Your search keyword '"GABA Modulators adverse effects"' showing total 187 results

1. Reversal of Benzodiazepine-Induced Myoclonus by Flumazenil in the Neonatal Intensive Care Unit.

Author

D'Onofrio G and Major P

Subjects

Humans, Infant, Newborn, GABA Modulators therapeutic use, GABA Modulators adverse effects, Male, Female, Antidotes, Flumazenil therapeutic use, Myoclonus chemically induced, Benzodiazepines adverse effects, Intensive Care Units, Neonatal

Abstract

Competing Interests: None declared.

Published

2024

2. Dimdazenil: First Approval.

Author

Syed YY

Subjects

Humans, China, GABA Modulators pharmacology, GABA Modulators therapeutic use, GABA Modulators adverse effects, GABA Modulators administration & dosage, Receptors, GABA-A metabolism, Receptors, GABA-A drug effects, Administration, Oral, Flumazenil pharmacology, Flumazenil therapeutic use, Drug Approval, Sleep Initiation and Maintenance Disorders drug therapy

Abstract

Dimdazenil (Junoenil ® ) is a small-molecule, oral, partial positive allosteric modulator of the gamma-aminobutyric acid (GABA) A receptor that is being developed by Zhejiang Jingxin Pharmaceutical in collaboration with Evotec for the treatment of insomnia. Dimdazenil is designed to overcome issues associated with full GABA A receptor agonists, such as tolerance, withdrawal symptoms and associated adverse effects. On 29 November 2023, dimdazenil oral capsules received approval in China for the short-term treatment of insomnia. This article summarizes the milestones in the development of dimdazenil leading to this first approval for insomnia., (© 2024. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published

2024

3. Effect of Zuranolone vs Placebo in Postpartum Depression: A Randomized Clinical Trial.

Author

Deligiannidis KM, Meltzer-Brody S, Gunduz-Bruce H, Doherty J, Jonas J, Li S, Sankoh AJ, Silber C, Campbell AD, Werneburg B, Kanes SJ, and Lasser R

Subjects

Adolescent, Adult, Double-Blind Method, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, Humans, Middle Aged, Outcome Assessment, Health Care, Postpartum Period, Pregnancy, Pregnancy Trimester, Third, Pregnanes administration & dosage, Pregnanes adverse effects, Pyrazoles administration & dosage, Pyrazoles adverse effects, Young Adult, Depression, Postpartum drug therapy, Depressive Disorder, Major drug therapy, GABA Modulators pharmacology, Pregnanes pharmacology, Pyrazoles pharmacology

Abstract

Importance: Postpartum depression (PPD) is one of the most common medical complications during and after pregnancy, negatively affecting both mother and child., Objective: To demonstrate the efficacy and safety of zuranolone, a neuroactive steroid γ-aminobutyric acid receptor-positive allosteric modulator, in PPD., Design, Setting, and Participants: This phase 3, double-blind, randomized, outpatient, placebo-controlled clinical trial was conducted between January 2017 and December 2018 in 27 enrolling US sites. Participant were women aged 18 to 45 years, 6 months or fewer post partum, with PPD (major depressive episode beginning third trimester or ≤4 weeks postdelivery), and baseline 17-item Hamilton Rating Scale for Depression (HAMD-17) score of 26 or higher. Analysis was intention to treat and began December 2018 and ended March 2019., Interventions: Randomization 1:1 to placebo:zuranolone, 30 mg, administered orally each evening for 2 weeks., Main Outcomes and Measures: Primary end point was change from baseline in HAMD-17 score for zuranolone vs placebo at day 15. Secondary end points included changes from baseline in HAMD-17 total score at other time points, HAMD-17 response (≥50% score reduction) and remission (score ≤7) rates, Montgomery-Åsberg Depression Rating Scale score, and Hamilton Rating Scale for Anxiety score. Safety was assessed by adverse events and clinical assessments., Results: Of 153 randomized patients, the efficacy set comprised 150 patients (mean [SD] age, 28.3 [5.4] years), and 148 (98.7%) completed treatment. A total of 76 patients were randomized to placebo, and 77 were randomized to zuranolone, 30 mg. Zuranolone demonstrated significant day 15 HAMD-17 score improvements from baseline vs placebo (-17.8 vs -13.6; difference, -4.2; 95% CI, -6.9 to -1.5; P = .003). Sustained differences in HAMD-17 scores favoring zuranolone were observed from day 3 (difference, -2.7; 95% CI, -5.1 to -0.3; P = .03) through day 45 (difference, -4.1; 95% CI, -6.7 to -1.4; P = .003). Sustained differences at day 15 favoring zuranolone were observed in HAMD-17 response (odds ratio, 2.63; 95% CI, 1.34-5.16; P = .005), HAMD-17 score remission (odds ratio, 2.53; 95% CI, 1.24-5.17; P = .01), change from baseline for Montgomery-Åsberg Depression Rating Scale score (difference, -4.6; 95% CI, -8.3 to -0.8; P = .02), and Hamilton Rating Scale for Anxiety score (difference, -3.9; 95% CI, -6.7 to -1.1; P = .006). One patient per group experienced a serious adverse event (confusional state in the zuranolone group and pancreatitis in the placebo group). One patient in the zuranolone group discontinued because of an adverse event vs none for placebo., Conclusions and Relevance: In this randomized clinical trial, zuranolone improved the core symptoms of depression as measured by HAMD-17 scores in women with PPD and was generally well tolerated, supporting further development of zuranolone in the treatment of PPD., Trial Registration: ClinicalTrials.gov Identifier: NCT02978326.

Published

2021

4. Safety, Tolerability, and Pharmacokinetics of Multiple Repeated Oral Doses of the α2/3/5-Subtype Selective GABA A -Positive Allosteric Modulator PF-06372865 in Healthy Volunteers.

Author

Gurrell R, Whitlock M, Wei H, Shen Z, and Ogden A

Subjects

Administration, Oral, Adult, Area Under Curve, Cohort Studies, Dose-Response Relationship, Drug, Double-Blind Method, Female, GABA Modulators adverse effects, GABA Modulators pharmacokinetics, Half-Life, Humans, Imidazoles adverse effects, Imidazoles pharmacokinetics, Male, Middle Aged, Pyridazines adverse effects, Pyridazines pharmacokinetics, GABA Modulators administration & dosage, Imidazoles administration & dosage, Pyridazines administration & dosage

Abstract

Multiple-dose pharmacokinetics (PK) and safety were investigated in this phase 1 study of PF-06372865, a positive allosteric modulator of α2/3/5 subunit-containing γ-aminobutyric acid A receptors (NCT03351751). In 2 cohorts (7-8 PF-06372865 and 2 placebo in each cohort), healthy adult subjects received twice-daily oral doses of PF-06372865 for 21 days, which included titration in the first 7 days, followed by a maintenance dose of 25 mg twice daily (Cohort 1) and 42.5 mg twice daily (Cohort 2) for 14 days. Serial PK samples were collected on days 1 and 21. Nineteen subjects were assigned to study treatments; 18 completed the study. Approximate dose-proportional increases in maximum plasma concentratin and area under the plasma concentration-time curve over the dosing interval were observed. PF-06372865 was rapidly absorbed with a median time to maximum concentration of 1 to 2 hours following both single- and multiple-dose administration. Mean terminal elimination half-life on day 21 was approximately 11 hours in both cohorts. All adverse events were mild; the most frequently reported was dizziness. After titration, there were no reports of somnolence. There were no clinically significant safety findings, including a lack of withdrawal symptoms on discontinuation of treatment. These results demonstrate that PF-06372865 is safe and well tolerated at doses estimated to achieve high receptor occupancy (>80%), a profile differentiated from nonselective benzodiazepines., (© 2021 Cerevel Therapeutics. Clinical Pharmacology in Drug Development published by Wiley Periodicals LLC on behalf of American College of Clinical Pharmacology.)

Published

2021

5. Pharmacological uses of flumazenil in benzodiazepine use disorders: a systematic review of limited data.

Author

Gallo AT and Hulse G

Subjects

Benzodiazepines administration & dosage, Flumazenil adverse effects, Flumazenil pharmacology, GABA Modulators administration & dosage, GABA Modulators adverse effects, GABA Modulators pharmacology, Humans, Randomized Controlled Trials as Topic, Substance Withdrawal Syndrome drug therapy, Benzodiazepines adverse effects, Flumazenil administration & dosage, Substance-Related Disorders drug therapy

Abstract

Background: The estimated annual prevalence of drug use disorders is as high as 3%, underpinning the need to continually develop more effective treatments. Central nervous system dysregulation, contributing to acute and post-withdrawal syndromes, has traditionally been managed with benzodiazepines; however, a small but growing body of data indicate that the GABA A receptor antagonist, flumazenil, may offer some advantages over traditional management., Aim: To review the literature on the safety and efficacy of flumazenil in benzodiazepine use disorders and identify gaps in the literature., Method: A systematic method was used to identify randomised control trials. Where randomised control trials existed, non-randomised control trials were included to supplement findings., Results: Eleven flumazenil trials were included with varying doses, frequencies and routes of administration. The evidence for flumazenil alone showed generally a reduction in withdrawal symptoms with the exception of one study where withdrawal symptoms initially increased. Flumazenil plus benzodiazepine tapering was assessed in one randomised control trial and a series of non-randomised control trials. Randomised control trial results showed that flumazenil plus benzodiazepine tapering was superior at reducing withdrawal symptoms compared to benzodiazepine tapering alone and placebo. Flumazenil was associated with no serious adverse events; however there remains a risk of seizures., Conclusion: Although flumazenil shows promising efficacy in the management of benzodiazepine use disorders and withdrawal, more randomized control trials are required before a definitive recommendation can be made around its use.

Published

2021

6. A randomized phase 1 single-dose polysomnography study of ASP8062, a GABA B receptor positive allosteric modulator.

Author

Walzer M, Wu R, Ahmad M, Freeman J, Zammit G, and Marek GJ

Subjects

Adult, Electroencephalography drug effects, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, GABA Modulators pharmacokinetics, Humans, Male, Middle Aged, Morpholines administration & dosage, Morpholines adverse effects, Morpholines pharmacokinetics, Paroxetine pharmacology, Pyrimidines administration & dosage, Pyrimidines adverse effects, Pyrimidines pharmacokinetics, Sleep Initiation and Maintenance Disorders psychology, GABA Modulators therapeutic use, Morpholines therapeutic use, Polysomnography drug effects, Pyrimidines therapeutic use, Receptors, GABA-B metabolism, Sleep Initiation and Maintenance Disorders drug therapy, Sleep, REM drug effects, Sleep, Slow-Wave drug effects

Abstract

Rationale: Previous research suggests that sleep polysomnography and EEG endpoints can be used to assess GABAergic activity; however, the impact of GABA B receptor positive allosteric modulators on sleep endpoints remains unclear., Objectives: This phase 1 study compared a single dose of ASP8062 (35 mg or 70 mg), a GABA B receptor positive allosteric modulator, with placebo and paroxetine (40 mg)., Methods: Healthy adult volunteers were randomized to four treatments (35 mg ASP8062, 70 mg ASP8062, paroxetine 40 mg, or matching placebo), each separated by a 14-day washout. Primary endpoints obtained by polysomnography were time in stage N3 or SWS and time in rapid eye movement (REM) sleep. Secondary endpoints included impact on sleep stages and electroencephalography parameters, pharmacokinetics, nighttime growth hormone (GH), and safety/tolerability., Results: In 20 randomized volunteers, ASP8062 led to a significant and seemingly dose-dependent increase in SWS over the entire night; this increase was mainly observed during the first third of the night. ASP8062 did not impact time in REM sleep. Paroxetine had no effect on SWS but produced a significant reduction in time spent in REM sleep. A dose-dependent trend in increased GH release was also observed with ASP8062. Headache and nausea were the most commonly reported treatment-emergent adverse events (TEAEs) for ASP8062; most TEAEs were mild in severity., Conclusions: Single-dose ASP8062 (35 and 70 mg) appeared to result in CNS penetration and enhanced GABAergic activity as measured by increases in slow-wave sleep and growth hormone release.

Published

2021

7. Recurrent Suicidal Ideation With Topiramate in Tourette Syndrome.

Author

Sarwar S, Sinha A, and Jolly T

Subjects

Adolescent, GABA Modulators administration & dosage, GABA Modulators adverse effects, Humans, Male, Topiramate administration & dosage, Suicidal Ideation, Topiramate adverse effects, Tourette Syndrome drug therapy

Published

2021

8. A Systematic Review of Intravaginal Diazepam for the Treatment of Pelvic Floor Hypertonic Disorder.

Author

Stone RH, Abousaud M, Abousaud A, and Kobak W

Subjects

Administration, Intravaginal, Female, Humans, Off-Label Use, Pelvic Pain drug therapy, Sexual Dysfunction, Physiological drug therapy, Diazepam administration & dosage, Diazepam adverse effects, GABA Modulators administration & dosage, GABA Modulators adverse effects, Muscle Hypertonia drug therapy, Pelvic Floor physiopathology, Pelvic Floor Disorders drug therapy

Abstract

This systematic review evaluates the efficacy of intravaginal diazepam in treating chronic pelvic pain and sexual dysfunction associated with high-tone pelvic floor dysfunction. A literature search was conducted in Medline and Web of Science, including articles from the database's inception to July 2019. The search identified 126 articles, and 5 articles met study inclusion criteria: 2 observational reviews and 3 small randomized, controlled trials (RCTs) evaluating intravaginal diazepam for high-tone pelvic floor dysfunction. The 2 observational studies identified subjective reports of improvement in sexual function for a majority of women, 96% and 71%, in each study. However, there were no statistical differences between Female Sexual Function Index (FSFI) and Visual Analog Scale (VAS) scores for pain identified. One RCT found no significant changes between groups in median FSFI or VAS scores, and a second RCT found no significant changes between groups in 100-mm VAS scores. The third RCT demonstrated that compared with placebo, treatment with transcutaneous electrical nerve stimulation and intravaginal diazepam for women with vestibulodynia and high-tone pelvic floor dysfunction yielded significant differences in reduction of dyspareunia (P ≤ .05), ability to relax pelvic floor muscles after contraction (P ≤.05), and current perception threshold values at a 5-Hz stimulation related to C fibers (P < .05), but no significant changes in 10-cm VAS scores. Intravaginal diazepam may be helpful in women with a specific diagnosis of high-tone pelvic floor dysfunction, but more and larger studies are needed to confirm these potential effects., (© 2020, The American College of Clinical Pharmacology.)

Published

2020

9. Safety and efficacy of midazolam nasal spray for the treatment of intermittent bouts of increased seizure activity in the epilepsy monitoring unit: A double-blind, randomized, placebo-controlled trial.

Author

Spencer DC, Sinha SR, Choi EJ, Cleveland JM, King A, Meng TC, Pullman WE, Sequeira DJ, Van Ess PJ, and Wheless JW

Subjects

Administration, Intranasal, Adolescent, Adult, Anticonvulsants administration & dosage, Anticonvulsants adverse effects, Child, Double-Blind Method, Epilepsy diagnosis, Epilepsy physiopathology, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, Headache chemically induced, Humans, Male, Midazolam adverse effects, Middle Aged, Seizures diagnosis, Seizures physiopathology, Treatment Outcome, Young Adult, Epilepsy drug therapy, Midazolam administration & dosage, Monitoring, Physiologic methods, Nasal Sprays, Seizures drug therapy

Abstract

Objective: Midazolam nasal spray (MDZ-NS) is indicated for acute treatment of intermittent, stereotypic episodes of frequent seizure activity (ie, seizure clusters, acute repetitive seizures) that are distinct from a patient's usual seizure pattern, in patients 12 years of age and older with epilepsy. This trial evaluated safety and efficacy of MDZ-NS in patients with epilepsy who were admitted to the epilepsy monitoring unit for seizure characterization/presurgical evaluation., Methods: In this randomized, double-blind, placebo-controlled phase 3 trial (P261-301; NCT01999777), eligible patients with ≥2 seizures in the 6-hour window preceding trial medication administration for whom treatment was appropriate based on investigator's judgment were randomized (1:1) to MDZ-NS 5 mg or placebo. Efficacy outcomes were proportion of patients seizure-free for 6 hours after treatment and time to first seizure within 6 hours. Safety and tolerability outcomes included treatment-emergent adverse events (TEAEs)., Results: Sixty-two patients were randomized (MDZ-NS n = 31; placebo n = 31), received trial medication, and completed the trial. A higher proportion of patients on MDZ-NS than placebo were seizure-free for 6 hours following treatment (54.8% vs 38.7%); however, the 16.1% difference was not statistically significant (P = .1972). The Kaplan-Meier curve of time to first seizure showed separation of both groups in favor of MDZ-NS from ~1.5 hours post-dose and throughout the 6-hour Treatment phase. Median time to first seizure was not estimable for MDZ-NS (>50% of patients had no seizure) and 3.9 hours for placebo (P = .1388). TEAEs with MDZ-NS were generally comparable to those with placebo. There were no deaths, serious TEAEs, or discontinuations due to TEAEs., Significance: Although the observed treatment difference may be clinically meaningful, statistical significance was not demonstrated. Results suggest that MDZ-NS 5 mg may provide improvement over placebo, with efficacy maintained for ≥6 hours post-dose. MDZ-NS was well tolerated in this population., (© 2020 International League Against Epilepsy.)

Published

2020

10. Efficacy, Tolerability, and Safety of Concentrated Intranasal Midazolam Spray as Emergency Medication in Epilepsy Patients During Video-EEG Monitoring.

Author

von Blomberg A, Kay L, Knake S, Fuest S, Zöllner JP, Reif PS, Herrmann E, Balaban Ü, Schubert-Bast S, Rosenow F, and Strzelczyk A

Subjects

Administration, Intranasal, Adolescent, Adult, Aged, Child, Child, Preschool, Electroencephalography, Emergencies, Female, GABA Modulators adverse effects, Humans, Male, Midazolam adverse effects, Middle Aged, Retrospective Studies, Young Adult, Epilepsy drug therapy, GABA Modulators administration & dosage, Midazolam administration & dosage, Status Epilepticus drug therapy

Abstract

Background: An efficient, well tolerated, and safe emergency treatment with a rapid onset of action is needed to prevent seizure clusters and to terminate prolonged seizures and status epilepticus., Objectives: This study aimed to examine the efficacy, tolerability, and safety of intranasal midazolam (in-MDZ) spray in clinical practice., Methods: In this retrospective, multicenter observational study, we evaluated all patients with peri-ictal application of in-MDZ during video-EEG monitoring at the epilepsy centers in Frankfurt and Marburg between 2 014 and 2017. For every patient, we analyzed the recurrence of any seizure or generalized tonic-clonic seizures after index seizures with and without in-MDZ administration. Treatment-emergent adverse events (TEAEs) were also evaluated., Results: In-MDZ was used in 243 patients with epilepsy (mean age 35.5 years; range 5-76 years; 46.5% female) for treatment of 459 seizures. A median dose of in-MDZ 5 mg (i.e., two puffs; range 2.5-15 mg) was administered within a median time from EEG seizure onset until in-MDZ application of 1.18 min [interquartile range (IQR) 1.27], while median time from clinical seizure onset until in-MDZ administration was 1.08 min (IQR 1.19). In-MDZ was given within 1 min after EEG seizure onset in 171 seizures. An intraindividual comparison of seizures with and without application of in-MDZ was feasible in 171 patients, demonstrating that in-MDZ reduced the occurrence of any (Cox proportional-hazard model p < 0.001) and generalized tonic-clonic seizure (Cox proportional-hazard model p = 0.0167) over a period of 24 h. The seizure-free timespan was doubled from a median of 5.0 h in controls to a median of 10.67 h after in-MDZ administration. We additionally clustered in-MDZ administrations for the 119 patients who received in-MDZ more than once, comparing them with the index cases without in-MDZ. Even when considering subsequent seizures with in-MDZ administration, a patient receiving in-MDZ is still half as likely to incur another seizure in the upcoming 24 h as compared with when the same patient does not receive in-MDZ (hazard ratio 0.50; 95% CI 0.42-0.60; p < 0.01). In-MDZ was well tolerated without major adverse events. The most common side effects were irritation of the nasal mucosa [37 cases (8.1%)], prolonged sedation [26 cases (5.7%)], and nausea and vomiting [12 cases (2.6%)]. A decline in oxygen saturation was measured after 78 seizures (17%)., Conclusion: We conclude that in-MDZ is a safe and efficient treatment option to prevent short-term recurrence of seizures. In-MDZ can be administered very quickly by trained staff within 1-2 min after seizure onset. No major cardiocirculatory or respiratory adverse events were observed.

Published

2020

11. Single- and Multiple-Dose Safety, Tolerability, and Pharmacokinetic Profiles of ASP8062: Results From 2 Phase 1 Studies.

Author

Walzer M, Marek GJ, Wu R, Nagata M, and Han D

Subjects

Administration, Oral, Adult, Area Under Curve, Dose-Response Relationship, Drug, Double-Blind Method, Female, GABA Modulators adverse effects, GABA Modulators pharmacokinetics, Half-Life, Humans, Male, Middle Aged, Morpholines adverse effects, Morpholines pharmacokinetics, Pyrimidines adverse effects, Pyrimidines pharmacokinetics, Young Adult, GABA Modulators administration & dosage, Morpholines administration & dosage, Pyrimidines administration & dosage

Abstract

ASP8062 is an orally active γ-amino-butyric acid type B (GABA B ) receptor positive allosteric modulator currently in phase 2 development. Safety and pharmacokinetic (PK) profiles of ASP8062 were evaluated in 2 studies in healthy subjects. The first study (a first-in-human study) evaluated single ascending doses (SAD) of ASP8062. The second study was composed of 2 parts: part 1 evaluated multiple ascending doses (MAD) of ASP8062 for 14 days, and part 2 was a single-dose arm to assess the PK of ASP8062 in cerebrospinal fluid (CSF). Fifty-six men (SAD) and 56 subjects (24 women and 32 men; MAD) were enrolled. Across the SAD dosing range, area under the concentration-time curve was dose proportional; increases in maximum plasma concentration appeared linear but were slightly less than dose proportional. Time to maximal concentration and half-life were 1-4 hours and ∼40-50 hours, respectively; no food effect was observed. ASP8062 PK properties at steady state were similar to those following a single dose. Steady state was achieved by ∼day 9 with ∼2-fold accumulation, and ASP8062 was detected in CSF. ASP8062 was well tolerated; no clear evidence of ASP8062's effects on safety, cognition, drug withdrawal, or suicidal ideation/behavior was observed. These data support the development of ASP8062 in indications where the GABA B receptor is a target., (© 2020, The American College of Clinical Pharmacology.)

Published

2020

12. Brexanolone Therapy for Postpartum Depression.

Author

Shabbir O, Khan KS, and Jawaid H

Subjects

Drug Combinations, Female, GABA Modulators adverse effects, Humans, Pregnanolone adverse effects, beta-Cyclodextrins adverse effects, Depression, Postpartum drug therapy, GABA Modulators therapeutic use, Pregnanolone therapeutic use, beta-Cyclodextrins therapeutic use

Published

2020

13. Cerebrospinal fluid neurotransmitter levels and central nervous system depression in a rat drug overdose model.

Author

Tsutsumi H, Yonemitsu K, Sasao A, Ohtsu Y, Furukawa S, and Nishitani Y

Subjects

Administration, Oral, Animals, Biomarkers cerebrospinal fluid, Carboxymethylcellulose Sodium administration & dosage, Carboxymethylcellulose Sodium adverse effects, Chromatography, Liquid, Diazepam administration & dosage, Diazepam adverse effects, Disease Models, Animal, GABA Modulators administration & dosage, Male, Phenobarbital administration & dosage, Phenobarbital adverse effects, Rats, Wistar, Tandem Mass Spectrometry, Drug Overdose cerebrospinal fluid, GABA Modulators adverse effects, Neurotransmitter Agents cerebrospinal fluid

Abstract

A neuropsychiatric drug overdose impairs physiological function via central nervous system (CNS) depression. In drug-related deaths, only the drug concentration can currently provide information regarding CNS depression in victims. In this study, using a drug overdose model, we investigated the ability of neurotransmitters in the cerebrospinal fluid (CSF) to serve as biomarkers for CNS depression. Four groups of rats were orally administered diazepam (200 mg/kg) and/or phenobarbital (100 mg/kg) or vehicle. In a hot plate test performed to assess physiological impairment, drug-administered animals showed prolongation of the response latency. Serum drug concentrations were also sufficient to observe the effect of drug overdose. The levels of benzoyl-derivatized neurotransmitters were measured using liquid chromatography-tandem mass spectrometry (LC-MS/MS) analysis. Noradrenaline, adrenaline, serotonin, melatonin, phosphoethanolamine, and histamine levels in the CSF decreased as the response latencies in the hot plate test increased. These reduced CSF neurotransmitter levels may represent physiological dysfunction through CNS depression.

Published

2020

14. Brexanolone for Postpartum Depression: Clinical Evidence and Practical Considerations.

Author

Leader LD, O'Connell M, and VandenBerg A

Subjects

Antidepressive Agents administration & dosage, Antidepressive Agents adverse effects, Antidepressive Agents pharmacology, Depression, Postpartum physiopathology, Drug Combinations, Female, GABA Modulators adverse effects, GABA Modulators pharmacology, Humans, Pregnancy, Pregnanolone adverse effects, Pregnanolone pharmacology, Psychiatric Status Rating Scales, Severity of Illness Index, beta-Cyclodextrins adverse effects, beta-Cyclodextrins pharmacology, Depression, Postpartum drug therapy, GABA Modulators administration & dosage, Pregnanolone administration & dosage, beta-Cyclodextrins administration & dosage

Abstract

Our aim was to review the efficacy, safety, and pharmacology of brexanolone (Zulresso), a new antidepressant with a novel mechanism of action, in the treatment of postpartum depression (PPD). Pertinent data and information were obtained via PubMed (1993 to August 2018). Articles published in English that evaluated the safety and efficacy of brexanolone and other off-label PPD treatments were included. Literature regarding epidemiology and pathophysiology of PPD was also selected. Brexanolone, administered as an intravenous infusion over 60 hours, produced a statistically significant and clinically meaningful reduction in Hamilton Depression Rating Scale (HAM-D) scores compared with placebo at both 60 and 90 μg/kg/hour in patients with moderate to severe PPD. Brexanolone groups had higher response and remission rates compared with placebo. Common adverse effects were somnolence, dizziness, and headache. A small percentage (4%) of patients required cessation of therapy due to excessive sedation or loss of consciousness. Although the evidence for brexanolone as a novel treatment for PPD looks promising, a Risk Evaluation and Mitigation Strategies (REMS) program requirement and the logistics of prolonged infusions serve as barriers to treatment. A discussion of these obstacles as well as pharmacokinetics, monitoring, and dosing is provided. Brexanolone is a novel antidepressant indicated for the treatment of PPD. Clinical trials demonstrated that brexanolone significantly reduces depression scores in women with moderate to severe PPD. Due to risk of oversedation and loss of consciousness, a REMS program will be put in place to mitigate the risk of adverse events., (© 2019 Pharmacotherapy Publications, Inc.)

Published

2019

15. The effect of early midazolam infusion on the duration of pediatric status epilepticus patients.

Author

Ulusoy E, Duman M, Türker HD, Çağlar A, Er A, Akgül F, Çitlenbik H, Öztürk A, and Yılmaz D

Subjects

Adolescent, Child, Child, Preschool, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, Humans, Infant, Male, Midazolam administration & dosage, Midazolam adverse effects, Retrospective Studies, Time Factors, Treatment Outcome, GABA Modulators pharmacology, Midazolam pharmacokinetics, Status Epilepticus drug therapy

Abstract

Purpose: Status epilepticus is one of the most common neurological emergencies in pediatric emergency departments. Although there are different approaches to treatment in the literature, early control of seizure activity is the most important factor determining prognosis. The purpose of this study was to evaluate the effect of early midazolam infusion on seizure duration., Method: This retrospective study included 150 episodes of 135 patients aged one month to 18 years old with status epilepticus. All patients were treated according to the local hospital protocol for SE, which included early midazolam infusion. Demographic data, medical history, applied treatments during SE, and seizure durations were recorded., Results: The median age of the patients (58.7% male) was 2.7 years (1.0-6.0 years). The most common identified etiologies were remote symptomatic etiologies, and generalized tonic-clonic seizure was the most common seizure type. The pediatricians had selected intravenous midazolam for 130 patients (86.7%) as the first-line therapy in emergency services. In 55 patients given continuous midazolam infusion, the cumulative bolus of midazolam was 0.5 mg/kg (0.4-0.7 mg/kg), and the median peak rate of midazolam infusion was 0.2 mg/kg/h (0.2-0.4 mg/kg/h). The median duration between the start of midazolam infusion and the complete cessation of SE was 15.0 min (9.0-25.0 min). The early-midazolam infusion group had shorter seizure duration after initiation of midazolam infusion (p = 0.020)., Conclusion: The current study shows that aggressive management of SE with early initiation of midazolam infusion was associated with a shorter seizure duration in SE patients., (Copyright © 2019 British Epilepsy Association. Published by Elsevier Ltd. All rights reserved.)

Published

2019

16. Trial of SAGE-217 in Patients with Major Depressive Disorder.

Author

Gunduz-Bruce H, Silber C, Kaul I, Rothschild AJ, Riesenberg R, Sankoh AJ, Li H, Lasser R, Zorumski CF, Rubinow DR, Paul SM, Jonas J, Doherty JJ, and Kanes SJ

Subjects

Administration, Oral, Adult, Allosteric Regulation, Antidepressive Agents adverse effects, Depressive Disorder, Major classification, Dizziness chemically induced, Double-Blind Method, Female, GABA Modulators adverse effects, Humans, Least-Squares Analysis, Male, Middle Aged, Nausea chemically induced, Pregnanes adverse effects, Psychiatric Status Rating Scales, Pyrazoles adverse effects, Antidepressive Agents therapeutic use, Depressive Disorder, Major drug therapy, GABA Modulators therapeutic use, Pregnanes therapeutic use, Pyrazoles therapeutic use, Receptors, GABA-A metabolism

Abstract

Background: Altered neurotransmission of γ-aminobutyric acid (GABA) has been implicated in the pathogenesis of depression. Whether SAGE-217, an oral, positive allosteric modulator of GABA type A receptors, is effective and safe for the treatment of major depressive disorder is unknown., Methods: In this double-blind, phase 2 trial, we enrolled patients with major depression and randomly assigned them in a 1:1 ratio to receive 30 mg of SAGE-217 or placebo once daily. The primary end point was the change from baseline to day 15 in the score on the 17-item Hamilton Depression Rating Scale (HAM-D; scores range from 0 to 52, with higher scores indicating more severe depression). Secondary efficacy end points, which were assessed on days 2 through 8 and on days 15, 21, 28, 35, and 42, included changes from baseline in scores on additional depression and anxiety scales, a reduction from baseline of more than 50% in the HAM-D score, a HAM-D score of 7 or lower, and a Clinical Global Impression of Improvement score of 1 (very much improved) or 2 (much improved) (on a scale of 1 to 7, with a score of 7 indicating that symptoms are very much worse)., Results: A total of 89 patients underwent randomization: 45 patients were assigned to the SAGE-217 group, and 44 to the placebo group. The mean baseline HAM-D score was 25.2 in the SAGE-217 group and 25.7 in the placebo group. The least-squares mean (±SE) change in the HAM-D score from baseline to day 15 was -17.4±1.3 points in the SAGE-217 group and -10.3±1.3 points in the placebo group (least-squares mean difference in change, -7.0 points; 95% confidence interval, -10.2 to -3.9; P<0.001). The differences in secondary end points were generally in the same direction as those of the primary end point. There were no serious adverse events. The most common adverse events in the SAGE-217 group were headache, dizziness, nausea, and somnolence., Conclusions: Administration of SAGE-217 daily for 14 days resulted in a reduction in depressive symptoms at day 15. Adverse events were more common in the SAGE-217 group than in the placebo group. Further trials are needed to determine the durability and safety of SAGE-217 in major depressive disorder and to compare SAGE-217 with available treatments. (Funded by Sage Therapeutics; ClinicalTrials.gov number, NCT03000530.)., (Copyright © 2019 Massachusetts Medical Society.)

Published

2019

17. Clonazepam-Related Paradoxical Behavioral Disinhibition: An Uncommon But Grave Adverse Effect.

Author

Gandotra K, Chen P, Konicki PE, and Strohl KP

Subjects

Aged, Humans, Male, Behavioral Symptoms chemically induced, Clonazepam adverse effects, GABA Modulators adverse effects, Inhibition, Psychological, Parasomnias drug therapy

Published

2019

18. Pharmacotherapy of Postpartum Depression: Current Approaches and Novel Drug Development.

Author

Frieder A, Fersh M, Hainline R, and Deligiannidis KM

Subjects

Animals, Depression, Postpartum epidemiology, Depression, Postpartum metabolism, Drug Combinations, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, Humans, Neurosteroids administration & dosage, Neurosteroids adverse effects, Pregnanes administration & dosage, Pregnanes adverse effects, Pregnanolone administration & dosage, Pregnanolone adverse effects, Pyrazoles administration & dosage, Pyrazoles adverse effects, Randomized Controlled Trials as Topic, United States, United States Food and Drug Administration, beta-Cyclodextrins administration & dosage, beta-Cyclodextrins adverse effects, Depression, Postpartum drug therapy, Drug Development, GABA Modulators therapeutic use, Neurosteroids therapeutic use, Pregnanes therapeutic use, Pregnanolone therapeutic use, Pyrazoles therapeutic use, beta-Cyclodextrins therapeutic use

Abstract

Postpartum depression is one of the most common complications of childbirth. Untreated postpartum depression can have substantial adverse effects on the well-being of the mother and child, negatively impacting child cognitive, behavioral, and emotional development with lasting consequences. There are a number of therapeutic interventions for postpartum depression including pharmacotherapy, psychotherapy, neuromodulation, and hormonal therapy among others, most of which have been adapted from the treatment of major depressive disorder outside of the peripartum period. Current evidence of antidepressant treatment for postpartum depression is limited by the small number of randomized clinical trials, underpowered samples, and the lack of long-term follow-up. The peripartum period is characterized by rapid and significant physiological change in plasma levels of endocrine hormones, peptides, and neuroactive steroids. Evidence supporting the role of neuroactive steroids and γ-aminobutyric acid (GABA) in the pathophysiology of postpartum depression led to the investigation of synthetic neuroactive steroids and their analogs as potential treatment for postpartum depression. Brexanolone, a soluble proprietary intravenous preparation of synthetic allopregnanolone, has been developed. A recent series of open-label and placebo-controlled randomized clinical trials of brexanolone in postpartum depression demonstrated a rapid reduction in depressive symptoms, and has led to the submission for regulatory approval to the US Food and Drug Administration (decision due in March 2019). SAGE-217, an allopregnanolone analog, with oral bioavailability, was recently tested in a randomized, double-blind, placebo-controlled phase III study in severe postpartum depression, with reportedly positive results. Finally, a 3β-methylated synthetic analog of allopregnanolone, ganaxolone, is being tested in both intravenous and oral forms, in randomized, double-blind, placebo-controlled phase II studies in severe postpartum depression.

Published

2019

19. Effect of single doses of pindolol and d-fenfluramine on flumazenil-induced anxiety in panic disorder patients.

Author

Bernik M, Ramos RT, Hetem LAB, and Graeff F

Subjects

Adult, Anxiety chemically induced, Anxiety etiology, Female, Flumazenil adverse effects, GABA Modulators adverse effects, Humans, Male, Middle Aged, Panic Disorder complications, Psychiatric Status Rating Scales, Regression Analysis, Young Adult, Anxiety drug therapy, Fenfluramine therapeutic use, Pindolol therapeutic use, Serotonin Antagonists therapeutic use, Selective Serotonin Reuptake Inhibitors therapeutic use

Abstract

The effects of the 5-HT 1A receptor blocker pindolol and the 5-HT releasing and uptake blocking agent d-fenfluramine, both used as indirect serotonin agonists, on flumazenil-induced acute anxiety reactions were studied in panic disorder patients to test the hypothesis that serotonin (5-HT) inhibits neural systems mediating panic attacks. Thirty never treated or drug free PD patients (16 females) aged 22-49 y (mean ± SD, 32.9 ± 8) received single doses of d-fenfluramine (n = 10; 30 mg, p.o.), pindolol (n = 10; 5 mg, p.o.), or placebo (n = 10) 90 and 45 min before a challenge test with flumazenil (1.5 mg, i.v., in 10 min), under double-blind conditions. Panic attacks occurred in 5 control subjects (placebo-flumazenil group), 5 subjects in the pindolol group and in 7 in the d-fenluramine pre-treated patients. Patients experiencing anxiety attacks following flumazenil reported higher increases in anxiety scores. Respiratory rate increases were not different between patients experiencing or not a panic attack. Despite sample size limitation, this study suggests that flumazenil induced anxiety reaction is not a good pharmacological model of panic attacks, considering the absence of serotonergic modulation of its effects., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2019

20. Biological profiling of piperazinediones for the management of anxiety.

Author

Kumar D, Gupta SK, Ganeshpurkar A, Singh R, Kumar D, Das N, Krishnamurthy S, and Singh SK

Subjects

Amygdala metabolism, Animals, Anti-Anxiety Agents administration & dosage, Anti-Anxiety Agents adverse effects, Anti-Anxiety Agents pharmacology, Behavior, Animal drug effects, Benzodiazepines chemistry, Catalytic Domain, Diazepam administration & dosage, Diazepam pharmacology, Diketopiperazines administration & dosage, Diketopiperazines adverse effects, Diketopiperazines pharmacology, Flumazenil administration & dosage, Flumazenil pharmacology, GABA Modulators administration & dosage, GABA Modulators adverse effects, GABA Modulators pharmacology, Hypnotics and Sedatives administration & dosage, Hypnotics and Sedatives pharmacology, Male, Maze Learning drug effects, Models, Animal, Norepinephrine metabolism, Rats, Rats, Wistar, Receptors, GABA-A metabolism, Serotonin metabolism, Anti-Anxiety Agents therapeutic use, Anxiety drug therapy, Diketopiperazines therapeutic use, GABA Modulators therapeutic use

Abstract

The anxiolytic effect of earlier reported piperazinediones was assessed by elevated plus maze (EPM), hole-board and open-field (OFT) tests. The rats were administered pretreatment of three different doses i.e. 2, 1 and 0.5 mg/kg of compounds 52, 53 and 55 for seven consecutive days. Compound 52 and diazepam showed increase in open arm entries, increase in time spent therein and total arm entries at 1 mg/kg dose. The compound also produced increase in the number of head dip, sniffing behavior and total number of squares crossed compared to diazepam. In OFT paradigm grooming behavior, number of central squares crossed and the time spent in central area did not reveal statistical differences for diazepam and compound 52 at 1 mg/kg dose. Flumazenil mediated antagonism experiments of these showed that they were acting through benzodiazepine site on GABAA receptor. The levels of 5HT and 5HIAA were estimated in amygdalar region. Level of 5HT was found to be equivalent in case of compound 52 and diazepam treatment at dose of 1 mg/kg. Interestingly, compound 52 did not display sedative effect at higher dose in both animal models. Thus, present study indicated that compound 52 produced anti-anxiety property through modulation of GABAergic transmission., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2019

21. Paradoxical reaction to benzodiazepines in elderly - Case series.

Author

Reddy MSS, Achary U, Harbishettar V, Sivakumar PT, and Varghese M

Subjects

Aged, Benzodiazepines therapeutic use, Clonazepam therapeutic use, GABA Modulators adverse effects, GABA Modulators therapeutic use, Humans, Lorazepam therapeutic use, Male, Aggression drug effects, Benzodiazepines adverse effects, Clonazepam adverse effects, Lorazepam adverse effects, Psychomotor Agitation drug therapy, Sleep Wake Disorders chemically induced

Published

2018

22. An observational study of benzodiazepine prescription during inpatient alcohol detoxification for patients with vs. without chronic pretreatment with high-dosage baclofen.

Author

Martinez L, Vorspan F, Declèves X, Azuar J, Fortias M, Questel F, Dereux A, Grichy L, Barreteau H, Bellivier F, Lépine JP, and Bloch V

Subjects

Administration, Oral, Adult, Alcohol Drinking adverse effects, Alcohol Drinking physiopathology, Alcohol Drinking psychology, Alcoholism diagnosis, Alcoholism physiopathology, Alcoholism psychology, Baclofen adverse effects, Diazepam adverse effects, Female, GABA Modulators adverse effects, GABA-B Receptor Agonists adverse effects, Humans, Male, Middle Aged, Oxazepam adverse effects, Retrospective Studies, Substance Withdrawal Syndrome diagnosis, Substance Withdrawal Syndrome physiopathology, Substance Withdrawal Syndrome psychology, Time Factors, Treatment Outcome, Alcohol Drinking prevention & control, Alcoholism drug therapy, Baclofen administration & dosage, Diazepam administration & dosage, GABA Modulators administration & dosage, GABA-B Receptor Agonists therapeutic use, Inpatients, Oxazepam administration & dosage, Substance Withdrawal Syndrome drug therapy

Abstract

High-dose baclofen is prescribed as a maintenance treatment to reduce alcohol use in patients with alcohol use disorder. Nevertheless, some patients still have massive alcohol intakes and require inpatient alcohol withdrawal. To compare the oral dose of benzodiazepine prescribed to manage alcohol withdrawal symptoms in patients with vs. without steady-state pretreatment with high-dose baclofen. Retrospective chart review study. Prescribed benzodiazepine dose expressed in diazepam-equivalent was compared between groups. Thirty-one patients were assessed in the high-dose maintenance baclofen group and compared to 31 matched patients not receiving baclofen. No statistically significant difference was evident between groups regarding levels of benzodiazepines prescribed. The mean diazepam-equivalent dose during the first 7 days was 294 ± 149 mg in the baclofen group vs. 310 ± 133 mg (t-test = 0.440, P = 0.661) in matched controls. Steady-state high-dose baclofen before an inpatient alcohol cessation hospitalization does not lower the needed benzodiazepine dose in the management of alcohol withdrawal symptoms., (© 2017 Société Française de Pharmacologie et de Thérapeutique.)

Published

2018

23. Investigations on clonazepam-loaded polymeric micelle-like nanoparticles for safe drug administration during pregnancy.

Author

Sezgin-Bayindir Z, Elcin AE, Parmaksiz M, Elcin YM, and Yuksel N

Subjects

Acrylic Resins adverse effects, Acrylic Resins chemistry, Cell Line, Clonazepam adverse effects, Clonazepam pharmacokinetics, Drug Carriers adverse effects, Drug Liberation, Female, GABA Modulators adverse effects, GABA Modulators pharmacokinetics, Humans, Lactates adverse effects, Lactates chemistry, Nanoparticles adverse effects, Phosphatidylethanolamines adverse effects, Phosphatidylethanolamines chemistry, Placenta drug effects, Polyethylene Glycols adverse effects, Polyethylene Glycols chemistry, Polymers adverse effects, Polystyrenes adverse effects, Polystyrenes chemistry, Pregnancy, Clonazepam administration & dosage, Drug Carriers chemistry, GABA Modulators administration & dosage, Nanoparticles chemistry, Polymers chemistry

Abstract

Medication during pregnancy is often a necessity for women to treat their acute or chronic diseases. The goal of this study is to evaluate the potential of micelle-like nanoparticles (MNP) for providing safe drug usage in pregnancy and protect both foetus and mother from medication side effects. Clonazepam-loaded MNP were prepared from copolymers [polystyrene-poly(acrylic acid) (PS-PAA), poly(ethylene glycol)-b-poly(lactic acid) (PEG-PLA) and distearyl-sn-glycero-3-phosphoethanolamine-N-[methoxy-poly(ethylene glycol) (PEG-DSPE)] with varying monomer ratios and their drug-loading efficiency, drug release ratio, particle size, surface charge and morphology were characterised. The cellular transport and cytotoxicity experiments were conducted on clonazepam and MNP formulations using placenta-choriocarcinoma-BeWo and brain-endothelial-bEnd3 cells. Clonazepam-loaded PEG 5000 -PLA 4500 MNP reduced the drug transport through BeWo cells demonstrating that MNP may lower foetal drug exposure, thus reduce the drug side effects. However, lipofectamine modified MNP improved the transport of clonazepam and found to be promising for brain and in-utero-specific drug treatment.

Published

2018

24. Efficacy and safety of flumazenil injection for the reversal of midazolam sedation after elective outpatient endoscopy.

Author

Lee SP, Sung IK, Kim JH, Lee SY, Park HS, and Shim CS

Subjects

Adult, Aged, Ambulatory Surgical Procedures methods, Anesthesia Recovery Period, Elective Surgical Procedures methods, Female, Flumazenil administration & dosage, Flumazenil adverse effects, GABA Modulators administration & dosage, GABA Modulators adverse effects, Humans, Injections, Intravenous, Male, Middle Aged, Pain, Postoperative etiology, Prospective Studies, Young Adult, Conscious Sedation methods, Endoscopy, Gastrointestinal methods, Flumazenil pharmacology, GABA Modulators pharmacology, Hypnotics and Sedatives antagonists & inhibitors, Midazolam antagonists & inhibitors

Abstract

Objective: Midazolam sedation during elective endoscopy is widely performed and flumazenil is frequently administered after endoscopy to reverse sedation in clinical practice. This study aimed to investigate the safety and efficacy of flumazenil injections after elective endoscopy under midazolam sedation., Methods: Participants who underwent an upper endoscopy under midazolam sedation were randomly divided into two groups. In group I, flumazenil was administered i.v. 10 min after the patient's transfer to the recovery room, and no antidote was injected in group II. The time of stay in the recovery room and adverse events were reviewed through the nursing records. We asked the patients about their pain and degree of satisfaction according to a visual analogue scale (VAS), their memory of the procedure, mental status and the presence of uncomfortable symptoms on the day of the procedure and the day afterwards., Results: The length of stay in recovery was significantly shorter in group I than in group II. No significant differences were found in the number of patients with pain (VAS ≥1), adverse events and discomfort between the two groups. Additionally, there were no differences in the patients' memory of the procedure, satisfaction with sedation, willingness to repeat the endoscopy and mental status., Conclusions: The time in the recovery room after flumazenil administration was significantly shortened, and the use of the drug did not increase the risk of adverse events or discomfort. The use of flumazenil for reversing midazolam sedation seems to be safe and effective., (© 2018 Chinese Medical Association Shanghai Branch, Chinese Society of Gastroenterology, Renji Hospital Affiliated to Shanghai Jiaotong University School of Medicine and John Wiley & Sons Australia, Ltd.)

Published

2018

25. Is flumazenil an alternative for the treatment of hepatic encephalopathy?

Author

Reyes D and Barrera F

Subjects

Databases, Factual, Flumazenil adverse effects, Flumazenil pharmacology, GABA Modulators adverse effects, GABA Modulators pharmacology, Hepatic Encephalopathy mortality, Hepatic Encephalopathy physiopathology, Humans, Randomized Controlled Trials as Topic, Treatment Outcome, Flumazenil therapeutic use, GABA Modulators therapeutic use, Hepatic Encephalopathy drug therapy

Abstract

Introduction: Flumazenil is an antagonist of the GABA/benzodiazepines receptor complex that might play a role in the treatment of hepatic encephalopathy. However, its efficacy and safety are a matter of debate., Methods: To answer this question we used Epistemonikos, the largest database of systematic reviews in health, which is maintained by screening multiple information sources, including MEDLINE, EMBASE, Cochrane, among others. We extracted data from the systematic reviews, reanalyzed data of primary studies, conducted a meta-analysis and generated a summary of findings table using the GRADE approach., Results and Conclusions: We identified two systematic reviews including fourteen randomized trials. We concluded flumazenil does not reduce mortality in patients with hepatic encephalopathy and it is not clear whether it leads to any clinical improvement because the certainty of the evidence is very low.

Published

2017

26. Lorazepam precipitated alcohol withdrawal delirium - Two case report.

Author

Ram D, Raman R, and Gowdappa B

Subjects

Alcohol Withdrawal Delirium drug therapy, Antipsychotic Agents therapeutic use, Drug Administration Schedule, Female, GABA Modulators therapeutic use, Haloperidol therapeutic use, Humans, Lorazepam therapeutic use, Male, Middle Aged, Alcohol Withdrawal Delirium etiology, GABA Modulators adverse effects, Lorazepam adverse effects

Published

2017

27. Flumazenil versus placebo or no intervention for people with cirrhosis and hepatic encephalopathy.

Author

Goh ET, Andersen ML, Morgan MY, and Gluud LL

Subjects

Cause of Death, Flumazenil adverse effects, GABA Modulators adverse effects, Hepatic Encephalopathy etiology, Hepatic Encephalopathy mortality, Humans, Liver Cirrhosis mortality, Placebos therapeutic use, Randomized Controlled Trials as Topic, Watchful Waiting, Flumazenil therapeutic use, GABA Modulators therapeutic use, Hepatic Encephalopathy drug therapy, Liver Cirrhosis complications

Abstract

Background: Hepatic encephalopathy is a common complication of cirrhosis which results in poor brain functioning. The spectrum of changes associated with hepatic encephalopathy ranges from the clinically 'indiscernible' or minimal hepatic encephalopathy to the clinically 'obvious' or overt hepatic encephalopathy. Flumazenil is a synthetic benzodiazepine antagonist with high affinity for the central benzodiazepine recognition site. Flumazenil may benefit people with hepatic encephalopathy through an indirect negative allosteric modulatory effect on gamma-aminobutyric acid receptor function. The previous version of this review, which included 13 randomised clinical trials, found no effect of flumazenil on all-cause mortality, based on an analysis of 10 randomised clinical trials, but found a beneficial effect on hepatic encephalopathy, based on an analysis of eight randomised clinical trials., Objectives: To evaluate the beneficial and harmful effects of flumazenil versus placebo or no intervention for people with cirrhosis and hepatic encephalopathy., Search Methods: We searched The Cochrane Hepato-Biliary Group Controlled Trials Register, CENTRAL, MEDLINE, Embase, Science Citation Index Expanded, and LILACS; meeting and conference proceedings; and bibliographies in May 2017., Selection Criteria: We included randomised clinical trials regardless of publication status, blinding, or language in the analyses of benefits and harms, and observational studies in the assessment of harms., Data Collection and Analysis: Two review authors extracted data independently. We undertook meta-analyses and presented results using risk ratios (RR) with 95% confidence intervals (CI) and I 2 values as a marker of heterogeneity. We assessed bias control using the Cochrane Hepato-Biliary Group domains; determined the quality of the evidence using GRADE; evaluated the risk of small-study effects in regression analyses; and conducted trial sequential, subgroup, and sensitivity analyses., Main Results: We identified 14 eligible randomised clinical trials with 867 participants, the majority of whom had an acute episode of overt hepatic encephalopathy. In addition, we identified one ongoing randomised clinical trial. We were unable to gather outcome data from two randomised clinical trials with 25 participants. Thus, our analyses include 842 participants from 12 randomised clinical trials comparing flumazenil versus placebo. We classified one randomised clinical trial at low risk of bias in the overall assessment and the remaining randomised clinical trials at high risk of bias. The duration of follow-up ranged from a few minutes to two weeks, but it was less than one day in the majority of the trials.In total, 32/433 (7.4%) participants allocated to flumazenil versus 38/409 (9.3%) participants allocated to placebo died (RR 0.75, 95% CI 0.48 to 1.16; 11 randomised clinical trials; low quality evidence). The Trial Sequential Analysis and the one randomised clinical trial assessed as low risk of bias (RR 0.76, 95% CI 0.37 to 1.53) found no beneficial or harmful effects of flumazenil on all-cause mortality. The methods used to evaluate hepatic encephalopathy included several different clinical scales, electrophysiological variables, and psychometric tests. Flumazenil was associated with a beneficial effect on hepatic encephalopathy when including all randomised clinical trials (RR 0.75, 95% CI 0.71 to 0.80; 824 participants; nine randomised clinical trials; low quality evidence), or just the trial at low risk of bias (RR 0.78, 95% CI 0.72 to 0.84; 527 participants). The Trial Sequential Analysis supported a beneficial effect of flumazenil on hepatic encephalopathy. The randomised clinical trials included little information about causes of death and little information on non-fatal serious adverse events., Authors' Conclusions: We found low quality evidence suggesting a short-term beneficial effect of flumazenil on hepatic encephalopathy in people with cirrhosis, but no evidence of an effect on all-cause mortality. Additional evidence from large, high quality randomised clinical trials is needed to evaluate the potential benefits and harms of flumazenil in people with cirrhosis and hepatic encephalopathy.

Published

2017

28. Ketamine versus midazolam in bipolar depression with suicidal thoughts: A pilot midazolam-controlled randomized clinical trial.

Author

Grunebaum MF, Ellis SP, Keilp JG, Moitra VK, Cooper TB, Marver JE, Burke AK, Milak MS, Sublette ME, Oquendo MA, and Mann JJ

Subjects

Adult, Anesthetics, Dissociative administration & dosage, Anesthetics, Dissociative adverse effects, Biomarkers analysis, Brain-Derived Neurotrophic Factor analysis, Dose-Response Relationship, Drug, Double-Blind Method, Drug Monitoring methods, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, Humans, Male, Middle Aged, Treatment Outcome, Bipolar Disorder diagnosis, Bipolar Disorder drug therapy, Bipolar Disorder psychology, Ketamine administration & dosage, Ketamine adverse effects, Memory drug effects, Midazolam administration & dosage, Midazolam adverse effects, Suicidal Ideation

Abstract

Objectives: To evaluate feasibility and effects of a sub-anesthetic infusion dose of ketamine versus midazolam on suicidal ideation in bipolar depression. Neurocognitive, blood and saliva biomarkers were explored., Methods: Sixteen participants with bipolar depression and a Scale for Suicidal Ideation (SSI) score of ≥4 were randomized to ketamine (0.5 mg/kg) or midazolam (0.02 mg/kg). Current pharmacotherapy was maintained excluding benzodiazepines within 24 hours. The primary clinical outcome was SSI score on day 1 post-infusion., Results: Results supported feasibility. Mean reduction of SSI after ketamine infusion was almost 6 points greater than after midazolam, although this was not statistically significant (estimate=5.84, SE=3.01, t=1.94, P=.074, 95% confidence interval ([CI)]=-0.65 to 12.31). The number needed to treat for response (SSI <4 and at least 50% below baseline) was 2.2, and for remission (SSI=0) was 3.2. The strongest neurocognitive correlation was between memory improvement on the Selective Reminding Test (SRT) and reduction in SSI score on day 1 after ketamine (ρ=-.89, P=.007). Pre- to post-infusion decrease in serum brain derived neurotrophic factor (BDNF) correlated with reduction in SSI from baseline to day 1 after ketamine (n=5, ρ=0.90, P=.037) but not midazolam (P=.087)., Conclusions: The study demonstrated feasibility. Suicidal thoughts were lower after ketamine than after midazolam at a trend level of significance, likely due to the small pilot sample. Memory improvement and BDNF are promising biomarkers. Replication is needed in an adequately powered full-scale trial., (© 2017 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2017

29. Toxicodynetics in nordiazepam and oxazepam overdoses.

Author

Sacre L, Ali SM, Villa A, Jouffroy R, Raphalen JH, Garnier R, and Baud FJ

Subjects

Adolescent, Adult, Aging metabolism, Central Nervous System Depressants adverse effects, Child, Child, Preschool, Ethanol adverse effects, Female, Humans, Male, Middle Aged, Retrospective Studies, Young Adult, Drug Overdose metabolism, GABA Modulators adverse effects, GABA Modulators pharmacokinetics, Nordazepam adverse effects, Nordazepam pharmacokinetics, Oxazepam adverse effects, Oxazepam pharmacokinetics, Toxicokinetics

Abstract

Objectives: Toxicodynetics aims at defining the time-course of major clinical events in drug overdose. We report the toxicodynetics in mono-intoxications with oxazepam and nordiazepam., Methods: Cases of oxazepam or nordiazepam overdoses collected at the Paris poison control centre from 1999 to 2014 on the basis of self-report. A particular attention was paid to eliminate the concomitant alcohol or psychotropic co-ingestions. The toxicodynetic parameters were assessed as previously described. Results are expressed using 10-90 percentiles. In adults, the dose was normalized (TI, toxic Index) by dividing the supposed ingested dose by the maximal recommended dose., Results: Two hundred and fifty-one and 74 cases of oxazepam and nordiazepam poisonings were included, respectively. The Emax for oxazepam and nordiazepam were sleepiness or obtundation in 106 and 36 cases, respectively. Coma was used to qualify only one oxazepam overdose. The median delay in onset of the Emax was 1.5h (0.33-15) in nordiazepam and 4h (0.5-15) in oxazepam overdose. In both overdoses, the onset of Emax occurred on an "on-off" mode. In adults, the greatest TIs in nordiazepam and oxazepam overdoses were 45 and 26.7, respectively. The TI in the oxazepam-induced coma was 26.7, the largest dose., Conclusion: Data collected in PCC allow determining a number of toxicodynetic parameters. Toxicodynetics showed that nordiazepam is not a cause of coma even in large overdose while oxazepam causes coma only at a very high dose. Deep coma in nordiazepam overdose whatever the dose and deep coma in overdose with oxazepam involving TI less than 20 result from unrecognized drug-drug interaction., (Copyright © 2017. Published by Elsevier Masson SAS.)

Published

2017

30. The Pharmacology and Toxicology of the 'Holy Trinity'.

Author

Horsfall JT and Sprague JE

Subjects

Analgesics, Opioid administration & dosage, Animals, Benzodiazepines administration & dosage, Carisoprodol administration & dosage, Contraindications, Dopamine metabolism, Drug Dosage Calculations, Drug Synergism, Drug Therapy, Combination, GABA Modulators administration & dosage, Humans, Neuromuscular Agents administration & dosage, Nucleus Accumbens metabolism, Nucleus Accumbens physiopathology, Opioid-Related Disorders metabolism, Opioid-Related Disorders physiopathology, Opioid-Related Disorders psychology, Practice Guidelines as Topic, Respiration drug effects, Respiratory Insufficiency metabolism, Respiratory Insufficiency physiopathology, Risk Assessment, Signal Transduction drug effects, gamma-Aminobutyric Acid metabolism, Analgesics, Opioid adverse effects, Benzodiazepines adverse effects, Carisoprodol adverse effects, Euphoria drug effects, GABA Modulators adverse effects, Neuromuscular Agents adverse effects, Nucleus Accumbens drug effects, Respiratory Insufficiency chemically induced

Abstract

Combining opioids with benzodiazepines and skeletal muscle relaxants ('The Holy Trinity') has been reported to potentiate the 'high'. Through unique interactions with colocalized μ-opioid and GABA A receptors, the combined use of these agents induces a synergistic increase in dopamine in the nucleus accumbens (NAc) and depression of respiration. The inhibition of GABA release mediated by μ 1 -opioid receptor activation results in a subsequent increase in dopamine in the NAc. Benzodiazepines activate the GABA A R to suppress respiration in the medullary respiratory centres. The skeletal muscle relaxant, carisoprodol, appears to bind to a unique binding domain within the GABA A R to further enhance the respiratory depressant effects of the benzodiazepines. Therefore, the opioids, the benzodiazepines and carisoprodol alone or in combination are capable of inducing respiratory depression. Current guidelines for opioid prescribing recommend against the concomitant use of benzodiazepines but do not recognize the potential risk associated with the addition of skeletal muscle relaxants., (© 2016 Nordic Association for the Publication of BCPT (former Nordic Pharmacological Society).)

Published

2017

31. Use of GABAergic sedatives after subarachnoid hemorrhage is associated with worse outcome-preliminary findings.

Author

Hertle DN, Beynon C, Neumann JO, Santos E, Sánchez-Porras R, Unterberg AW, and Sakowitz OW

Subjects

Adult, Aged, Conscious Sedation methods, Female, Flunitrazepam administration & dosage, Flunitrazepam adverse effects, Flunitrazepam therapeutic use, GABA Modulators administration & dosage, GABA Modulators therapeutic use, Glasgow Coma Scale, Humans, Hypnotics and Sedatives administration & dosage, Hypnotics and Sedatives therapeutic use, Male, Midazolam administration & dosage, Midazolam adverse effects, Midazolam therapeutic use, Middle Aged, Propofol administration & dosage, Propofol adverse effects, Propofol therapeutic use, Retrospective Studies, Subarachnoid Hemorrhage complications, Brain physiology, GABA Modulators adverse effects, Hypnotics and Sedatives adverse effects, Regeneration drug effects, Subarachnoid Hemorrhage drug therapy

Abstract

Study Objective: Recent experimental evidence identified GABAergic sedation as a possible cause for deprived neuroregeneration and poor outcome after acute brain injury. Patients with aneurysmal subarachnoid hemorrhage are often sedated, and GABAergic sedation, such as midazolam and propofol, is commonly used., Design: Retrospective cohort study based on a prospectively established database., Setting: Single-center neurointensive care unit., Patients: Twenty-nine patients after subarachnoid hemorrhage., Intervention: Noninterventional study., Measurements: The relationship between mean GABAergic sedative dose during the acute phase and outcome after 6 months according to the Glasgow Outcome Scale, and initial Glasgow Coma Scale was investigated., Main Results: Use of GABAergic sedatives was negatively correlated with Glasgow Outcome Scale (r 2 =0.267; P=.008). Administration of sedatives was independent of the initial Glasgow Coma Scale. GABAergic sedatives flunitrazepam, midazolam, and propofol were used differently during the first 10 days after ictus., Conclusion: Administration of GABAergic sedation was associated with an unfavorable outcome after 6 months. To avoid bias (mainly through the indication to use sedation), additional experimental and comparative clinical investigation of, for example, non-GABAergic sedation, and clinical protocols of no sedation is necessary., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

32. Disproportionality Analysis for the Assessment of Abuse and Dependence Potential of Pregabalin in the French Pharmacovigilance Database.

Author

Bossard JB, Ponté C, Dupouy J, Lapeyre-Mestre M, and Jouanjus E

Subjects

Adult, Adverse Drug Reaction Reporting Systems, Aged, Amitriptyline adverse effects, Antidepressive Agents, Tricyclic adverse effects, Clonazepam adverse effects, Databases, Factual, Female, France, GABA Modulators adverse effects, Humans, Male, Middle Aged, Pharmacovigilance, Pregabalin adverse effects, Substance-Related Disorders epidemiology

Abstract

Background and Objective: Pregabalin abuse and dependence has been increasingly described; however, it is not described in France. Our study aimed to investigate the abuse and dependence potential of pregabalin by a disproportionality analysis, in the French Pharmacovigilance Database (FPVD), in comparison with amitriptyline and clonazepam., Methods: We performed a case/noncase study in the FPVD. Between January, 1 2010 and December, 31 2015, we identified cases of abuse and or dependence (excluding isolated withdrawal syndromes) using MedDRA (Medical Dictionary for Regular Activities) terms. Exposure to pregabalin was defined as the mention of pregabalin in the report. Clonazepam was used as positive control and amitriptyline as negative control., Results: Among the 184,310 reports in the database, 521 were abuse or dependence cases. Exposure to pregabalin was found in eight (1.5 %) of them. We did not find any significant association between exposure to pregabalin and drug abuse or dependence: reporting odds ratio (ROR) = 1.1 95 % confidence interval (CI) (0.6-2.3). ROR for clonazepam was 5.7 95 % CI (3.5-9.2). No case of an amitriptyline-related abuse or dependence was recorded in the FPVD., Conclusions: The first cases of pregabalin-related abuse or dependence reported in France occurred later than in other European countries, since none had been described before 2010. This analysis in the FPVD did not find a higher proportion of abuse/dependence with pregabalin in comparison with other drugs. Considering evidence of pregabalin abuse worldwide, this analysis underlines the limitations of spontaneous reporting system in the field of addictovigilance.

Published

2016

33. Prenatal stress alters diazepam withdrawal syndrome and 5HT1A receptor expression in the raphe nuclei of adult rats.

Author

Lakehayli S, Said N, El Khachibi M, El Ouahli M, Nadifi S, Hakkou F, and Tazi A

Subjects

Animals, Diazepam pharmacology, Electroshock, Female, GABA Modulators pharmacology, Male, Pregnancy, RNA, Messenger metabolism, Random Allocation, Raphe Nuclei drug effects, Raphe Nuclei growth & development, Rats, Wistar, Receptor, Serotonin, 5-HT1A metabolism, Diazepam adverse effects, GABA Modulators adverse effects, Prenatal Exposure Delayed Effects, Raphe Nuclei metabolism, Stress, Psychological physiopathology, Substance Withdrawal Syndrome metabolism

Abstract

Early-life events have long-term effects on brain structures and cause behavioral alterations that persist into adulthood. The present experiments were designed to investigate the effects of prenatal stress on diazepam-induced withdrawal syndrome and serotonin-1A (5HT1A) receptor expression in the raphe nuclei of adult offspring. The results of the present study reveal that maternal exposure to chronic footshock stress increased the anxiety-like behavior in the prenatally stressed (PS) animals withdrawn from chronic diazepam (2.5mg/kg/day i.p for 1week). Moreover, prenatal stress induced a down-regulation of 5HT1A mRNA in the raphe nuclei of adult offspring. To our knowledge, this study is the first to demonstrate that maternal exposure to chronic footshock stress enhances diazepam withdrawal symptoms and alters 5HT1A receptor gene expression in the raphe nuclei of adult offspring. Thus, more studies are needed to clarify the mechanisms underlying the decrease of 5HT1A receptors expression in the raphe nuclei of PS rats., (Copyright © 2016 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2016

34. Safety and Abuse Liability of Oxazepam: Is This Benzodiazepine Drug Underutilized?

Author

Howland RH

Subjects

Benzodiazepines adverse effects, Benzodiazepines classification, GABA Modulators adverse effects, Humans, Oxazepam adverse effects, Safety legislation & jurisprudence, Substance-Related Disorders prevention & control, Benzodiazepines pharmacology, GABA Modulators pharmacology, Oxazepam pharmacology

Abstract

Benzodiazepine drugs are controversial because of safety and abuse liability concerns, although they have clinically relevant pharmacological differences. The current article reviews studies pertaining to the pharmacology, safety, and abuse liability of oxazepam. Compared to other benzodiazepine drugs, oxazepam has a favorable safety and abuse liability profile, which may be related to its pharmacology. Oxazepam is more slowly absorbed and enters the brain more slowly than other benzodiazepine drugs; it does not have active metabolites and does not accumulate with chronic dosing; its metabolism is not affected by age or by mild/moderate liver disease; and it is not prone to drug-drug interactions. Oxazepam also binds to the translocator protein, which stimulates the synthesis of neurosteroids, and this effect may contribute to its reduced abuse liability., (Copyright 2016, SLACK Incorporated.)

Published

2016

35. A Case Report of Clonazepam Dependence: Utilization of Therapeutic Drug Monitoring During Withdrawal Period.

Author

Kacirova I, Grundmann M, Silhan P, and Brozmanova H

Subjects

Adult, Clonazepam administration & dosage, Clonazepam blood, GABA Modulators administration & dosage, GABA Modulators blood, Humans, Male, Clonazepam adverse effects, Drug Monitoring, GABA Modulators adverse effects, Substance Withdrawal Syndrome etiology

Abstract

Clonazepam is long-acting benzodiazepine agonist used in short-acting benzodiazepine withdrawal; however, recent observations suggest the existence of its abuse. We demonstrate a 40-year-old man with a 20-year history of psychiatric care with recently benzodiazepine dependence (daily intake of ∼60 mg of clonazepam and 10 mg of alprazolam). High serum levels of both drugs were analyzed 3 weeks before admission to hospitalization (clonazepam 543.9 ng/mL, alprazolam 110 ng/mL) and at the time of admission (clonazepam 286.2 ng/mL, alprazolam 140 ng/mL) without any signs of benzodiazepine intoxication. Gradual withdrawal of clonazepam with monitoring of its serum levels and increase of gabapentin dose were used to minimize physical signs and symptoms of clonazepam withdrawal. Alprazolam was discontinued promptly. Clinical consequences of the treatment were controllable tension, intermittent headache, and rarely insomia. It is the first case report showing utilization of therapeutic drug monitoring during withdrawal period in the patient with extreme toleration to severe benzodiazepine dependence.

Published

2016

36. Recurrent Bilateral Dislocation of the Temporomandibular Joint Induced by Clonazepam in a Parkinsonian Patient.

Author

Le Goff F, Lefaucheur R, Fetter D, Rouille A, and Maltête D

Subjects

Aged, Female, Humans, Joint Dislocations complications, Parkinson Disease drug therapy, Temporomandibular Joint Disorders complications, Clonazepam adverse effects, GABA Modulators adverse effects, Joint Dislocations chemically induced, Temporomandibular Joint Disorders chemically induced

Published

2016

37. Current Phase II investigational therapies for insomnia.

Author

Zisapel N

Subjects

Clinical Trials, Phase II as Topic, Drugs, Investigational adverse effects, Drugs, Investigational pharmacology, Drugs, Investigational therapeutic use, GABA Modulators adverse effects, GABA Modulators pharmacology, GABA Modulators therapeutic use, Humans, Hypnotics and Sedatives adverse effects, Hypnotics and Sedatives pharmacology, Receptors, GABA-A drug effects, Receptors, GABA-A metabolism, Sleep Initiation and Maintenance Disorders physiopathology, Drug Design, Hypnotics and Sedatives therapeutic use, Sleep Initiation and Maintenance Disorders drug therapy

Abstract

Introduction: Insomnia is typified by a difficulty in sleep initiation, maintenance and/or quality (non-restorative sleep) resulting in significant daytime distress., Areas Covered: This review summarizes the available efficacy and safety data for drugs currently in the pipeline for treating insomnia. Specifically, the authors performed MEDLINE and internet searches using the keywords 'Phase II' and 'insomnia'. The drugs covered target GABAA (zaleplon-CR, lorediplon, EVT-201), orexin (filorexant, MIN-202), histamine-H1 (LY2624803), serotonin 5-HT2A (ITI-007), melatonin/serotonin5-HT1A (piromelatine) and melatonin (indication expansions of prolonged-release melatonin and tasimelteon for pediatric sleep and circadian rhythm disorders) receptors., Expert Opinion: Low-priced generic environments and high development costs limit the further development of drugs that treat insomnia. However, the bidirectional link between sleep and certain comorbidities may encourage development of specific drugs for comorbid insomnia. New insomnia therapies will most likely move away from GABAAR receptors' modulation to more subtle neurological pathways that regulate the sleep-wake cycle.

Published

2015

38. My sleep fest: an autoethnographic short story.

Author

Jago BJ

Subjects

Anthropology, Cultural, Antipsychotic Agents therapeutic use, Aripiprazole adverse effects, Aripiprazole therapeutic use, Clonazepam adverse effects, Clonazepam therapeutic use, Depressive Disorder drug therapy, GABA Modulators adverse effects, GABA Modulators therapeutic use, Humans, Inappropriate Prescribing, Quetiapine Fumarate adverse effects, Quetiapine Fumarate therapeutic use, Antipsychotic Agents adverse effects, Sleep drug effects

Published

2015

39. Exacerbation of benign familial neonatal epilepsy induced by massive doses of phenobarbital and midazolam.

Author

Maeda T, Shimizu M, Sekiguchi K, Ishii A, Ihara Y, Hirose S, and Izumi T

Subjects

Electroencephalography, Epilepsy, Benign Neonatal genetics, Epilepsy, Benign Neonatal physiopathology, Female, Humans, Seizures physiopathology, Epilepsy, Benign Neonatal drug therapy, GABA Modulators adverse effects, Midazolam adverse effects, Phenobarbital adverse effects, Seizures chemically induced

Abstract

Background: Barbiturates and benzodiazepines are the first-line anticonvulsants for neonatal seizures. However, in immature brains, those drugs may lead to paradoxical neuronal excitation., Patient: A patient with benign familial neonatal epilepsy developed epileptic encephalopathy after massive doses of phenobarbital that were followed by a continuous infusion of midazolam on postnatal day 3. Electroencephalography revealed rhythmic delta activity in clusters with migrating epileptic foci. After discontinuation of both drugs, the patient's consciousness promptly improved and her electroencephalography normalized on postnatal day 5., Results: This baby developed persistent electroencephalographic seizures due to massive doses of phenobarbital and midazolam., Conclusion: Clinicians should be aware of this anticonvulsant-induced paradoxical neuronal excitation and the uncoupling phenomenon, especially in individuals with benign familial neonatal epilepsy, who have low seizure thresholds., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

40. Serotonin syndrome versus neuroleptic malignant syndrome: a challenging clinical quandary.

Author

Dosi R, Ambaliya A, Joshi H, and Patell R

Subjects

Benzodiazepines adverse effects, Diagnosis, Differential, Humans, Lithium Compounds adverse effects, Male, Neuroleptic Malignant Syndrome complications, Neuroleptic Malignant Syndrome etiology, Olanzapine, Risperidone adverse effects, Serotonin Syndrome chemically induced, Serotonin Syndrome complications, Valproic Acid adverse effects, Young Adult, Antimanic Agents adverse effects, Antipsychotic Agents adverse effects, Clonazepam adverse effects, GABA Modulators adverse effects, Neuroleptic Malignant Syndrome diagnosis, Serotonin Syndrome diagnosis

Abstract

Serotonin syndrome and neuroleptic malignant syndrome are two drug toxidromes that have often overlapping and confusing clinical pictures. We report a case of a young man who presented with alteration of mental status, autonomic instability and neuromuscular hyperexcitability following ingestion of multiple psychiatric and antiepileptic medications. The patient satisfied criteria for serotonin syndrome and neuroleptic malignant syndrome, and based on the characteristic clinical features, laboratory findings and clinical course it was concluded that the patient had both toxidromes. The patient was managed with cyproheptadine and supportive measures, and recovered over the course of 3 weeks. A brief review of literature highlighting the diagnostic clues as well as the importance of recognising and distinguishing the often missed and confounding diagnoses follows., (2014 BMJ Publishing Group Ltd.)

Published

2014

41. Safety and efficacy of flumazenil for reversal of iatrogenic benzodiazepine-associated delirium toxicity during treatment of alcohol withdrawal, a retrospective review at one center.

Author

Moore PW, Donovan JW, Burkhart KK, Waskin JA, Hieger MA, Adkins AR, Wert Y, Haggerty DA, and Rasimas JJ

Subjects

Adult, Aged, Aged, 80 and over, Alcohol Deterrents chemistry, Alcohol Deterrents therapeutic use, Alcohol Withdrawal Delirium etiology, Alcohol Withdrawal Delirium prevention & control, Alcohol Withdrawal Seizures etiology, Alcohol Withdrawal Seizures prevention & control, Antidotes adverse effects, Benzodiazepines adverse effects, Benzodiazepines therapeutic use, Delirium etiology, Delirium prevention & control, Diagnosis, Differential, Diagnostic and Statistical Manual of Mental Disorders, Drug Monitoring, Ethanol adverse effects, Female, Flumazenil adverse effects, GABA Modulators adverse effects, GABA Modulators therapeutic use, Hospitals, University, Humans, Hypnotics and Sedatives adverse effects, Hypnotics and Sedatives therapeutic use, Male, Middle Aged, Neurotoxicity Syndromes diagnosis, Neurotoxicity Syndromes physiopathology, Pennsylvania, Retrospective Studies, Substance Withdrawal Syndrome physiopathology, Alcohol Deterrents adverse effects, Antidotes therapeutic use, Benzodiazepines antagonists & inhibitors, Flumazenil therapeutic use, Hypnotics and Sedatives antagonists & inhibitors, Neurotoxicity Syndromes drug therapy, Substance Withdrawal Syndrome drug therapy

Abstract

Both alcohol withdrawal syndrome (AWS) and benzodiazepines can cause delirium. Benzodiazepine-associated delirium can complicate AWS and prolong hospitalization. Benzodiazepine delirium can be diagnosed with flumazenil, a GABA-A receptor antagonist. By reversing the effects of benzodiazepines, flumazenil is theorized to exacerbate symptoms of AWS and precludes its use. For patients being treated for alcohol withdrawal, flumazenil can diagnose and treat benzodiazepine delirium without precipitating serious or life-threatening adverse events. Hospital admission records were retrospectively reviewed for patients with the diagnosis of AWS who received both benzodiazepines and flumazenil from December 2006 to June 2012 at a university-affiliated inpatient toxicology center. The day of last alcohol consumption was estimated from available blood alcohol content or subjective history. Corresponding benzodiazepine, flumazenil, and adjunctive sedative pharmacy records were reviewed, as were demographic, clinical course, and outcome data. Eighty-five patients were identified (average age 50.3 years). Alcohol concentrations were detectable for 42 patients with average 261 mg/dL (10-530 mg/dL). Eighty patients were treated with adjunctive agents for alcohol withdrawal including antipsychotics (n = 57), opioids (n = 27), clonidine (n = 35), and phenobarbital (n = 23). Average time of flumazenil administration was 4.7 days (1-11 days) after abstinence, and average dose was 0.5 mg (0.2-1 mg). At the time of flumazenil administration, delirium was described as hypoactive (n = 21), hyperactive (n = 15), mixed (n = 41), or not specified (n = 8). Response was not documented in 11 cases. Sixty-two (72.9 %) patients had significant objective improvement after receiving flumazenil. Fifty-six patients required more than one dose (average 5.6 doses). There were no major adverse events and minor adverse effects included transiently increased anxiety in two patients: 1 patient who received 0.5 mg on abstinence day 2 and another patient who received 0.2 mg flumazenil on abstinence day 11. This is the largest series diagnosing benzodiazepine delirium after AWS in patients receiving flumazenil. During the treatment of AWS, if delirium is present on day 5, a test dose of flumazenil may be considered to establish benzodiazepine delirium. With the limited data set often accompanying patients with AWS, flumazenil diagnosed benzodiazepine delirium during the treatment of AWS and improved impairments in cognition and behavior without serious or life-threatening adverse events in our patients.

Published

2014

42. Alcohol withdrawal and flumazenil: not for the faint of heart.

Author

Nelson LS

Subjects

Alcohol Deterrents chemistry, Alcohol Deterrents therapeutic use, Alcohol Withdrawal Delirium etiology, Alcohol Withdrawal Delirium prevention & control, Alcohol Withdrawal Seizures etiology, Alcohol Withdrawal Seizures prevention & control, Antidotes adverse effects, Delirium etiology, Delirium prevention & control, Drug Monitoring, Flumazenil adverse effects, GABA Modulators adverse effects, Humans, Hypnotics and Sedatives adverse effects, Hypnotics and Sedatives antagonists & inhibitors, Hypnotics and Sedatives therapeutic use, Neurotoxicity Syndromes metabolism, Neurotoxicity Syndromes physiopathology, Substance Withdrawal Syndrome metabolism, Substance Withdrawal Syndrome physiopathology, Alcohol Deterrents adverse effects, Antidotes therapeutic use, Ethanol adverse effects, Flumazenil therapeutic use, GABA Modulators therapeutic use, Neurotoxicity Syndromes drug therapy, Substance Withdrawal Syndrome drug therapy

Published

2014

43. Good clinical outcome after accidental intra-arterial injection of flunitrazepam tablets in 16 drug abusers with critical limb ischaemia.

Author

Rohm S, Staab H, Schulz H, Richter O, and Aust G

Subjects

Accidents, Adult, Amputation, Surgical, Analgesics administration & dosage, Anticoagulants administration & dosage, Combined Modality Therapy, Critical Illness, Drug Administration Schedule, Drug Therapy, Combination, Female, Fibrinolytic Agents administration & dosage, Flunitrazepam administration & dosage, GABA Modulators administration & dosage, Humans, Injections, Intra-Arterial, Ischemia diagnosis, Ischemia therapy, Limb Salvage, Male, Physical Therapy Modalities, Retrospective Studies, Time Factors, Time-to-Treatment, Treatment Outcome, Vasodilator Agents administration & dosage, Young Adult, Drug Users, Extremities blood supply, Flunitrazepam adverse effects, GABA Modulators adverse effects, Ischemia chemically induced, Substance Abuse, Intravenous

Abstract

Objectives: Inadvertent intra-arterial injection of flunitrazepam tablets intended for intravenous use by drug abusers has devastating effects. We report here on the clinical outcome of 16 drug abusers developing critical limb ischaemia after flunitrazepam injection., Methods: Treatment combined immediate analgesia and anticoagulation, long-lasting local thrombolysis and vasodilatation, antibiotic prophylaxis, and physical mobilization. The immediate bolus injection of 5,000 IU heparin was followed by a continuous heparin infusion up to the target partial thromboplastin time. Under arteriographic control local intra-arterial infusion with alternating 4-h cycles of 5 mg recombinant tissue plasminogen activator followed by 5 μg prostaglandinE1 (PGE1) was performed for 24-48 hours. Subsequently, 60 μg PGE1 was applied once daily., Results: Drug abusers, having been injected with 4-30 mg flunitrazepam, were treated 3-72 hours after the accident, with six of them not being treated until after 24 hours. All showed a high tissue ischaemia score. At the time of being discharged from hospital 13 patients had a normal extremity. In one patient, first receiving treatment 72 hours after injection, minor amputation of fingers was necessary. The life of the patient who injected 30 mg flunitrazepam in the leg was saved after hip disarticulation. One patient developed neurological dysfunction in the affected toes., Conclusions: Intensive treatment after inadvertent intra-arterial drug injection normalized the affected extremity in most drug abusers, even after the late onset of therapy., (Copyright © 2013 European Society for Vascular Surgery. Published by Elsevier Ltd. All rights reserved.)

Published

2014

44. Chemical submission to commit robbery: a series of involuntary intoxications with flunitrazepam in Asian travellers in Brussels.

Author

Ramadan AS, Wenanu O, Cock AD, Maes V, Lheureux P, and Mols P

Subjects

Adult, Asian People, Belgium, Confusion chemically induced, Fatigue chemically induced, Flunitrazepam administration & dosage, Forensic Toxicology, GABA Modulators administration & dosage, Humans, Male, Middle Aged, Travel, Amnesia, Anterograde chemically induced, Flunitrazepam adverse effects, Food Contamination, GABA Modulators adverse effects, Theft

Abstract

Between January 17, 2003 and August 29, 2003, the Emergency Department admitted a patient who had been surreptitiously intoxicated and robbed of his valuables every Friday. The first cases were considered anecdotal, but criminal activity was rapidly suspected. The cohort includes 16 male Asian patients aged 28-50 years. All the victims had just arrived in Brussels through one of the main rail station of the town and were admitted via the emergency ambulance service from different locations in the centre of Brussels around the CHU Saint-Pierre Hospital. Haemodynamic parameters upon admission were within normal limits. The Glasgow Coma Scale was equal or higher than 9/15 in 14 of the 16 victims. Toxicology screening obtained in 12 patients revealed the presence of flunitrazepam, which was further quantified at levels ranging from 21 to 75 μg/l. One of the Japanese patients, who returned to Belgium afterwards for professional reasons, was approached by the police and accepted to press charges. This allowed the police to investigate and send undercover agents to the railway station on Friday afternoons and evenings. They found a person who was offering welcome cookies to Asian travellers. He arrived from Amsterdam and returned once his crime was committed. Flunitrazepam is well known as a rape drug. We report a series of victims in whom flunitrazepam was used to facilitate robbery., (Copyright © 2013 Elsevier Ltd and Faculty of Forensic and Legal Medicine. All rights reserved.)

Published

2013

45. Haloperidol overdosing in the treatment of agitated hospitalized older people with delirium: a retrospective chart review from a community teaching hospital.

Author

Zirker W, Dorokhine I, Knapp CM, Patel N, and Musuku M

Subjects

Aged, Aged, 80 and over, Anti-Anxiety Agents adverse effects, Anti-Anxiety Agents therapeutic use, Delirium physiopathology, Dopamine Antagonists adverse effects, Dopamine Antagonists therapeutic use, Dose-Response Relationship, Drug, Drug Prescriptions, Drug Therapy, Combination adverse effects, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, GABA Modulators therapeutic use, Haloperidol adverse effects, Haloperidol therapeutic use, Hospitals, Community, Hospitals, Teaching, Humans, Length of Stay, Lorazepam administration & dosage, Lorazepam adverse effects, Lorazepam therapeutic use, Male, Medical Records, Pennsylvania, Practice Patterns, Physicians', Psychomotor Agitation etiology, Retrospective Studies, Aging, Anti-Anxiety Agents administration & dosage, Delirium drug therapy, Dopamine Antagonists administration & dosage, Haloperidol administration & dosage, Psychomotor Agitation prevention & control

Abstract

Background: Practice guidelines recommend the use of low dose haloperidol when medication is needed to treat delirium with acute agitation in hospitalized older people. Despite this, high dose haloperidol may frequently be used and result in higher rates of complications., Objective: To describe dosages and effects of haloperidol used in the initial treatment of delirium with acute agitation in hospitalized older people, and prescriber use of low and high dose haloperidol., Methods: Retrospective chart reviews were performed from June 2008 to May 2009 in a community teaching hospital located in Upland, PA, USA. Patients aged 65 years and older with acute agitated delirium were included. Patients admitted to ICU and those with psychiatric conditions were excluded. Data were collected on haloperidol dosing, responses, sedation, length of stay, and concurrent use of lorazepam., Results: A total of 261 charts of patients who received haloperidol were reviewed and 56 patients met inclusion criteria (14 males, 42 females). The mean age of subjects was 83 years. The recommended starting dose of haloperidol (0.5 mg) was administered to 35.7 % of the patients. An initial dose of more than 1 mg was received by 37.5 % of the patients. The remaining 26.8 % of patients received 1 mg. The relative risk of sedation was significantly greater for subjects receiving more than 1 mg of haloperidol in 24 h. The length of hospitalization was not predicted by haloperidol doses or lorazepam but by the number of days of agitation., Conclusions: Higher than recommended initial doses of haloperidol were frequently used in the treatment of delirium with acute agitation in hospitalized older people. We found no evidence to suggest that higher dosages were more effective in decreasing the duration of agitation or the length of hospital stay. Low dose haloperidol appears to be as effective as and safer than higher doses in the treatment of acute agitation in this older population.

Published

2013

46. Treatment outcomes in REM sleep behavior disorder.

Author

McCarter SJ, Boswell CL, St Louis EK, Dueffert LG, Slocumb N, Boeve BF, Silber MH, Olson EJ, and Tippmann-Peikert M

Subjects

Adult, Aged, Aged, 80 and over, Central Nervous System Depressants administration & dosage, Central Nervous System Depressants adverse effects, Clonazepam adverse effects, Drug Therapy, Combination, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, Health Surveys, Humans, Longitudinal Studies, Male, Melatonin adverse effects, Middle Aged, Retrospective Studies, Treatment Outcome, Wounds and Injuries prevention & control, Clonazepam administration & dosage, Melatonin administration & dosage, REM Sleep Behavior Disorder drug therapy, REM Sleep Parasomnias drug therapy

Abstract

Objective: REM sleep behavior disorder (RBD) is usually characterized by potentially injurious dream enactment behaviors (DEB). RBD treatment aims to reduce DEBs and prevent injury, but outcomes require further elucidation. We surveyed RBD patients to describe longitudinal treatment outcomes with melatonin and clonazepam., Methods: We surveyed and reviewed records of consecutive RBD patients seen at Mayo Clinic between 2008-2010 to describe RBD-related injury frequency-severity as well as RBD visual analog scale (VAS) ratings, medication dosage, and side effects. Statistical analyses were performed with appropriate non-parametric matched pairs tests before and after treatment, and with comparative group analyses for continuous and categorical variables between treatment groups. The primary outcome variables were RBD VAS ratings and injury frequency., Results: Forty-five (84.9%) of 53 respondent surveys were analyzed. Mean age was 65.8 years and 35 (77.8%) patients were men. Neurodegenerative disorders were seen in 24 (53%) patients and 25 (56%) received antidepressants. Twenty-five patients received melatonin, 18 received clonazepam, and two received both as initial treatment. Before treatment, 27 patients (60%) reported an RBD associated injury. Median dosages were melatonin 6 mg and clonazepam 0.5 mg. RBD VAS ratings were significantly improved following both treatments (p(m) = 0.0001, p(c) = 0.0005). Melatonin-treated patients reported significantly reduced injuries (p(m) = 0.001, p(c) = 0.06) and fewer adverse effects (p = 0.07). Mean durations of treatment were no different between groups (for clonazepam 53.9 ± 29.5 months, and for melatonin 27.4 ± 24 months, p = 0.13) and there were no differences in treatment retention, with 28% of melatonin and 22% of clonazepam-treated patients discontinuing treatment (p = 0.43)., Conclusions: Melatonin and clonazepam were each reported to reduce RBD behaviors and injuries and appeared comparably effective in our naturalistic practice experience. Melatonin-treated patients reported less frequent adverse effects than those treated with clonazepam. More effective treatments that would eliminate injury potential and evidence-based treatment outcomes from prospective clinical trials for RBD are needed., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2013

47. Safety and effectiveness of a fixed-dose phenobarbital protocol for inpatient benzodiazepine detoxification.

Author

Kawasaki SS, Jacapraro JS, and Rastegar DA

Subjects

Adult, Dose-Response Relationship, Drug, Electronic Health Records, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, GABA Modulators therapeutic use, Humans, Inpatients, Male, Middle Aged, Patient Readmission statistics & numerical data, Phenobarbital administration & dosage, Phenobarbital adverse effects, Treatment Outcome, Young Adult, Benzodiazepines adverse effects, Phenobarbital therapeutic use, Substance Withdrawal Syndrome drug therapy, Substance-Related Disorders rehabilitation

Abstract

Benzodiazepine dependence is a common problem. However, there is limited data on safe and effective detoxification protocols for benzodiazepine-dependent patients. We reviewed the medical records of 310 patients treated with a 3-day fixed-dose phenobarbital taper for benzodiazepine dependence over a 5-year period between 2004 and 2009. We recorded the incidence of seizures, falls, delirium, and emergency department (ED) visits or readmission to our institution within 30 days as markers for safety; we also recorded how many patients had doses held because of sedation. The taper was well tolerated, although one quarter of the patients had at least one dose held because of sedation. There were no seizures, falls, or injuries reported. Six percent had a readmission, and 7% had an ED visit at our institution within 30 days of discharge, but only 3 patients required readmission for withdrawal symptoms. Overall, this protocol appears to be safe and effective., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

48. Drugs for insomnia.

Author

Zisapel N

Subjects

Clinical Trials as Topic, GABA Modulators administration & dosage, GABA Modulators adverse effects, GABA Modulators economics, Histamine H1 Antagonists administration & dosage, Histamine H1 Antagonists adverse effects, Histamine H1 Antagonists economics, Humans, Hypnotics and Sedatives administration & dosage, Hypnotics and Sedatives adverse effects, Hypnotics and Sedatives economics, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Marketing, Neuropeptides antagonists & inhibitors, Orexins, Receptors, GABA-A metabolism, Receptors, Melatonin agonists, Serotonin 5-HT2 Receptor Antagonists administration & dosage, Serotonin 5-HT2 Receptor Antagonists adverse effects, Serotonin 5-HT2 Receptor Antagonists economics, Treatment Outcome, Drug Discovery, GABA Modulators therapeutic use, Histamine H1 Antagonists therapeutic use, Hypnotics and Sedatives therapeutic use, Serotonin 5-HT2 Receptor Antagonists therapeutic use, Sleep Initiation and Maintenance Disorders drug therapy

Abstract

Introduction: Sleep is a vital neurochemical process involving sleep-promoting and arousal centers in the brain. Insomnia is a pervasive disorder characterized by difficulties in initiating or maintaining or non-refreshing (poor quality) sleep and clinically significant daytime distress. Insomnia is more prevalent in women and old age and puts sufferers at significant physical and mental health risks. This review summarizes published data on the current and emerging insomnia drug classes, rationale for development and associated risks/benefits. (Summary of Product Characteristics and Medline search on "hypnotic" or specific drug names and "Insomnia")., Areas Covered: GABA(A) receptor modulators facilitate sleep onset and some improve maintenance but increase risk of dependence, memory, cognitive and psychomotor impairments, falls, accidents and mortality. Melatonin receptor agonists improve quality of sleep and/or sleep onset but response may develop over several days. They have more benign safety profiles and are indicated for milder insomnia, longer usage and (prolonged release melatonin) older patients. Histamine H-1 receptor antagonists improve sleep maintenance but their effects on cognition, memory and falls remain to be demonstrated. Late-stage pipeline orexin OX1/OX2 and serotonin 5HT2A receptor antagonists may hold the potential to address several unmet needs in insomnia pharmacotherapy but safety issues cast some doubts over their future., Expert Opinion: Current and new insomnia drugs in the pipeline target different sleep regulating mechanisms and symptoms and have different tolerability profiles. Drug selection would ideally be based on improvement in the quality of patients' sleep, overall quality of life and functional status weighed against risk to the individual and public health.

Published

2012

49. Recurrent clozapine and lorazepam withdrawal psychosis with catatonia.

Author

Wang BZ, Gupta A, Bastiampillai T, and Sani F

Subjects

Adult, Antipsychotic Agents administration & dosage, Antipsychotic Agents adverse effects, Antipsychotic Agents pharmacokinetics, Disease Management, Female, GABA Modulators administration & dosage, GABA Modulators adverse effects, GABA Modulators pharmacokinetics, Humans, Remission Induction, Treatment Outcome, Withholding Treatment, Catatonia chemically induced, Clozapine administration & dosage, Clozapine adverse effects, Clozapine pharmacokinetics, Lorazepam administration & dosage, Lorazepam adverse effects, Lorazepam pharmacokinetics, Schizophrenia drug therapy, Substance Withdrawal Syndrome therapy

Published

2012

50. Localized exfoliating rash with paresthesia possibly due to clonazepam.

Author

Munoli RN, Praharaj SK, and Bhatt SM

Subjects

Child, Clonazepam therapeutic use, Drug Eruptions pathology, GABA Modulators therapeutic use, Humans, Male, Clonazepam adverse effects, Drug Eruptions etiology, GABA Modulators adverse effects, Paresthesia chemically induced

Published

2012