatonin, acting as an antioxidant, prevented the lipid peroxidation and the physiological changes induced by CH. Larger cells (as estimated by their cell capacitance) were also more susceptible to oxidative stress. Our results provide previously unavailable
doi_str_mv	10.1016/j.neuro.2016.02.005
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It has been claimed that oxidative stress and the production of reactive oxygen radicals can contribute to neuron degeneration and might be one factor in the development of different neurological diseases. In our study, we have attempted to clarify how oxidative damage induces dose dependent changes in functional membrane properties of neurons by means of whole cell patch clamp techniques in brain slices from young adult rats. Our research demonstrates physiological changes in membrane properties of pyramidal motor cortex neurons exposed to 3 concentrations of cumene hydroperoxide (CH; 1, 10 and 100μM) during 30min. Results show that oxidative stress induced by CH evokes important changes, in a concentration and time dependent manner, in the neuronal excitability of motor cortex neurons of the rat: (i) Low concentration of the drug (1μM) already blocks inward rectifications (sag) and decreases action potential amplitude and gain, a drug concentration which has no effects on other neuronal populations, (ii) 10μM of CH depresses the excitability of pyramidal motor cortex neurons by decreasing input resistance, amplitude of the action potential, and gain and maximum frequency of the repetitive firing discharge, and (iii) 100μM completely blocks the capability to produce repetitive discharge of action potentials in all cells. Both larger drug concentrations and/or longer times of exposure to CH narrow the current working range. This happens because of the increase in the rheobase, and the reduction of the cancelation current. The effects caused by oxidative stress, including those produced by the level of lipid peroxidation, are practically irreversible and, this, therefore, indicates that neuroprotective agents should be administered at the first symptoms of alterations to membrane properties. In fact, the pre-treatment with melatonin, acting as an antioxidant, prevented the lipid peroxidation and the physiological changes induced by CH. Larger cells (as estimated by their cell capacitance) were also more susceptible to oxidative stress. Our results provide previously unavailable observations that large size and high sensitivity to oxidative stress (even at low concentrations) make pyramidal neurons of the motor cortex, in particular corticofugal neurons, more susceptible to cell death when compared with other neuronal populations. 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It has been claimed that oxidative stress and the production of reactive oxygen radicals can contribute to neuron degeneration and might be one factor in the development of different neurological diseases. In our study, we have attempted to clarify how oxidative damage induces dose dependent changes in functional membrane properties of neurons by means of whole cell patch clamp techniques in brain slices from young adult rats. Our research demonstrates physiological changes in membrane properties of pyramidal motor cortex neurons exposed to 3 concentrations of cumene hydroperoxide (CH; 1, 10 and 100μM) during 30min. Results show that oxidative stress induced by CH evokes important changes, in a concentration and time dependent manner, in the neuronal excitability of motor cortex neurons of the rat: (i) Low concentration of the drug (1μM) already blocks inward rectifications (sag) and decreases action potential amplitude and gain, a drug concentration which has no effects on other neuronal populations, (ii) 10μM of CH depresses the excitability of pyramidal motor cortex neurons by decreasing input resistance, amplitude of the action potential, and gain and maximum frequency of the repetitive firing discharge, and (iii) 100μM completely blocks the capability to produce repetitive discharge of action potentials in all cells. Both larger drug concentrations and/or longer times of exposure to CH narrow the current working range. This happens because of the increase in the rheobase, and the reduction of the cancelation current. The effects caused by oxidative stress, including those produced by the level of lipid peroxidation, are practically irreversible and, this, therefore, indicates that neuroprotective agents should be administered at the first symptoms of alterations to membrane properties. In fact, the pre-treatment with melatonin, acting as an antioxidant, prevented the lipid peroxidation and the physiological changes induced by CH. Larger cells (as estimated by their cell capacitance) were also more susceptible to oxidative stress. Our results provide previously unavailable observations that large size and high sensitivity to oxidative stress (even at low concentrations) make pyramidal neurons of the motor cortex, in particular corticofugal neurons, more susceptible to cell death when compared with other neuronal populations. These results could also shed some light on explaining the causes behind diseases such as Amyotrophic Lateral Sclerosis.</description><subject>Amyotrophic Lateral Sclerosis</subject><subject>Analysis of Variance</subject><subject>Animals</subject><subject>Animals, Newborn</subject><subject>Benzene Derivatives - pharmacology</subject><subject>Biophysical Phenomena - drug effects</subject><subject>Biophysics</subject><subject>Cumene hydroperoxide</subject><subject>Dose-Response Relationship, Drug</subject><subject>Electric Stimulation</subject><subject>In Vitro Techniques</subject><subject>Lipid peroxidation</subject><subject>Membrane Potentials - drug effects</subject><subject>Motor Cortex - cytology</subject><subject>Neuronal excitability</subject><subject>Neurons - drug effects</subject><subject>Oxidants - pharmacology</subject><subject>Oxidative Stress - drug effects</subject><subject>Patch clamp</subject><subject>Patch-Clamp Techniques</subject><subject>Pyramidal neurons</subject><subject>Rats</subject><subject>Rats, Wistar</subject><subject>Time Factors</subject><issn>0161-813X</issn><issn>1872-9711</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2016</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNqNkctu1DAUQC1ERaeFL0BCXrJJ8GNsJwsWqGqhUiU2rcTOcuwb4VFiD7ZTzfwBn13PA5aIlW3dcx--B6H3lLSUUPlp0wZYUmxZfbSEtYSIV2hFO8WaXlH6Gq1qgDYd5T8u0VXOG0KoULJ_gy6Z7JRijK7Q70c_AzbBYRczYAdbCA5CwTCOYEvGccRx550p_hlwLglyxj64xYLDwx7bZYYA-OfepbiFdEChxvFxtGAmDDvrixn85Mv-UCyZgudYYsI2pgK7M5nfoovRTBnenc9r9HR3-3jzrXn4_vX-5stDYwXhpRl4J43rmOmlo5Q7YutlLQ3pqXGgLDfrXqhBsKEbpRCcEaYII44NXI2ScX6NPp7qblP8tUAuevbZwjSZAHHJmqpOsDXve_IfqJKkX4sjyk-oTTHnBKPeJj-btNeU6IMtvdHHj-qDLU2YrrZq1odzg2WYwf3N-aOnAp9PANSNPHtIOlsPoe7ep2pHu-j_2eAFVqWpGQ</recordid><startdate>201603</startdate><enddate>201603</enddate><creator>Pardillo-Díaz, R.</creator><creator>Carrascal, L.</creator><creator>Muñoz, M.F.</creator><creator>Ayala, A.</creator><creator>Nunez-Abades, P.</creator><general>Elsevier B.V</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope><scope>7TK</scope><scope>7U7</scope><scope>C1K</scope></search><sort><creationdate>201603</creationdate><title>Time and dose dependent effects of oxidative stress induced by cumene hydroperoxide in neuronal excitability of rat motor cortex neurons</title><author>Pardillo-Díaz, R. ; 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It has been claimed that oxidative stress and the production of reactive oxygen radicals can contribute to neuron degeneration and might be one factor in the development of different neurological diseases. In our study, we have attempted to clarify how oxidative damage induces dose dependent changes in functional membrane properties of neurons by means of whole cell patch clamp techniques in brain slices from young adult rats. Our research demonstrates physiological changes in membrane properties of pyramidal motor cortex neurons exposed to 3 concentrations of cumene hydroperoxide (CH; 1, 10 and 100μM) during 30min. Results show that oxidative stress induced by CH evokes important changes, in a concentration and time dependent manner, in the neuronal excitability of motor cortex neurons of the rat: (i) Low concentration of the drug (1μM) already blocks inward rectifications (sag) and decreases action potential amplitude and gain, a drug concentration which has no effects on other neuronal populations, (ii) 10μM of CH depresses the excitability of pyramidal motor cortex neurons by decreasing input resistance, amplitude of the action potential, and gain and maximum frequency of the repetitive firing discharge, and (iii) 100μM completely blocks the capability to produce repetitive discharge of action potentials in all cells. Both larger drug concentrations and/or longer times of exposure to CH narrow the current working range. This happens because of the increase in the rheobase, and the reduction of the cancelation current. The effects caused by oxidative stress, including those produced by the level of lipid peroxidation, are practically irreversible and, this, therefore, indicates that neuroprotective agents should be administered at the first symptoms of alterations to membrane properties. In fact, the pre-treatment with melatonin, acting as an antioxidant, prevented the lipid peroxidation and the physiological changes induced by CH. Larger cells (as estimated by their cell capacitance) were also more susceptible to oxidative stress. Our results provide previously unavailable observations that large size and high sensitivity to oxidative stress (even at low concentrations) make pyramidal neurons of the motor cortex, in particular corticofugal neurons, more susceptible to cell death when compared with other neuronal populations. These results could also shed some light on explaining the causes behind diseases such as Amyotrophic Lateral Sclerosis.</abstract><cop>Netherlands</cop><pub>Elsevier B.V</pub><pmid>26877221</pmid><doi>10.1016/j.neuro.2016.02.005</doi><tpages>14</tpages><oa>free_for_read</oa></addata></record>
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subjects	Amyotrophic Lateral Sclerosis Analysis of Variance Animals Animals, Newborn Benzene Derivatives - pharmacology Biophysical Phenomena - drug effects Biophysics Cumene hydroperoxide Dose-Response Relationship, Drug Electric Stimulation In Vitro Techniques Lipid peroxidation Membrane Potentials - drug effects Motor Cortex - cytology Neuronal excitability Neurons - drug effects Oxidants - pharmacology Oxidative Stress - drug effects Patch clamp Patch-Clamp Techniques Pyramidal neurons Rats Rats, Wistar Time Factors
title	Time and dose dependent effects of oxidative stress induced by cumene hydroperoxide in neuronal excitability of rat motor cortex neurons
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