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Clinical neuropharmacology

ISSN 1537-162X

8 papers in the library · 80 citations · publishing 0-2026

Papers

Phenomenologic comparison of the idiopathic psychosis of schizophrenia and drug-induced cocaine and phencyclidine psychoses: a retrospective study.

Clinical neuropharmacology August 1, 1994 R B Rosse, J P Collins, M Fay-Mccarthy et al. 62 citations

Cocaine-induced psychosis and PCP-induced psychosis each resemble some symptoms of schizophrenia but differ in their specific features. In a retrospective study of 34 male crack-cocaine-dependent patients without other psychiatric disorders and 16 actively psychotic men with schizophrenia, certain First Rank Schneiderian Symptoms such as thought broadcasting and thought withdrawal were more common in the schizophrenic group. In a separate group of 22 cocaine addicts with past use of both cocaine and PCP, the frequency of these symptoms during intoxication was similar for both drugs.

The Impact of Preoperative Low-Dose Esketamine and Dexmedetomidine Nasal Administration on the Emergence Delirium in Children Undergoing Fiber Bronchoscopy: A Prospective Randomized Controlled Trial.

Clinical neuropharmacology Wei Xie, Le Wang, Zhe Peng et al. 6 citations

Preoperative nasal administration of low-dose esketamine or dexmedetomidine reduces emergence delirium after pediatric fiberoptic bronchoscopy. In a randomized trial of 126 children aged 1–6 years, emergence delirium occurred in 7.14% of those given 1.0 mg/kg esketamine and 18.6% of those given 1.0 μg/kg dexmedetomidine, compared with 48.78% in the saline control group. Both drugs also lowered postoperative pain intensity. Dexmedetomidine prolonged the time to awaken and open eyes in the recovery unit, while hemodynamics, oral secretions, and recovery-stay duration did not differ among groups.

Effectiveness of Mindfulness-Based Cognitive Therapy on Depressive Symptoms, Brain Potential, and Neuroimmunoinflammatory Factors in Depressed Patients.

Clinical neuropharmacology Jiancheng Qiu, Yifei Gong, Xiucui Zhang et al. 4 citations

Adding mindfulness-based cognitive therapy (MBCT) to standard treatment reduces depressive symptoms more than standard treatment alone in people with depression. In a randomized trial with 64 patients, those receiving MBCT plus conventional therapy showed greater decreases on the Hamilton Depression Rating Scale and lower levels of inflammatory markers tumor necrosis factor α and interleukin-6, along with larger increases in quality of life scores, response execution, and serotonin. Brain potential measures also improved, with shorter latency and longer amplitude. The combination therapy appears to suppress inflammation and sharpen attention and response to target stimuli.

Effect of Ketamine Treatment on Social Withdrawal in Autism and Autism-Like Conditions.

Clinical neuropharmacology Megan Ralston, Alim Osman, Pavan Suryadevara et al. 4 citations

A review of the current literature on ketamine for social withdrawal in autism spectrum disorder (ASD) found only two original studies and five case reports. The two studies showed mixed results: esketamine produced no statistically significant improvement, while intravenous ketamine alleviated social withdrawal symptoms, especially in the short term. Neither study reported many serious adverse events. The five case reports indicated decreased depressive symptoms and some evidence of improved social functioning. Evidence for improved social condition exists, but research is limited, and further studies with larger samples and varied doses and administration methods are needed.

Exploring Psychedelics Pharmacology: A Scoping Review Charting the Course of Psilocybin Pharmacokinetics.

Clinical neuropharmacology Ramiro Manzano-Nunez, Diego A Gomez, Catalina Toledo-Mendoza et al. 3 citations

A scoping review of five controlled clinical trials involving 112 healthy volunteers describes how psilocybin is processed in the body after oral administration. Peak psilocin concentrations in plasma ranged from 8.2 to 37.2 ng/mL, typically reached about two hours after dosing. The elimination half-life varied from 1.2 to 3.3 hours. A strong positive relationship between dose and maximum concentration was observed. No serious adverse events occurred. No studies reported pharmacokinetic data from patients with depression or those transitioning to palliative care, highlighting a gap in research on target populations.

Evaluating Delta-8-THC-Induced Psychosis: A Systematic Review.

Clinical neuropharmacology Megan Jayne Ralston, Alim Osman 1 citation

Delta-8-THC, a cannabinoid gaining popularity, poses significant psychiatric risks including psychosis, mood lability, and cannabinoid hyperemesis syndrome, particularly in individuals with preexisting conditions, despite being less intoxicating than delta-9-THC. A review of six case reports involving 9 patients, mostly males in their 20s with varied psychiatric histories, found that symptoms and clinical outcomes varied. The lack of FDA regulation and easy availability of delta-8-THC products heighten these risks, highlighting the need for more rigorous studies to inform regulatory actions.

Ketamine for the Treatment of Obsessive-Compulsive Disorder (OCD): A Systematic Review on Efficacy and Tolerability.

Clinical neuropharmacology June 19, 2026 Isabela Heroiu, Gia Han Le, Maria-Christina Sioufi et al.

Ketamine, an N-methyl-D-aspartate receptor antagonist, consistently and significantly reduced obsessive-compulsive disorder symptom severity by up to 50% to 60% across five studies, though the duration of effects ranged from a few hours to six weeks. Ketamine was generally well tolerated. The review included three randomized controlled trials and two open-label trials with variable routes of administration (intravenous, intramuscular, and oral) and dosing frequencies. Further research is needed to optimize ketamine treatment for sustained symptom reduction.

An Open-Label Study of Single-Dose Psilocybin for Borderline Personality Disorder With Co-Occurring Major Depressive Disorder.

Clinical neuropharmacology April 1, 2026 Jon E Grant, Sophia Boutouis, Margaret O'Brien et al.

A small open-label pilot study tested a single dose of psilocybin in nine adults aged 18 to 65 with both borderline personality disorder (BPD) and major depressive disorder (MDD). Depressive symptoms significantly improved from baseline to four weeks after dosing, with average scores dropping from 28.56 to 17.22. However, BPD symptoms did not show a significant change. The findings suggest that BPD may not interfere with psilocybin's effect on depressive symptoms, but larger clinical trials are needed.