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Basic and Clinical Neuroscience، جلد ۵، شماره ۱، صفحات ۶۶-۷۳
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عنوان انگلیسی Unilateral Hypothalamus Inactivation Prevents PTZ Kindling Development through Hippocampal Orexin Receptor 1 Modulation
چکیده انگلیسی مقاله Introduction: Epilepsy is a neural disorder in which abnormal plastic changes during short and long term periods lead to increased excitability of brain tissue. Kindling is an animal model of epileptogenesis which results in changes of synaptic plasticity due to repetitive electrical or chemical sub-convulsive stimulations of the brain. Lateral hypothalamus, as the main niche of orexin neurons with extensive projections, is involved in sleep and wakefulness and so it affects the excitability of the brain. Therefore, we investigated whether lateral hypothalamic area (LHA) inactivation or orexin-A receptor blocking could change convulsive behavior of acute and kindled PTZ treated animals and if glutamate has a role in this regard. Methods: Kindling was induced by 40 mg/kg PTZ, every 48 hours up to 13 injections to each rat. Three consecutive stages 4 or 5 of convulsive behavior were used to ensure kindling. Lidocaine was injected stereotaxically to inactivate LHA, unilaterally. SB334867 used for orexin receptor 1 (OX1R) blocking administered in CSF. Results: We demonstrated that LHA inactivation prevented PTZ kindling and hence, excitability evolution. Hippocampal glutamate content was decreased due to LHA inactivation, OX1R antagonist infusion, lidocaine injection and kindled groups. In accordance, OX1R antagonist (SB334867) and lidocaine injection decreased PTZ single dose induced convulsive behavior. While orexin-A i.c.v. infusion increased hippocampal glutamate content, it did not change PTZ induced convulsive intensity. Discussion: It is concluded that LHA inactivation prevented kindling development probably through orexin receptor antagonism. CSF orexin probably acts as an inhibitory step on convulsive intensity through another unknown process.
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نویسندگان مقاله نسیبه اکبری | nasibe akbari
school of biology, damghan university, damghan, iran.

سازمان اصلی تایید شده: دانشگاه دامغان (Damghan university)

محمود اله دادی سلمانی | mahmoud elahdadi salmani
school of biology, damghan university, damghan, iran.

سازمان اصلی تایید شده: دانشگاه دامغان (Damghan university)

مهدی گودرزوند | mahdi goudarzvand
faculty of medicine, alborz university of medical sciences, karaj, iran.


تقی لشگربلوکی | taghi lashkarboluki
school of biology, damghan university, damghan, iran

سازمان اصلی تایید شده: دانشگاه دامغان (Damghan university)

ایران گودرزی | iran goudarzi
school of biology, damghan university, damghan, iran

سازمان اصلی تایید شده: دانشگاه دامغان (Damghan university)

کتانه ابراری | kataneh abrari
school of biology, damghan university, damghan, iran

سازمان اصلی تایید شده: دانشگاه دامغان (Damghan university)

نشانی اینترنتی http://bcn.iums.ac.ir/browse.php?a_code=A-10-1-197&slc_lang=en&sid=en
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کد مقاله (doi)
زبان مقاله منتشر شده en
موضوعات مقاله منتشر شده Behavioral Neuroscience
نوع مقاله منتشر شده Original
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