The effects of Acorus calamus L. in preventing memory loss, anxiety, and oxidative stress on lipopolysaccharide-induced neuroinflammation rat models
Objective: Several factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The need of finding preventive treatments of memory impairment in elderly encouraged authors to assess the effect of Acorus calamus on memory lo...
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| Published in | International journal of preventive medicine Vol. 9; no. 1; p. 85 |
|---|---|
| Main Authors | , , , , |
| Format | Journal Article |
| Language | English |
| Published |
Iran
Wolters Kluwer India Pvt. Ltd
01.01.2018
Medknow Publications & Media Pvt. Ltd Medknow Publications & Media Pvt Ltd Wolters Kluwer Medknow Publications |
| Subjects | |
| Online Access | Get full text |
| ISSN | 2008-7802 2008-8213 |
| DOI | 10.4103/ijpvm.IJPVM_75_18 |
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| Abstract | Objective: Several factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The need of finding preventive treatments of memory impairment in elderly encouraged authors to assess the effect of Acorus calamus on memory loss, anxiety, and antioxidant indices on neuroinflammation rat models. Materials and Methods: Different fractions of A. calamus were prepared. The subject rats were grouped in 11 groups of 10 each. In the nine treated groups, the extract gavage began 1 week before intraperitoneal (i.p.) injection of lipopolysaccharide (LPS) and continued for 2 weeks after the last injection of LPS. Behavioral tests, including passive avoidance and elevated plus-maze (EPM) tests, were run on days 24, 25, and 26 and the subjects were sacrificed on the day after the last behavioral test, and their hippocampus was isolated to measure the oxidative stress markers. Results: Assessment of oxidative stress markers in hippocampus samples revealed that the amounts of endogenous antioxidant enzymes (superoxide dismutase, glutathione peroxidase, and total antioxidant activity) in the groups that received different fractions were less than their equivalent figures in LPS-control group, and levels of malondialdehyde (MDA) in treatment groups were less than MDA level in LPS-control group. Moreover, the treatment groups with different fractions of A. calamus revealed better performance compared to LPS-control group in shuttle-box test. In EPM test, the groups with different fractions revealed lower stress level in comparison with LPS-control group. The best performance in memory test and the lowest level of stress in EPM was observed in the group with aqueous fraction at 600 mg/kg dose, and the least figures of oxidative stress markers were of the group with aqueous fraction at 600 mg/kg dose. Conclusion: The oral administration of different fractions of A. calamus, especially aqueous fraction, prevented from memory deficits and stress through controlling oxidative stress and inflammation processes. |
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| AbstractList | Objective: Several factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The need of finding preventive treatments of memory impairment in elderly encouraged authors to assess the effect of Acorus calamus on memory loss, anxiety, and antioxidant indices on neuroinflammation rat models. Materials and Methods: Different fractions of A. calamus were prepared. The subject rats were grouped in 11 groups of 10 each. In the nine treated groups, the extract gavage began 1 week before intraperitoneal (i.p.) injection of lipopolysaccharide (LPS) and continued for 2 weeks after the last injection of LPS. Behavioral tests, including passive avoidance and elevated plus-maze (EPM) tests, were run on days 24, 25, and 26 and the subjects were sacrificed on the day after the last behavioral test, and their hippocampus was isolated to measure the oxidative stress markers. Results: Assessment of oxidative stress markers in hippocampus samples revealed that the amounts of endogenous antioxidant enzymes (superoxide dismutase, glutathione peroxidase, and total antioxidant activity) in the groups that received different fractions were less than their equivalent figures in LPS-control group, and levels of malondialdehyde (MDA) in treatment groups were less than MDA level in LPS-control group. Moreover, the treatment groups with different fractions of A. calamus revealed better performance compared to LPS-control group in shuttle-box test. In EPM test, the groups with different fractions revealed lower stress level in comparison with LPS-control group. The best performance in memory test and the lowest level of stress in EPM was observed in the group with aqueous fraction at 600 mg/kg dose, and the least figures of oxidative stress markers were of the group with aqueous fraction at 600 mg/kg dose. Conclusion: The oral administration of different fractions of A. calamus, especially aqueous fraction, prevented from memory deficits and stress through controlling oxidative stress and inflammation processes. Several factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The need of finding preventive treatments of memory impairment in elderly encouraged authors to assess the effect of Acorus calamus on memory loss, anxiety, and antioxidant indices on neuroinflammation rat models.OBJECTIVESeveral factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The need of finding preventive treatments of memory impairment in elderly encouraged authors to assess the effect of Acorus calamus on memory loss, anxiety, and antioxidant indices on neuroinflammation rat models.Different fractions of A. calamus were prepared. The subject rats were grouped in 11 groups of 10 each. In the nine treated groups, the extract gavage began 1 week before intraperitoneal (i.p.) injection of lipopolysaccharide (LPS) and continued for 2 weeks after the last injection of LPS. Behavioral tests, including passive avoidance and elevated plus-maze (EPM) tests, were run on days 24, 25, and 26 and the subjects were sacrificed on the day after the last behavioral test, and their hippocampus was isolated to measure the oxidative stress markers.MATERIALS AND METHODSDifferent fractions of A. calamus were prepared. The subject rats were grouped in 11 groups of 10 each. In the nine treated groups, the extract gavage began 1 week before intraperitoneal (i.p.) injection of lipopolysaccharide (LPS) and continued for 2 weeks after the last injection of LPS. Behavioral tests, including passive avoidance and elevated plus-maze (EPM) tests, were run on days 24, 25, and 26 and the subjects were sacrificed on the day after the last behavioral test, and their hippocampus was isolated to measure the oxidative stress markers.Assessment of oxidative stress markers in hippocampus samples revealed that the amounts of endogenous antioxidant enzymes (superoxide dismutase, glutathione peroxidase, and total antioxidant activity) in the groups that received different fractions were less than their equivalent figures in LPS-control group, and levels of malondialdehyde (MDA) in treatment groups were less than MDA level in LPS-control group. Moreover, the treatment groups with different fractions of A. calamus revealed better performance compared to LPS-control group in shuttle-box test. In EPM test, the groups with different fractions revealed lower stress level in comparison with LPS-control group. The best performance in memory test and the lowest level of stress in EPM was observed in the group with aqueous fraction at 600 mg/kg dose, and the least figures of oxidative stress markers were of the group with aqueous fraction at 600 mg/kg dose.RESULTSAssessment of oxidative stress markers in hippocampus samples revealed that the amounts of endogenous antioxidant enzymes (superoxide dismutase, glutathione peroxidase, and total antioxidant activity) in the groups that received different fractions were less than their equivalent figures in LPS-control group, and levels of malondialdehyde (MDA) in treatment groups were less than MDA level in LPS-control group. Moreover, the treatment groups with different fractions of A. calamus revealed better performance compared to LPS-control group in shuttle-box test. In EPM test, the groups with different fractions revealed lower stress level in comparison with LPS-control group. The best performance in memory test and the lowest level of stress in EPM was observed in the group with aqueous fraction at 600 mg/kg dose, and the least figures of oxidative stress markers were of the group with aqueous fraction at 600 mg/kg dose.The oral administration of different fractions of A. calamus, especially aqueous fraction, prevented from memory deficits and stress through controlling oxidative stress and inflammation processes.CONCLUSIONThe oral administration of different fractions of A. calamus, especially aqueous fraction, prevented from memory deficits and stress through controlling oxidative stress and inflammation processes. Several factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The need of finding preventive treatments of memory impairment in elderly encouraged authors to assess the effect of on memory loss, anxiety, and antioxidant indices on neuroinflammation rat models. Different fractions of were prepared. The subject rats were grouped in 11 groups of 10 each. In the nine treated groups, the extract gavage began 1 week before intraperitoneal (i.p.) injection of lipopolysaccharide (LPS) and continued for 2 weeks after the last injection of LPS. Behavioral tests, including passive avoidance and elevated plus-maze (EPM) tests, were run on days 24, 25, and 26 and the subjects were sacrificed on the day after the last behavioral test, and their hippocampus was isolated to measure the oxidative stress markers. Assessment of oxidative stress markers in hippocampus samples revealed that the amounts of endogenous antioxidant enzymes (superoxide dismutase, glutathione peroxidase, and total antioxidant activity) in the groups that received different fractions were less than their equivalent figures in LPS-control group, and levels of malondialdehyde (MDA) in treatment groups were less than MDA level in LPS-control group. Moreover, the treatment groups with different fractions of revealed better performance compared to LPS-control group in shuttle-box test. In EPM test, the groups with different fractions revealed lower stress level in comparison with LPS-control group. The best performance in memory test and the lowest level of stress in EPM was observed in the group with aqueous fraction at 600 mg/kg dose, and the least figures of oxidative stress markers were of the group with aqueous fraction at 600 mg/kg dose. The oral administration of different fractions of , especially aqueous fraction, prevented from memory deficits and stress through controlling oxidative stress and inflammation processes. |
| Author | Ghanadian, Mustafa Vatankhah, Amir Esfandiari, Ebrahim Rashidi, Bahman Mokhtarian, Amir |
| AuthorAffiliation | Department of Anatomical Sciences, Isfahan University of Medical Sciences, Isfahan, Iran 1 Pharmaceutical Sciences Research Center, Faculty of Pharmacy and Pharmaceutical Sciences, Isfahan University of Medical Sciences, Isfahan, Iran 2 Drug Applied Research Center, Tabriz Medical University, Tabriz, Iran |
| AuthorAffiliation_xml | – name: 2 Drug Applied Research Center, Tabriz Medical University, Tabriz, Iran – name: Department of Anatomical Sciences, Isfahan University of Medical Sciences, Isfahan, Iran – name: 1 Pharmaceutical Sciences Research Center, Faculty of Pharmacy and Pharmaceutical Sciences, Isfahan University of Medical Sciences, Isfahan, Iran |
| Author_xml | – sequence: 1 givenname: Ebrahim surname: Esfandiari fullname: Esfandiari, Ebrahim organization: Department of Anatomical Sciences, Isfahan University of Medical Sciences, Isfahan – sequence: 2 givenname: Mustafa surname: Ghanadian fullname: Ghanadian, Mustafa organization: Pharmaceutical Sciences Research Center, Faculty of Pharmacy and Pharmaceutical Sciences, Isfahan University of Medical Sciences, Isfahan – sequence: 3 givenname: Bahman surname: Rashidi fullname: Rashidi, Bahman organization: Department of Anatomical Sciences, Isfahan University of Medical Sciences, Isfahan – sequence: 4 givenname: Amir surname: Mokhtarian fullname: Mokhtarian, Amir organization: Department of Anatomical Sciences, Isfahan University of Medical Sciences, Isfahan – sequence: 5 givenname: Amir surname: Vatankhah fullname: Vatankhah, Amir organization: Drug Applied Research Center, Tabriz Medical University, Tabriz |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/30450168$$D View this record in MEDLINE/PubMed |
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| Cites_doi | 10.1016/S0076-6879(99)99017-1 |
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| Keywords | stress and anxiety neuroinflammation memory impairment oxidative stress Acorus calamus L |
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| References | Joshi (key-10.4103/2008-7802.243273-21) 2016 Ishiyama (key-10.4103/2008-7802.243273-33) 2007 Naplekova (key-10.4103/2008-7802.243273-34) 39;n Kaya (key-10.4103/2008-7802.243273-40) 2004 Heneka (key-10.4103/2008-7802.243273-11) 2007 Kim (key-10.4103/2008-7802.243273-45) 2009 Patki (key-10.4103/2008-7802.243273-6) 2013 Sharma (key-10.4103/2008-7802.243273-23) 2014 Hardy (key-10.4103/2008-7802.243273-2) 2002 Yang (key-10.4103/2008-7802.243273-7) 2016 Nunomura (key-10.4103/2008-7802.243273-4) 2006 Guo (key-10.4103/2008-7802.243273-12) 2002 Lee (key-10.4103/2008-7802.243273-31) 2008 Paglia (key-10.4103/2008-7802.243273-37) 1967 Yamamoto (key-10.4103/2008-7802.243273-10) 2007 Qin (key-10.4103/2008-7802.243273-30) 2007 Fukui (key-10.4103/2008-7802.243273-5) 2002 Woolliams (key-10.4103/2008-7802.243273-38) 1983 Shukla (key-10.4103/2008-7802.243273-44) 2002 Hebert (key-10.4103/2008-7802.243273-1) 2013 Dastmalchi (key-10.4103/2008-7802.243273-19) 2007 Lim (key-10.4103/2008-7802.243273-46) 2014 Eikelenboom (key-10.4103/2008-7802.243273-14) 1994 Tasset (key-10.4103/2008-7802.243273-16) 2012 Garcia (key-10.4103/2008-7802.243273-15) 2005 Huang (key-10.4103/2008-7802.243273-22) 2013 Nunomura (key-10.4103/2008-7802.243273-3) 2000 Blasko (key-10.4103/2008-7802.243273-9) 1999 Biswas (key-10.4103/2008-7802.243273-17) 2016 Shukla (key-10.4103/2008-7802.243273-43) 2006 Shin (key-10.4103/2008-7802.243273-26) 2014 Muthuraman (key-10.4103/2008-7802.243273-42) 2011 Ahmadian-Attari (key-10.4103/2008-7802.243273-18) 2015 Lee (key-10.4103/2008-7802.243273-32) 2010 Manikandan (key-10.4103/2008-7802.243273-41) 2005 Yan (key-10.4103/2008-7802.243273-13) 2003 key-10.4103/2008-7802.243273-29 key-10.4103/2008-7802.243273-28 Shi (key-10.4103/2008-7802.243273-47) 2014 Parki (key-10.4103/2008-7802.243273-24) 2017 Holmes (key-10.4103/2008-7802.243273-35) 2000 Salim (key-10.4103/2008-7802.243273-8) 2011 Manikandan (key-10.4103/2008-7802.243273-25) 2005 Nandakumar (key-10.4103/2008-7802.243273-20) 2013 Lim (key-10.4103/2008-7802.243273-27) 2014 Ghadrdoost (key-10.4103/2008-7802.243273-36) 2011 Miller (key-10.4103/2008-7802.243273-39) 1993 |
| References_xml | – start-page: 631 volume-title: Involvement of oxidative stress in Alzheimer disease year: 2006 ident: key-10.4103/2008-7802.243273-4 publication-title: J Neuropathol Exp Neurol – start-page: 353 volume-title: The amyloid hypothesis of Alzheimer's disease: Progress and problems on the road to therapeutics year: 2002 ident: key-10.4103/2008-7802.243273-2 publication-title: Science – start-page: 1 volume-title: Alpha-asarone from Acorus gramineus alleviates epilepsy by modulating A-type GABA receptors year: 2013 ident: key-10.4103/2008-7802.243273-22 publication-title: Neuropharmacology – start-page: 680 volume-title: Interferon-γ and tumor necrosis factor-α regulate amyloid-β plaque deposition and β-secretase expression in Swedish mutant APP transgenic mice year: 2007 ident: key-10.4103/2008-7802.243273-10 publication-title: Am J Pathol – start-page: 56 volume-title: LPS-induced inflammation exacerbates phospho-tau pathology in rTg4510 mice year: 2010 ident: key-10.4103/2008-7802.243273-32 publication-title: J Neuroinflammation – start-page: 318 volume-title: A rapid HPLC-ESI-MS/MS method for determination of β-asarone, a potential anti-epileptic agent, in plasma after oral administration of Acorus calamus extract to rats year: 2013 ident: key-10.4103/2008-7802.243273-20 publication-title: Biomed Chromatogr – start-page: 17 volume-title: α-Asarone ameliorates memory deficit in lipopolysaccharide-treated mice via suppression of pro-inflammatory cytokines and microglial activation year: 2014 ident: key-10.4103/2008-7802.243273-26 publication-title: Biomol Ther – start-page: 7504 volume-title: Anti-inflammatory drug therapy alters β-amyloid processing and deposition in an animal model of Alzheimer's disease year: 2003 ident: key-10.4103/2008-7802.243273-13 publication-title: J Neurosci – ident: key-10.4103/2008-7802.243273-28 – start-page: 81 volume-title: Seasonal Variation in Essential Oil Compositions and Antioxidant Properties of Acorus calamus L year: 2017 ident: key-10.4103/2008-7802.243273-24 publication-title: Accessions Medicines – start-page: 253 volume-title: Variation in the activities of glutathione peroxidase and superoxide dismutase and in the concentration of copper in the blood in various breed crosses of sheep year: 1983 ident: key-10.4103/2008-7802.243273-38 publication-title: Res Vet Sci – start-page: 265 volume-title: β-Asarone (cis-2, 4, 5-trimethoxy-1-allyl phenyl), attenuates pro-inflammatory mediators by inhibiting NF-κB signaling and the JNK pathway in LPS activated BV-2 microglia cells year: 2014 ident: key-10.4103/2008-7802.243273-46 publication-title: Food Chem Toxicol – start-page: 1778 volume-title: Alzheimer disease in the United States (2010–2050) estimated using the 2010 census year: 2013 ident: key-10.4103/2008-7802.243273-1 publication-title: Neurology – start-page: 149 volume-title: Anti-inflammatory activity of a water extract of Acorus calamus L.leaves on keratinocyte HaCaT cells year: 2009 ident: key-10.4103/2008-7802.243273-45 publication-title: J Ethnopharmacol – start-page: 5900 volume-title: Inflammation-dependent cerebral deposition of serum amyloid a protein in a mouse model of amyloidosis year: 2002 ident: key-10.4103/2008-7802.243273-12 publication-title: J Neurosci – start-page: 164 volume-title: Acorus calamus Linn.: phytoconstituents and bactericidal property year: 2016 ident: key-10.4103/2008-7802.243273-21 publication-title: World J Microbiol Biotechnol – start-page: 1011 volume-title: Neuronal oxidative stress precedes amyloid-β deposition in Down syndrome year: 2000 ident: key-10.4103/2008-7802.243273-3 publication-title: J Neuropathol Exp Neurol – start-page: 222 volume-title: Protective effects of saffron extract and its active constituent crocin against oxidative stress and spatial learning and memory deficits induced by chronic stress in rats year: 2011 ident: key-10.4103/2008-7802.243273-36 publication-title: Eur J Pharmacol – start-page: 440 volume-title: Peripheral oxidative stress in relapsing–remitting multiple sclerosis year: 2012 ident: key-10.4103/2008-7802.243273-16 publication-title: Clin Biochem – start-page: 453 volume-title: Systemic LPS causes chronic neuroinflammation and progressive neurodegeneration year: 2007 ident: key-10.4103/2008-7802.243273-30 publication-title: Glia – start-page: 127 volume-title: Lipid peroxidation measurement by thiobarbituric acid assay in rat cerebellar slices year: 2005 ident: key-10.4103/2008-7802.243273-15 publication-title: J Neurosci Methods – start-page: 1 volume-title: Treatment of Alzheimer's disease in Iranian traditional medicine.Iranian Red Crescent Medical Journal year: 2015 ident: key-10.4103/2008-7802.243273-18 – start-page: 1454 volume-title: Acorus calamus (The Healing Plant): A review on its medicinal potential, micropropagation and conservation year: 2014 ident: key-10.4103/2008-7802.243273-23 publication-title: Nat Prod Res – start-page: 160 volume-title: Lurasidone (SM-13496), a novel atypical antipsychotic drug, reverses MK-801-induced impairment of learning and memory in the rat passive-avoidance test year: 2007 ident: key-10.4103/2008-7802.243273-33 publication-title: Eur J Pharmacol – start-page: 265 volume-title: β-Asarone (cis-2, 4, 5-trimethoxy-1-allyl phenyl), attenuates pro-inflammatory mediators by inhibiting NF-κB signaling and the JNK pathway in LPS activated BV-2 microglia cells year: 2014 ident: key-10.4103/2008-7802.243273-27 publication-title: Food Chem Toxicol – start-page: 91 volume-title: Evaluation of the wound-healing activity and anti-inflammatory activity of aqueous extracts from Acorus calamus L year: 2014 ident: key-10.4103/2008-7802.243273-47 publication-title: Pak J Pharm Sci – start-page: 352 volume-title: Systemic inflammation induces anxiety disorder through CXCL12/CXCR4 pathway year: 2016 ident: key-10.4103/2008-7802.243273-7 publication-title: Brain Behav Immun – start-page: 63 volume-title: TNFα plus IFNγ induce the production of Alzheimer β-amyloid peptides and decrease the secretion of APPs year: 1999 ident: key-10.4103/2008-7802.243273-9 publication-title: FASEB J – start-page: 693 volume-title: Lipid peroxidation at various estradiol concentrations in human circulation during ovarian stimulation with exogenous gonadotropins year: 2004 ident: key-10.4103/2008-7802.243273-40 publication-title: Horm Metab Res – start-page: 24 volume-title: Attenuating effect of Acorus calamus extract in chronic constriction injury induced neuropathic pain in rats: An evidence of anti-oxidative, anti-inflammatory, neuroprotective and calcium inhibitory effects year: 2011 ident: key-10.4103/2008-7802.243273-42 publication-title: BMC Complement Altern Med – start-page: 2327 volume-title: Protective effect of Acorus calamus LINN on free radical scavengers and lipid peroxidation in discrete regions of brain against noise stress exposed rat year: 2005 ident: key-10.4103/2008-7802.243273-25 publication-title: Biol Pharm Bull – start-page: 2327 volume-title: Protective effect of Acorus calamus LINN on free radical scavengers and lipid peroxidation in discrete regions of brain against noise stress exposed rat year: 2005 ident: key-10.4103/2008-7802.243273-41 publication-title: Biol Pharm Bull – start-page: 5698931 volume-title: Does the interdependence between oxidative stress and inflammation explain the antioxidant paradox.? year: 2016 ident: key-10.4103/2008-7802.243273-17 publication-title: Oxid Med Cell Longev – start-page: 256 volume-title: Protective effect of Acorus calamus against acrylamide induced neurotoxicity year: 2002 ident: key-10.4103/2008-7802.243273-44 publication-title: Phytother Res – start-page: 407 volume-title: A novel method for measuring antioxidant capacity and its application to monitoring the antioxidant status in premature neonates year: 1993 ident: key-10.4103/2008-7802.243273-39 publication-title: Clin Sci – start-page: 447 volume-title: Inflammatory mechanisms in Alzheimer's disease year: 1994 ident: key-10.4103/2008-7802.243273-14 publication-title: Trends Pharmacol Sci – start-page: 69 volume-title: Inflammatory processes in Alzheimer's disease year: 2007 ident: key-10.4103/2008-7802.243273-11 publication-title: J Neuroimmunol – start-page: 73 volume-title: Depression, anxiety-like behavior and memory impairment are associated with increased oxidative stress and inflammation in a rat model of social stress year: 2013 ident: key-10.4103/2008-7802.243273-6 publication-title: Brain Res – start-page: 63 volume-title: Potential contribution of oxidative stress and inflammation to anxiety and hypertension year: 2011 ident: key-10.4103/2008-7802.243273-8 publication-title: Brain Res – ident: key-10.4103/2008-7802.243273-29 doi: 10.1016/S0076-6879(99)99017-1 – start-page: 509 volume-title: Behavioral profile of wild mice in the elevated plus-maze test for anxiety year: 2000 ident: key-10.4103/2008-7802.243273-35 publication-title: Physiol Behav – start-page: 275 volume-title: Cognitive impairment of rats caused by oxidative stress and aging, and its prevention by vitamin E year: 2002 ident: key-10.4103/2008-7802.243273-5 publication-title: Ann N Y Acad Sci – start-page: 37 volume-title: Neuro-inflammation induced by lipopolysaccharide causes cognitive impairment through enhancement of beta-amyloid generation year: 2008 ident: key-10.4103/2008-7802.243273-31 publication-title: J Neuroinflammation – start-page: 3 volume-title: STUDYING ANXIOLYTIC AND ANTIDEPRESSANT PROPERTIES OF 2, 2, 6, 6-TETRAMETHYLPIPERIDONE DERIVATIVE year: 39;n ident: key-10.4103/2008-7802.243273-34 publication-title: Eksperimental – start-page: 158 volume-title: Studies on the quantitative and qualitative characterization of erythrocyte glutathione peroxidase year: 1967 ident: key-10.4103/2008-7802.243273-37 publication-title: Transl Res – start-page: 187 volume-title: Neuroprotective effect of Acorus calamus against middle cerebral artery occlusion–induced ischaemia in rat.Hum Exp Toxicol year: 2006 ident: key-10.4103/2008-7802.243273-43 – start-page: 83 volume-title: Plants as potential sources for drug development against Alzheimer's disease year: 2007 ident: key-10.4103/2008-7802.243273-19 publication-title: Int J Biomed Pharm Sci |
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| Snippet | Objective: Several factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The... Several factors lead to memory loss, the most important of which is brain aging that is caused mostly by neuroinflammation and oxidative stress. The need of... |
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| SubjectTerms | Acorus calamus L Alzheimer's disease Animals Antioxidants Anxiety Calibration Cytokines Drug dosages Enzymes Ethics Inflammation Lipid peroxidation Lipids Memory memory impairment neuroinflammation Original Oxidative stress Rodents stress and anxiety Studies |
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| Title | The effects of Acorus calamus L. in preventing memory loss, anxiety, and oxidative stress on lipopolysaccharide-induced neuroinflammation rat models |
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