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corticosterone and Behavior Disorders

corticosterone has been researched along with Behavior Disorders in 33 studies

Research Excerpts

ExcerptRelevanceReference
"Some patients with psychiatric disorders show hyperactivity of the hypothalamic-pituitary-adrenal (HPA) axis."1.46A Protocol for Generation of a Corticosterone Model of Psychiatric Disorders. ( Guest, PC, 2017)
"Psychiatric disorders have been hypothesized to originate during development, with genetic and environmental factors interacting in the etiology of disease."1.40Transient downregulation of Dab1 protein levels during development leads to behavioral and structural deficits: relevance for psychiatric disorders. ( Bosch, C; Howell, B; Masachs, N; Muhaisen, A; Pérez-Martínez, J; Soriano, E; Teixeira, CM, 2014)

Research

Studies (33)

TimeframeStudies, this research(%)All Research%
pre-19908 (24.24)18.7374
1990's2 (6.06)18.2507
2000's8 (24.24)29.6817
2010's12 (36.36)24.3611
2020's3 (9.09)2.80

Authors

AuthorsStudies
Gupta, P1
Mohanty, B1
Sun, CY1
Li, JR1
Wang, YY1
Lin, SY1
Ou, YC1
Lin, CJ1
Wang, JD1
Liao, SL1
Chen, CJ1
Basu, T1
Maguire, J1
Salpekar, JA1
Guest, PC1
Lebedeva, KA1
Caruncho, HJ1
Kalynchuk, LE1
Sobolewski, M1
Conrad, K1
Marvin, E1
Allen, JL1
Cory-Slechta, DA1
Godoy, LD1
Umeoka, EHL1
Ribeiro, DE1
Santos, VR1
Antunes-Rodrigues, J1
Joca, SRL1
Garcia-Cairasco, N1
Zhang, J1
Abdallah, CG1
Chen, Y1
Huang, T1
Huang, Q1
Xu, C1
Xiao, Y1
Liu, Y1
Ding, Y1
Wu, R1
Teixeira, CM1
Masachs, N1
Muhaisen, A1
Bosch, C1
Pérez-Martínez, J1
Howell, B1
Soriano, E1
MacRae, M1
Macrina, T1
Khoury, A1
Migliore, MM1
Kentner, AC1
de Lima, AP1
Sandini, TM1
Reis-Silva, TM1
Massoco, CO1
Couto-Pereira, NS1
Ferreira, CF1
Lampert, C1
Arcego, DM1
Toniazzo, AP1
Bernardi, JR1
da Silva, DC1
Von Poser Toigo, E1
Diehl, LA1
Krolow, R1
Silveira, PP1
Dalmaz, C1
O'Mahony, SM1
Marchesi, JR1
Scully, P1
Codling, C1
Ceolho, AM1
Quigley, EM1
Cryan, JF1
Dinan, TG1
Viveros, MP1
Llorente, R1
López-Gallardo, M1
Suarez, J1
Bermúdez-Silva, F1
De la Fuente, M1
Rodriguez de Fonseca, F1
Garcia-Segura, LM1
Watanabe, M1
Tamano, H1
Kikuchi, T1
Takeda, A1
Wainwright, SR1
Lieblich, SE1
Galea, LA1
Stasi, C1
Zignego, AL1
Laffi, G1
Rosselli, M1
Lee, PR1
Brady, D1
Koenig, JI1
Terpstra, J1
Gispen-De Wied, CC1
Broekhoven, MH1
Frankhuijzen, AC1
Kahn, RS1
van Ree, JM1
Wiegant, VM1
KOCH, B1
MIALHE-VOLOSS, C1
STUTINSKY, F1
SHIMA, S1
MATSUBA, M1
HODGES, JR1
JONES, MT1
Dhanalakshmi, S1
Devi, RS1
Srikumar, R1
Manikandan, S1
Thangaraj, R1
Ishikawa, M1
Ohdo, S1
Watanabe, H1
Hara, C1
Ogawa, N1
Zalcman, S1
Murray, L1
Dyck, DG1
Greenberg, AH1
Nance, DM1
McEwen, BS1
Haller, J1
van de Schraaf, J1
Kruk, MR1
Sánchez, MM1
Ladd, CO1
Plotsky, PM1
Ottenweller, JE1
Natelson, BH1
Pitman, DL1
Drastal, SD1
Arana, GW1
Wilens, TE1
Baldessarini, RJ1
Yamashita, I1
Moroji, T1
Yamazaki, K1
Kato, H1
Sakashita, A1
Bennett, R1
Hughes, GR1
Bywaters, EG1
Holt, PJ1
Silbergeld, S1
Noble, EP1

Clinical Trials (6)

Trial Overview

TrialPhaseEnrollmentStudy TypeStart DateStatus
Kynurenine Pathway Metabolites as Novel Translational Biological Markers of Irritable Bowel Syndrome: Relationship to Gastrointestinal Function, Cognition and Co-morbid Depression[NCT01304355]85 participants (Anticipated)Observational2011-01-31Recruiting
Characterization of Rebound Pain Following Peripheral Nerve Block and Its Association With Gut Microbiome Diversity[NCT02998177]20 participants (Actual)Observational2016-11-30Completed
The Safety and Effectiveness of Probiotic Supplementation on Bipolar Depression: a Proof of Concept Randomized Controlled Trial[NCT02155972]Phase 216 participants (Actual)Interventional2013-05-31Terminated (stopped due to The trial was terminated because of inability to recruit the needed number of participants)
Smartphone Stress Management Training for Irritable Bowel Syndrome[NCT05083091]325 participants (Anticipated)Interventional2022-02-10Recruiting
"Proof-of-Concept Stress & Anxiety Dampening Effects of Lpc-37"[NCT03494725]120 participants (Actual)Interventional2018-04-10Completed
Detecting Depression and Bipolar Disorder in Adolescents Using a Biomarker Panel[NCT01957501]75 participants (Actual)Observational2013-07-31Terminated (stopped due to Funding has been terminated for this study.)
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

Trial Outcomes

Change of Diastolic Blood Pressure (BP) in Response to the TSST

Efficacy of the intake of Lpc-37 on reduction of the increase of the diastolic BP in response to the TSST compared to placebo. (NCT03494725)
Timeframe: 3 minutes before the TSST and 1 minute after the TSST after 5 weeks of study product intake

,
InterventionmmHg (Mean)
Pre-TSST -3minPost-TSST +1min
Lpc-3779.1390.38
Placebo78.4188.36

Change of Mood Scale Scores Over the Course of the Treatment

"Efficacy of the intake of Lpc-37 on the increase of mood scale scores over the course of the treatment~Measured with a daily online diary. Mood was rated by participants on an 11-point scale (0-10; very bad to very well) and monitored through the washout phase (week 1 and 2) and the subsequent treatment phase (weeks 3-7). Higher scores indicate a better mood. Efficacy is defined as an increase, or (in case of a general decrease) reduced decrease for the active treatment group as compared to the placebo group and operationalized as the interaction between time and treatment group. Time is coded as a continuous variable with one average value for each week and participant. Values reflect summary measures for mood ratings on a scale from 0 to 10 for the averaged ratings per participant and week." (NCT03494725)
Timeframe: Daily for 2 weeks before treatment intake and 5 weeks during treatment intake

,
Interventionscore (Mean)
Week 1 (run-in)Week 2 (run-in)Week 3 (treatment)Week 4 (treatment)Week 5 (treatment)Week 6 (treatment)Week 7 (treatment)
Lpc-377.317.537.667.777.737.907.77
Placebo7.277.497.467.537.507.407.55

Change of Perceived Health Status Scores Over the Course of the Treatment

"Efficacy of the intake of Lpc-37 on the increase of perceived health status scores over the course of the treatment.~Measured with a daily online diary. Health status was rated by participants on an 11-point scale (0-10; not at all to very) and monitored through the wash-out phase (week 1 and 2) and the subsequent treatment phase (weeks 3-7). Higher scores indicate a high perceived health.Efficacy is defined as an increase, or (in case of a general decrease) reduced decrease for the active treatment group as compared to the placebo group and operationalized as the interaction between time and treatment group. Time is coded as a continuous variable with one value for each day and participant. Values reflect summary measures for perceived health status on a scale from 0 to 10 for the averaged ratings per participant and week." (NCT03494725)
Timeframe: Daily for 2 weeks before treatment intake and 5 weeks during treatment intake

,
Interventionscore (Mean)
Week 1 (run-in)Week 2 (run-in)Week 3 (treatment)Week 4 (treatment)Week 5 (treatment)Week 6 (treatment)Week 7 (treatment)
Lpc-377.807.897.887.918.058.117.91
Placebo7.867.927.928.017.927.737.75

Change of Perceived Productivity Scores Over the Course of the Treatment

"Efficacy of the intake of Lpc-37 on the increase of perceived productivity scores over the course of the treatment~Measured with a daily online diary. Productivity was rated by participants on an 11-point scale (0-10; not at all to very) and monitored through the wash-out phase (week 1 and 2) and the subsequent treatment phase (weeks 3-7). Higher scores indicate a higher perceived productivity. Efficacy is defined as an increase, or (in case of a general decrease) reduced decrease for the active treatment group as compared to the placebo group and operationalized as the interaction between time and treatment group.Time is coded as a continuous variable with one value for each day and participant. The values reflect summary measures for perceived productivity on a scale from 0 to 10 for the averaged ratings per participant and week." (NCT03494725)
Timeframe: Daily for 2 weeks before treatment intake and 5 weeks during treatment intake

,
Interventionscore (Mean)
Week 1 (run-in)Week 2 (run-in)Week 3 (treatment)Week 4 (treatment)Week 5 (treatment)Week 6 (treatment)Week 7 (treatment)
Lpc-376.987.347.537.487.597.577.50
Placebo7.157.297.307.347.437.317.32

Change of Reported Number of Sleep Disruptions Over the Course of the Treatment

"Efficacy of the intake of Lpc-37 on the decrease of reported number of sleep disruptions over the course of the treatment measured with a daily online diary (mean of week summary).~Sleep disruptions were monitored through the wash-out phase (Week 1 and 2) and the subsequent treatment phase (Weeks 3-7). In the count version, the value can be 0 or a natural number for each day and each participant. Efficacy is defined as a decrease, or (in case of a general increase) reduced increase for the active treatment group as compared to the placebo group and operationalized as the interaction between time and treatment group. Time is coded as a continuous variable with one value for each day and participant. Values reflect summary measures for sleep disruptions (count) for the summed counts per participant and week." (NCT03494725)
Timeframe: Daily for 2 weeks before treatment intake and 5 weeks during treatment intake

,
Interventionsleep disruptions per participant & week (Mean)
Week 1 (run-in)Week 2 (run-in)Week 3 (treatment)Week 4 (treatment)Week 5 (treatment)Week 6 (treatment)Week 7 (treatment)
Lpc-377.305.504.895.433.523.804.66
Placebo6.095.495.114.303.534.025.83

Change of Reported Sleep Disruptions Over the Course of the Treatment by Week (Proportion Yes/Total)

"Efficacy of the intake of Lpc-37 on the decrease of sleep disruptions over the course of the treatment measured with a daily online diary (Proportion (yes/total)).~Sleep disruptions were monitored through the wash-out phase and the subsequent treatment phase for each week. In the binary version, the value is either Yes or No for each day and each participant.~Efficacy is defined as a decrease, or (in case of a general increase) reduced increase for the active treatment group as compared to the placebo group and operationalized as the interaction between time and treatment group. Time is coded as a continuous variable with one value for each day and participant.~The proportion of participants with at least one sleep disruption by treatment group is given, treatment commenced after week 2. Data listed here reflect the proportion of participants who answered Yes (e.g. 0,477 * 44 = 20.99 participants answered with Yes in week 1 in the Lpc-37 group)." (NCT03494725)
Timeframe: Daily for 2 weeks before treatment intake and 5 weeks during treatment intake

,
InterventionProportion of participants (yes/total) (Number)
Week 1 (run-in)Week 2 (run-in)Week 3 (treatment)Week 4 (treatment)Week 5 (treatment)Week 6 (treatment)Week 7 (treatment)
Lpc-370.4770.4350.3540.3670.3060.2790.290
Placebo0.4650.4260.4180.3100.2920.3310.389

Change of sAA in Response to the TSST

Efficacy of the intake of Lpc-37 on reduction of the increase of salivary Alpha-Amylase (sAA) in response to the TSST compared to placebo. (NCT03494725)
Timeframe: 1 minute before the TSST and 1, 10, 20, 30 and 45 minutes after the TSST after 5 weeks of study product intake

,
InterventionU/ml (Mean)
Pre-TSST -2minPost-TSST +1minPost-TSST +10minPost-TSST +20minPost-TSST +30minPost-TSST +45min
Lpc-37154.04246.29146.53130.11125.19141.13
Placebo161.67270.55158.85141.49138.48148.15

Change of Salivary Cortisol in Response to the TSST

Efficacy of the intake of Lpc-37 on reduction of the increase of salivary cortisol in response to the TSST compared to placebo. (NCT03494725)
Timeframe: 1 minute before the TSST and 1, 10, 20, 30 and 45 minutes after the TSST after 5 weeks of study product intake

,
Interventionnmol/L (Mean)
Pre-TSST -2minPost-TSST +1minPost-TSST +10minPost-TSST +20minPost-TSST +30minPost-TSST +45min
Lpc-374.796.969.489.898.046.21
Placebo4.826.858.979.217.716.16

Change of Sleep Duration Over the Course of the Treatment

"Efficacy of the intake of Lpc-37 on the increase of sleep duration over the course of the treatment.~Sleep duration was monitored through the wash-out phase (week 1 and 2) and the subsequent treatment phase (weeks 3-7). Efficacy is defined as an increase, or (in case of a general decrease) reduced decrease for the active treatment group as compared to the placebo group and operationalized as the interaction between time and treatment group. Time is coded as a continuous variable with one value for each day and participant. Summary measures for Sleep duration for the averaged ratings per participant and week" (NCT03494725)
Timeframe: Daily for 2 weeks before treatment intake and 5 weeks during treatment intake

,
Interventionmin (Mean)
Week 1 (run-in)Week 2 (run-in)Week 3 (treatment)Week 4 (treatment)Week 5 (treatment)Week 6 (treatment)Week 7 (treatment)
Lpc-37447.27444.01449.45450.62454.50450.88445.60
Placebo447.45448.13456.90459.81457.26450.16459.66

Change of Sleep Related Recovery Scores Over the Course of the Treatment

"Efficacy of the intake of Lpc-37 on the increase of sleep related recovery scores over the course of the treatment.~Measured with a daily online diary. Sleep related recovery was rated by participants on an 11-point scale (0-10; not at all to very) and monitored throughout the wash-out phase (Week 1 and 2) and the subsequent treatment phase (weeks 3-7). High scores indicate a high recovery.~Efficacy is defined as an increase, or (in case of a general decrease) reduced decrease for the active treatment group as compared to the placebo group and operationalized as the interaction between time and treatment group. Time is coded as a continuous variable with one value for each day and participant. Summary measures for sleep related recovery for the averaged ratings per participant and week." (NCT03494725)
Timeframe: Daily for 2 weeks before treatment intake and 5 weeks during treatment intake

,
Interventionscore (Mean)
Week 1 (run-in)Week 2 (run-in)Week 3 (treatment)Week 4 (treatment)Week 5 (treatment)Week 6 (treatment)Week 7 (treatment)
Lpc-376.717.077.327.307.367.427.31
Placebo6.917.157.277.297.367.107.28

Change of STAI-State Scores in Response to the TSST

"Efficacy of the intake of Lpc-37 on reduction of the increase of STAI-State scores in response to the TSST compared to placebo.~Measured with the german version of the State-Trait-Anxiety Inventory, scale anxiety as a temporary emotional state (STAI-X1). Answers are given on a four-point rating scale ranging from 1=not at all to 4=very true. The score range is 20-80; Higher scores indicate more anxiety." (NCT03494725)
Timeframe: 10 minutes before the TSST and 1 minute after the TSST after 5 weeks of study product intake

,
Interventionscore (Mean)
Pre-TSST -10minPost-TSST +1min
Lpc-3736.0942.38
Placebo36.8343.60

Change of Systolic BP in Response to the TSST

Efficacy of the intake of Lpc-37 on reduction of the increase of the systolic BP in response to the TSST compared to placebo. (NCT03494725)
Timeframe: 3 minutes before the TSST and 1 minute after the TSST after 5 weeks of study product intake

,
InterventionmmHg (Mean)
Pre-TSST -3minPost-TSST +1min
Lpc-37115.11127.47
Placebo114.33129.19

Change of the Heart Rate (HR) in Response to the Trier Social Stress Test (TSST)

Efficacy was defined as a lower increase in HR in response to the TSST following intervention with Lpc-37, compared to placebo. (NCT03494725)
Timeframe: Continuous measurement starting 20 minutes before and ending 20 minutes after the TSST after 5 weeks of product intake. Mean values were calculated per group at seven-time windows before, during and after the TSST

,
Interventionbpm (Mean)
Pre-TSST -20minPre-TSST -10minPre-TSST -3minduring TSST (Interview)during TSST (Arithmetic)Post-TSST +10minPost-TSST +20min
Lpc-3774.8488.1597.34107.56102.7793.3275.88
Placebo74.3486.6997.62105.66100.8190.8174.97

Change of VAS Anxiety Scores in Response to the TSST

"Efficacy of the intake of Lpc-37 on reduction of the increase of VAS anxiety scores in response to the TSST compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating greater anxiety." (NCT03494725)
Timeframe: 10 minutes before the TSST, during the TSST and 1 minute after the TSST after 5 weeks of study product intake

,
Interventionscore (Mean)
Pre-TSST -10minInterview TSST (during)Post-TSST +1min
Lpc-376.8020.8510.68
Placebo8.5022.4711.74

Change of VAS Exhaustion Scores in Response to the TSST

"Efficacy of the intake of Lpc-37 on reduction of the increase of VAS exhaustion scores in response to the TSST compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating greater exhaustion." (NCT03494725)
Timeframe: 10 minutes before the TSST, during the TSST and 1 minute after the TSST after 5 weeks of study product intake

,
Interventionscore (Mean)
Pre-TSST -10minInterview TSST (during)Post-TSST +1min
Lpc-3721.1819.2022.12
Placebo19.7921.3025.68

Change of VAS Insecurity Scores in Response to the TSST

"Efficacy of the intake of Lpc-37 on reduction of the increase of VAS insecurity scores in response to the TSST compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating greater insecurity." (NCT03494725)
Timeframe: 10 minutes before the TSST, during the TSST and 1 minute after the TSST after 5 weeks of study product intake

,
Interventionscore (Mean)
Pre-TSST -10minInterview TSST (during)Post-TSST +1min
Lpc-3714.4745.0823.92
Placebo17.1952.1923.69

Change of VAS Stress Perception Scores in Response to the TSST

"Efficacy of the intake of Lpc-37 on reduction of the increase of VAS Stress perception scores in response to the TSST compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating higher perceived stress." (NCT03494725)
Timeframe: 10 minutes before the TSST, during the TSST and 1 minute after the TSST after 5 weeks of study product intake

,
Interventionscore (Mean)
Pre-TSST -10minInterview TSST (during)Post-TSST +1min
Lpc-3719.8947.7131.72
Placebo18.5251.5132.85

Changes in Pre and Post Treatment BAI Scores

"Efficacy of the intake of Lpc-37 on the reduction of Beck Anxiety Inventory (BAI) scores compared to placebo.~Measured with the german version of the Beck Anxiety Inventory as a self-rating scale designed to measure anxiety. It comprises 21 sentences describing feelings that can occur when being anxious. These sentences are rated on a four-point rating scale ranging from 0=not at all to 3=severely, considering the last 7 days. The score range is 0-63; Higher scores indicate higher anxiety." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-375.514.75
Placebo5.856.33

Changes in Pre and Post Treatment DASS Anxiety Scores

"Efficacy of the intake of Lpc-37 on the reduction of Depression Anxiety Stress Scale (DASS) anxiety scores compared to placebo.~Measured with the german version of the DASS as a 42-item self report instrument designed to measure negative emotional states of depression, anxiety and stress during the past week. The DASS includes three scales (depression, anxiety and stress) of which each scale includes 14 items that are divided into subscales of 2-5 items of similar content.~Items are answered on a four point rating scale ranging from 0 = not at all to 3 = very much. Scores of each scale are calculated by summing the scores for the relevant items.~The anxiety scale assesses autonomic arousal, skeletal muscle effects, situational anxiety, and subjective experience of anxious affect. The items are 2, 4, 7, 9, 15, 19, 20, 23, 25, 28, 30, 36, 40, 41 and individual scores can range from 0 to 42 with higher scores indicating greater severity of the symptoms." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-372.602.44
Placebo3.073.45

Changes in Pre and Post Treatment DASS Depression Scores

"Efficacy of the intake of Lpc-37 on the reduction of Depression Anxiety Stress Scale (DASS) depression scores compared to placebo.~Measured with the german version of the DASS as a 42-item self report instrument designed to measure negative emotional states of depression, anxiety and stress during the past week. The DASS includes three scales (depression, anxiety and stress) of which each scale includes 14 items that are divided into subscales of 2-5 items of similar content.~Items are answered on a four point rating scale ranging from 0 = not at all to 3 = very much. Scores of each scale are calculated by summing the scores for the relevant items.~The Depression scale assesses dysphoria, hopelessness, devaluation of life, self-deprecation, lack of interest/involvement, anhedonia, and inertia. The items are 3, 5, 10, 13, 16, 17, 21, 24, 26, 31, 34, 37, 38, 42 and individual scores can range from 0 to 42 with higher scores indicating greater severity of the symptoms." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-374.604.15
Placebo5.215.10

Changes in Pre and Post Treatment DASS Stress Scores

"Efficacy of the intake of Lpc-37 on the reduction of Depression Anxiety Stress Scale (DASS) stress scores compared to placebo.~Measured with the german version of the DASS as a 42-item self report instrument designed to measure negative emotional states of depression, anxiety and stress during the past week. The DASS includes three scales (depression, anxiety and stress) of which each scale includes 14 items that are divided into subscales of 2-5 items of similar content.~Items are answered on a four point rating scale ranging from 0 = not at all to 3 = very much. Scores of each scale are calculated by summing the scores for the relevant items.~The stress scale (items) is sensitive to levels of chronic non-specific arousal.The stress scale items are 1, 6, 8, 11, 12, 14, 18, 22, 27, 29, 32, 33, 35, 39 and individual scores can range from 0 to 42 with higher scores indicating greater severity of the symptoms." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-379.768.91
Placebo9.4110.09

Changes in Pre and Post Treatment Diastolic BP

Efficacy of the intake of Lpc-37 on the reduction of diastolic BP. (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
InterventionmmHg (Mean)
BaselineEnd of Study
Lpc-3771.8973.18
Placebo71.6874.62

Changes in Pre and Post Treatment Perceived Stress Scale (PSS) Scores

"Efficacy of the intake of Lpc-37 on the reduction of Perceived Stress Scale (PSS) scores compared to placebo.~Measured with the german version of the PSS as a psychological instrument for measuring stress perception. It assesses how unpredictable, uncontrollable and overloaded participants perceived their lives to have been within the last month. The PSS comprises 14 items that are answered on a five-point rating scale ranging from 0 = never to 4 = very often. Individual scores on the PSS can range from 0 to 56 with higher scores indicating higher perceived stress." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-3721.8920.49
Placebo20.7221.56

Changes in Pre and Post Treatment STAI-state Scores

"Efficacy of the intake of Lpc-37 on the reduction of State-Trait-Anxiety-Inventory (STAI)-state scores compared to placebo.~Measured with the german version of the State-Trait-Anxiety Inventory, scale anxiety as a temporary emotional state (STAI-X1). Answers are given on a four-point rating scale ranging from 1=not at all to 4=very true. The score range is 20-80; Higher scores indicate more anxiety." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-3733.6535.18
Placebo34.3335.33

Changes in Pre and Post Treatment Systolic BP

Efficacy of the intake of Lpc-37 on the reduction of systolic blood pressure (BP). (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
InterventionmmHg (Mean)
BaselineEnd of Study
Lpc-37119.60121.87
Placebo119.66122.86

Changes in Pre and Post Treatment VAS Anxiety Scores

"Efficacy of the intake of Lpc-37 on the reduction of VAS anxiety scores compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating greater anxiety." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-377.299.26
Placebo7.587.85

Changes in Pre and Post Treatment VAS Exhaustion Scores

"Efficacy of the intake of Lpc-37 on the reduction of VAS exhaustion scores compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating greater exhaustion." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-3729.5624.66
Placebo23.1918.45

Changes in Pre and Post Treatment VAS Insecurity Scores

"Efficacy of the intake of Lpc-37 on the reduction of VAS insecurity scores compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating greater insecurity." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-3713.5816.44
Placebo15.9117.30

Changes in Pre and Post Treatment VAS Stress Perception Scores

"Efficacy of the intake of Lpc-37 on the reduction of Visual Analog Scale (VAS) stress perception scores compared to placebo.~Measured with a german version of the Visual Analog Scale (VAS) as a 10cm bipolar scale ranging from not at all to highly. The participant indicated his/her actual perception by placing a mark on a line. VAS scores were obtained by using a ruler and measuring the position of the participants's mark with millimeter precision. To control for possible variations due to printing, the total length of the line was also measured and percentage scores for each participant were computed. Percentage scores range from 0-100. Higher scores indicating higher perceived stress." (NCT03494725)
Timeframe: Before and after 5 weeks of study product intake.

,
Interventionscore (Mean)
BaselineEnd of Study
Lpc-3719.1123.32
Placebo19.3420.67

The Change of the Difference From Baseline and 5 Weeks of Treatment to the Respective Mean of CAR 8pm Measures

"Efficacy of the intake of Lpc-37 on the reduction of the difference of cortisol at 8 pm values to the respective mean before and after 5 weeks of treatment~Efficacy for the CAR variable cortisol at 8 pm is defined in terms of a normalization: Number of participants with normal values (between first and third quantile of reference measures) and numbers of participants with low or high values are compared before treatment and after treatment. More participants in the normal range after treatment is defined as efficacy." (NCT03494725)
Timeframe: Baseline (average of 2 days before first product intake) and end of study (average of 2 days before last product intake

,
Interventionnumber of participants (Number)
Baseline (<25% quantile)Baseline (25% - 75% quantile)Baseline (>75% quantile)End of Study (<25% quantile)End of Study (25% - 75% quantile)End of Study (>75% quantile)
Lpc-374202932822
Placebo6232671830

The Change of the Difference From Baseline and 5 Weeks of Treatment to the Respective Mean of CAR AUCg Measures

"Efficacy of the intake of Lpc-37 on the reduction of the difference of Cortisol Awakening Response (CAR) area under the curve with respect to the ground (AUCg) values to the respective mean before and after 5 weeks of treatment.~The CAR is summarized in the variables AUCg, AUCi, mean increase and peak value. These cortisol indices are frequently used to describe hypothalamic-pituitary-adrenal axis activity and represent information either of the total cortisol production or of the change in cortisol levels. AUCg is the total area under the curve of all measurements (i.e., the intensity or magnitude of the response).~Efficacy for the CAR variables AUCg is defined in terms of a normalization: Number of participants with normal values (between first and third quantile of reference measures) and numbers of participants with low or high values are compared before treatment and after treatment. More participants in the normal range after treatment is defined as efficacy." (NCT03494725)
Timeframe: Baseline (average of 2 days before first product intake) and end of study (average of 2 days before last product intake)

,
Interventionnumber of participants (Number)
Baseline (<25% quantile)Baseline (25% - 75% quantile)Baseline (>75% quantile)End of Study (<25% quantile)End of Study (25% - 75% quantile)End of Study (>75% quantile)
Lpc-3763611112814
Placebo12301373513

The Change of the Difference From Baseline and 5 Weeks of Treatment to the Respective Mean of Cortisol at Awakening Measures

"Efficacy of the intake of Lpc-37 on the reduction of the difference of Cortisol at Awakening values to the respective mean before and after 5 weeks of treatment~Efficacy for the CAR variable cortisol at awakening is defined in terms of a normalization: Number of participants with normal values (between first and third quantile of reference measures) and numbers of participants with low or high values are compared before treatment and after treatment. More participants in the normal range after treatment is defined as efficacy." (NCT03494725)
Timeframe: Baseline (average of 2 days before first product intake) and end of study (average of 2 days before last product intake)

,
Interventionnumber of participants (Number)
Baseline (<25% quantile)Baseline (25% - 75% quantile)Baseline (>75% quantile)End of Study (<25% quantile)End of Study (25% - 75% quantile)End of Study (>75% quantile)
Lpc-371431819268
Placebo16261312349

The Change of the Difference From Baseline and 5 Weeks of Treatment to the Respective Mean of Cortisol Awakening Response (CAR) AUCi Measures

"Efficacy of the intake of Lpc-37 on the reduction of the difference of CAR area under the curve with respect to the increase (AUCi) values to the respective mean before and after the treatment.~The CAR is summarized in the variables AUCg, AUCi, mean increase and peak value. These cortisol indices are frequently used to describe hypothalamic-pituitary-adrenal axis activity and represent information either of the total cortisol production or of the change in cortisol levels. AUCi is calculated with reference to the baseline measurement and it ignores the distance from zero for all measurements and emphasizes the changes over time. Efficacy for the CAR variables AUCi is defined in terms of a normalization: Number of participants with normal values (between first and third quantile of reference measures) and numbers of participants with low or high values are compared before treatment and after treatment. More participants in the normal range after treatment is defined as efficacy." (NCT03494725)
Timeframe: Baseline (average of 2 days before first product intake) and end of study (average of 2 days before last product intake)

,
Interventionnumber of participants (Number)
Baseline (<25% quantile)Baseline (25% - 75% quantile)Baseline (>75% quantile)End of Study (<25% quantile)End of Study (25% - 75% quantile)End of Study (>75% quantile)
Lpc-371634315344
Placebo2228515364

Reviews

4 reviews available for corticosterone and Behavior Disorders

ArticleYear
Hypothalamic-pituitary-adrenal axis targets for the treatment of epilepsy.
    Neuroscience letters, 2021, 02-16, Volume: 746

    Topics: Adrenocorticotropic Hormone; Animals; Anticonvulsants; Corticosterone; Desoxycorticosterone; Epileps

2021
Sex-dependent alterations in response to maternal deprivation in rats.
    Psychoneuroendocrinology, 2009, Volume: 34 Suppl 1

    Topics: Animals; Animals, Newborn; Behavior, Animal; Body Weight; Brain; Cannabinoid Receptor Modulators; Ch

2009
The liver-cytokine-brain circuit in interferon-based treatment of patients with chronic viral hepatitis.
    Journal of viral hepatitis, 2011, Volume: 18, Issue:8

    Topics: Adrenocorticotropic Hormone; Antiviral Agents; Brain; Central Nervous System Viral Diseases; Cortico

2011
Early adverse experience as a developmental risk factor for later psychopathology: evidence from rodent and primate models.
    Development and psychopathology, 2001,Summer, Volume: 13, Issue:3

    Topics: Adrenocorticotropic Hormone; Age Factors; Animals; Animals, Newborn; Anxiety; Behavior, Animal; Cort

2001

Trials

1 trial available for corticosterone and Behavior Disorders

ArticleYear
Corticosteroids in psychiatric patients: subacute and diurnal effects on free fatty acid and catecholamine metabolism.
    Journal of psychiatric research, 1973, Volume: 10, Issue:1

    Topics: Catecholamines; Circadian Rhythm; Corticosterone; Dexamethasone; Epinephrine; Fatty Acids, Nonesteri

1973

Other Studies

28 other studies available for corticosterone and Behavior Disorders

ArticleYear
Atypical antipsychotic drug modulates early life infection induced impairment of hypothalamic-pituitary-adrenal axis: An age related study in mice.
    European journal of pharmacology, 2020, Apr-05, Volume: 872

    Topics: Adolescent; Adrenocorticotropic Hormone; Adult; Age Factors; Animals; Antipsychotic Agents; Chromaff

2020
p-Cresol Sulfate Caused Behavior Disorders and Neurodegeneration in Mice with Unilateral Nephrectomy Involving Oxidative Stress and Neuroinflammation.
    International journal of molecular sciences, 2020, Sep-12, Volume: 21, Issue:18

    Topics: Animals; Brain-Derived Neurotrophic Factor; Carbon; Cell Survival; Corticosterone; Cresols; Inflamma

2020
A Protocol for Generation of a Corticosterone Model of Psychiatric Disorders.
    Advances in experimental medicine and biology, 2017, Volume: 974

    Topics: Animals; Corticosterone; Disease Models, Animal; Drug Implants; Electrophoresis, Gel, Two-Dimensiona

2017
Cyclical corticosterone administration sensitizes depression-like behavior in rats.
    Neuroscience letters, 2017, 05-22, Volume: 650

    Topics: Animals; Behavior, Animal; Corticosterone; Depressive Disorder; Disease Models, Animal; Dose-Respons

2017
Endocrine active metals, prenatal stress and enhanced neurobehavioral disruption.
    Hormones and behavior, 2018, Volume: 101

    Topics: Animals; Animals, Newborn; Arsenic; Behavior, Animal; Corticosterone; Endocrine Disruptors; Female;

2018
Multimodal early-life stress induces biological changes associated to psychopathologies.
    Hormones and behavior, 2018, Volume: 100

    Topics: Animals; Animals, Newborn; Anxiety Disorders; Corticosterone; Depressive Disorder; Female; Hippocamp

2018
Behavioral deficits, abnormal corticosterone, and reduced prefrontal metabolites of adolescent rats subject to early life stress.
    Neuroscience letters, 2013, Jun-17, Volume: 545

    Topics: Aging; Animals; Corticosterone; Depression; Female; Male; Maternal Deprivation; Mental Disorders; Pr

2013
Transient downregulation of Dab1 protein levels during development leads to behavioral and structural deficits: relevance for psychiatric disorders.
    Neuropsychopharmacology : official publication of the American College of Neuropsychopharmacology, 2014, Volume: 39, Issue:3

    Topics: Animals; Animals, Newborn; Antipsychotic Agents; beta-Galactosidase; Brain; Clozapine; Corticosteron

2014
Tracing the trajectory of behavioral impairments and oxidative stress in an animal model of neonatal inflammation.
    Neuroscience, 2015, Jul-09, Volume: 298

    Topics: Age Factors; Animals; Animals, Newborn; Corticosterone; Developmental Disabilities; Disease Progress

2015
Long-lasting monoaminergic and behavioral dysfunctions in a mice model of socio-environmental stress during adolescence.
    Behavioural brain research, 2017, 01-15, Volume: 317

    Topics: Adrenal Glands; Animals; Biogenic Monoamines; Brain; Circadian Rhythm; Corticosterone; Dark Adaptati

2017
Neonatal interventions differently affect maternal care quality and have sexually dimorphic developmental effects on corticosterone secretion.
    International journal of developmental neuroscience : the official journal of the International Society for Developmental Neuroscience, 2016, Volume: 55

    Topics: Age Factors; Analysis of Variance; Animals; Animals, Newborn; Brain-Derived Neurotrophic Factor; Cor

2016
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Early life stress alters behavior, immunity, and microbiota in rats: implications for irritable bowel syndrome and psychiatric illnesses.
    Biological psychiatry, 2009, Feb-01, Volume: 65, Issue:3

    Topics: Animals; Animals, Newborn; Colon; Corticosterone; Cytokines; DNA, Bacterial; Electrophoresis, Polyac

2009
Susceptibility to stress in young rats after 2-week zinc deprivation.
    Neurochemistry international, 2010, Volume: 56, Issue:3

    Topics: Animals; Brain Chemistry; Corticosterone; Depressive Disorder; Dietary Supplements; Disease Models,

2010
Hypogonadism predisposes males to the development of behavioural and neuroplastic depressive phenotypes.
    Psychoneuroendocrinology, 2011, Volume: 36, Issue:9

    Topics: Animals; Corticosterone; Depressive Disorder; Disease Progression; Disease Susceptibility; Exercise

2011
Corticosterone alters N-methyl-D-aspartate receptor subunit mRNA expression before puberty.
    Brain research. Molecular brain research, 2003, Jul-04, Volume: 115, Issue:1

    Topics: Adolescent; Adrenalectomy; Animals; Brain; Corticosterone; Gene Expression Regulation; Hippocampus;

2003
Attenuated stress responsiveness in an animal model for neurodevelopmental psychopathological disorders.
    European neuropsychopharmacology : the journal of the European College of Neuropsychopharmacology, 2003, Volume: 13, Issue:4

    Topics: Adrenocorticotropic Hormone; Amygdala; Animals; Animals, Newborn; Attention; Behavior, Animal; Catec

2003
[On the mechanism of corticosterone cumulation in the regenerating rat adrenal during stress].
    Comptes rendus des seances de la Societe de biologie et de ses filiales, 1962, Volume: 156

    Topics: Adrenal Cortex Hormones; Adrenal Glands; Animals; Corticosterone; Mental Disorders; Rats; Stress, Ph

1962
[EFFECTS OF X-IRRADIATION ON ADRENAL FUNCTION IN RATS].
    Nihon seirigaku zasshi. Journal of the Physiological Society of Japan, 1963, Volume: 25

    Topics: Adrenocorticotropic Hormone; Blood Chemical Analysis; Corticosterone; Mental Disorders; Pituitary-Ad

1963
CHANGES IN PITUITARY CORTICOTROPHIC FUNCTION IN THE ADRENALECTOMIZED RAT.
    The Journal of physiology, 1964, Volume: 173

    Topics: Adrenalectomy; Adrenocorticotropic Hormone; Corticosterone; Mental Disorders; Pharmacology; Physiolo

1964
Protective effect of Triphala on cold stress-induced behavioral and biochemical abnormalities in rats.
    Yakugaku zasshi : Journal of the Pharmaceutical Society of Japan, 2007, Volume: 127, Issue:11

    Topics: Animals; Behavior, Animal; Cold Temperature; Corticosterone; Disease Models, Animal; Lipid Peroxidat

2007
Alteration in circadian rhythm of plasma corticosterone in rats following sociopsychological stress induced by communication box.
    Physiology & behavior, 1995, Volume: 57, Issue:1

    Topics: Animals; Behavior, Animal; Body Weight; Circadian Rhythm; Corticosterone; Disease Models, Animal; El

1995
Interleukin-2 and -6 induce behavioral-activating effects in mice.
    Brain research, 1998, Nov-16, Volume: 811, Issue:1-2

    Topics: Adaptation, Physiological; Animals; Behavior, Animal; Corticosterone; Exploratory Behavior; Interleu

1998
Effects of adverse experiences for brain structure and function.
    Biological psychiatry, 2000, Oct-15, Volume: 48, Issue:8

    Topics: Adult; Animals; Atrophy; Brain; Corticosterone; Dendrites; Dentate Gyrus; Hippocampus; Humans; Male;

2000
Deviant forms of aggression in glucocorticoid hyporeactive rats: a model for 'pathological' aggression?
    Journal of neuroendocrinology, 2001, Volume: 13, Issue:1

    Topics: Adrenalectomy; Aggression; Animals; Anti-Inflammatory Agents; Behavior, Animal; Corticosterone; Dise

2001
Adrenocortical and behavioral responses to repeated stressors: toward an animal model of chronic stress and stress-related mental illness.
    Biological psychiatry, 1989, Volume: 26, Issue:8

    Topics: Adrenal Cortex; Animals; Arousal; Behavior, Animal; Body Weight; Corticosterone; Disease Models, Ani

1989
Plasma corticosterone and cortisol following dexamethasone in psychiatric patients.
    Psychoneuroendocrinology, 1985, Volume: 10, Issue:1

    Topics: Bipolar Disorder; Corticosterone; Depressive Disorder; Dexamethasone; Humans; Hydrocortisone; Hypoth

1985
Neuroendocrinological studies in mental disorders and psychotropic drugs. I. On the circadian rhythm of the plasma adrenocortical hormone in mental patients and methamphetamine- and chlorpromazine-treated animals.
    Folia psychiatrica et neurologica japonica, 1969, Volume: 23, Issue:2

    Topics: 17-Hydroxycorticosteroids; Adrenocorticotropic Hormone; Adult; Animals; Chlorpromazine; Circadian Rh

1969
Neuropsychiatric problems in systemic lupus erythematosus.
    British medical journal, 1972, Nov-11, Volume: 4, Issue:5836

    Topics: Adolescent; Adult; Cognition Disorders; Corticosterone; Cranial Nerves; Depression; Epilepsy; Female

1972