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13. Pharmacokinetics and Bioequivalence Evaluation of Trazodone Hydrochloride Sustained‐Release Tablets in Healthy Chinese Volunteers.

Author

Wang, Jingyan, Xu, Yuan, Zhao, Zhicheng, Meng, Tian, Zou, Yang, and Lan, Yi

Abstract

The aim of this study was to investigate the pharmacokinetics, bioequivalence, and safety of generic trazodone hydrochloride sustained‐release tablet and its reference listed product in healthy Chinese subjects. An open, randomized, single‐dose, and 2‐period crossover study was involved under fasting and fed conditions, with a 7‐day washout period. A single oral dose of 150 mg of 2 trazodone hydrochloride sustained‐release tablets was administered to 84 healthy volunteers, with 36 in the fasting group and 48 consuming a high‐fat diet, respectively. The plasma concentrations of trazodone were analyzed using a liquid chromatography‐tandem mass spectrometry method, and pharmacokinetic parameters were obtained from concentration‐time profiles. The geometric mean ratio with 90% confidence intervals of the maximum trazodone concentration, area under the plasma concentration‐time curve (AUC) from time 0 to the last measurable concentration, and AUC from time 0 to infinity were within the bioequivalence acceptance criteria (80%‐125%) under fasting and fed conditions, which indicated that the test and reference formulations were bioequivalent. Compared with the fasting study, the concomitant administration of trazodone with a high‐fat diet had a negligible influence on the drug pharmacokinetic behavior. Adverse events were recorded, and no serious adverse events were observed during either fasting or fed conditions. Trazodone has proven to have an acceptable safety profile in the Chinese population, with bioequivalence successfully established under both fasting and fed conditions. [ABSTRACT FROM AUTHOR]

Published
2024
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14. Efficacy comparison of five antidepressants in treating anxiety and depression in cancer and non-cancer patients.

Author

Zhao, Kuan, Wang, Youyang, Liu, Qun, Yu, Ze, and Feng, Wei

Subjects
GENERALIZED anxiety disorder, MENTAL depression, SLEEP quality, TRAZODONE, OLDER people, ANXIETY disorders
Abstract

Introduction: Cancer patients have a heightened susceptibility to anxiety and depressive disorders, which significantly impact the effectiveness of cancer treatments and long-term quality of life. This study aimed to compare the efficacy of different antidepressants in cancer and non-cancer patients. Methods: A total of 610 patients diagnosed with depressive episodes and/or anxiety disorders were retrospectively included and divided into a cancer group and a non-cancer control group. Antidepressants used included escitalopram, duloxetine, sertraline, venlafaxine, and vortioxetine, combined with trazodone or not. The Patient Health Questionnaire-9 (PHQ-9) and the Generalized Anxiety Disorder Questionnaire-7 (GAD-7) scores were used to evaluate the efficacy after 4 weeks and 8 weeks of systematic antidepressants treatment. Results: Compared to the non-cancer group, the cancer group had higher proportions of females, older individuals, and patients with poor sleep quality, while reporting fewer somatic symptoms at baseline (all p < 0.05). PHQ-9 and GAD-7 scores in cancer patients treated with antidepressants were significantly lower than baseline at week 4 and week 8 (all p < 0.05). The sertraline group demonstrated significantly less improvement in GAD-7 scores at week 4 and in both GAD-7 and PHQ-9 scores at week 8 compared to the escitalopram group, while duloxetine, venlafaxine, and vortioxetine showed comparable efficacy to escitalopram. Antidepressants combined with trazodone showed significant improvement in PHQ-9 scores at week 4 compared to those without trazodone. The gynecological cancer group showed significantly more improvement in GAD-7 and PHQ-9 scores at week 4 and 8 compared to breast cancer patients. Conclusion: Antidepressant treatment in cancer patients with anxiety and depression is as effective as in non-cancer patients. The efficacy of escitalopram is comparable to duloxetine, venlafaxine, and vortioxetine, all of which outperformed sertraline in cancer patients. [ABSTRACT FROM AUTHOR]

Published
2024
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15. Oral trazodone results in quantifiable sedation but does not result in a xylazine-sparing effect in healthy adult horses.

Author

Swanton, William E., Johnson, Rebecca, Qianqian Zhao, and Schroeder, Carrie

Subjects
*ORAL drug administration, *TRAZODONE, *CONSCIOUS sedation, *XYLAZINE, *COLLEGE teaching
Abstract

OBJECTIVE: To evaluate sedation and IV xylazine requirements to achieve 45% of baseline head height above ground measurements following oral (PO) administration of 2 trazodone dosages. METHODS: 8 healthy, adult mares of various weights and breeds belonging to a university teaching herd were utilized in a blinded, crossover study design. Horses were randomly assigned to 1 of 3 PO treatments: control (no trazodone), trazodone at 3 mg/kg (low dose [LD]), or trazodone at 6 mg/kg (high dose [HD]). Before treatment, cardiac auscultation, EquiSed sedation score, and head height above ground (HHAG; cm) measurements were performed (baseline) followed by feeding of the treatment mixture. After 120 minutes, sedation score and HHAG were recorded. Xylazine was administered IV (0.25 mg/kg bolus followed by 0.1 mg/kg/min) until HHAG reached 45% of baseline or a total dose of 1 mg/kg was reached. Individual data for xylazine dosage, sedation scores, and HHAG were analyzed using mixed linear models with repeated measures. RESULTS: Sedation scores were significantly improved (LD, P = .045; HD, P = .01) and HHAG was lowered (LD, P = .045; HD, P = .09) by trazodone administration. Xylazine dose requirements were increased by LD trazodone administration (increase of 0.26 ± 0.26 mg/kg; P = .03) and unchanged by HD (increase of 0.13 ± 0.25 mg/kg; P = .38). CONCLUSIONS: Oral trazodone administration increases quantifiable sedation in horses. Xylazine requirements are significantly increased by LD trazodone administration. CLINICAL RELEVANCE: Oral administration of LD trazodone may increase xylazine requirements. Further clinical studies are required to fully assess the CLINICAL RELEVANCE: of this finding on other parameters such as cardiovascular physiology. [ABSTRACT FROM AUTHOR]

Published
2024
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16. A Randomized-Controlled Trial Targeting Cognition in Early Alzheimer's Disease by Improving Sleep with Trazodone (REST).

Author

Eyob, Estelle, Shaw, Jacob S., Bakker, Arnold, Munro, Cynthia, Spira, Adam, Wu, Mark, Rabinowitz, Jill A., Peters, Matthew, Wanigatunga, Sarah, Zipunnikov, Vadim, Thompson, Richard, Burhanullah, M. Haroon, Leoutsakos, Jeannie-Marie, Rosenberg, Paul, and Greenberg, Barry

Subjects
*SLEEP interruptions, *SLOW wave sleep, *ALZHEIMER'S disease, *MILD cognitive impairment, *SLEEP stages
Abstract

Alzheimer's disease (AD) is a leading cause of mortality and morbidity among aging populations worldwide. Despite arduous research efforts, treatment options for this devastating neurodegenerative disease are limited. Sleep disturbances, through their link to changes in neural excitability and impaired clearance of interstitial abnormal protein aggregates, are a key risk factor for the development of AD. Research also suggests that the neuroprotective effects of sleep are particularly active during slow wave sleep. Given the strong link between sleep disturbance and AD, targeting sleep in the prodromal stages of AD, such as in mild cognitive impairment (MCI), represents a promising avenue for slowing the onset of AD-related cognitive decline. In efforts to improve sleep in older individuals, several pharmacologic approaches have been employed, but many pose safety risks, concern for worsening cognitive function, and fail to effectively target slow wave sleep. Trazodone, a safe and widely used drug in the older adult population, has shown promise in inducing slow wave sleep in older adults, but requires more rigorous research to understand its effects on sleep and cognition in the prodromal stages of AD. In this review, we present the rationale and study design for our randomized, double-bind, placebo-controlled, crossover trial (NCT05282550) investigating the effects of trazodone on sleep and cognition in 100 older adults with amnestic MCI and sleep complaints. [ABSTRACT FROM AUTHOR]

Published
2024
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17. Safety and efficacy of memantine and trazodone versus placebo for motor neuron disease (MND SMART): stage two interim analysis from the first cycle of a phase 3, multiarm, multistage, randomised, adaptive platform trial.

Author

Pal, Suvankar, Chataway, Jeremy, Swingler, Robert, Macleod, Malcolm R, Carragher, Neil O, Hardingham, Giles, Selvaraj, Bhuvaneish Thangaraj, Smith, Colin, Wong, Charis, Newton, Judith, Lyle, Dawn, Stenson, Amy, Dakin, Rachel S, Ihenacho, Amarachi, Colville, Shuna, Mehta, Arpan R, Stallard, Nigel, Carpenter, James R, Parker, Richard A, and Keerie, Catriona

Subjects
*SPINAL muscular atrophy, *MOTOR neuron diseases, *AMYOTROPHIC lateral sclerosis, *TERMINATION of treatment, *TRAZODONE
Abstract

Motor neuron disease represents a group of progressive and incurable diseases that are characterised by selective loss of motor neurons, resulting in an urgent need for rapid identification of effective disease-modifying therapies. The MND SMART trial aims to test the safety and efficacy of promising interventions efficiently and definitively against a single contemporaneous placebo control group. We now report results of the stage two interim analysis for memantine and trazodone. MND SMART is an investigator-led, phase 3, double-blind, placebo-controlled, multiarm, multistage, randomised, adaptive platform trial recruiting at 20 hospital centres in the UK. Individuals older than 18 years with a confirmed diagnosis of either amyotrophic lateral sclerosis classified by the revised El Escorial criteria, primary lateral sclerosis, progressive muscular atrophy, or progressive bulbar palsy, regardless of disease duration, were eligible for screening. Participants were randomised (1:1:1) to receive oral trazodone 200 mg once a day, oral memantine 20 mg once a day, or matched placebo using a computer-generated minimisation algorithm delivered via a secure web-based system. Co-primary outcome measures were clinical functioning, measured by rate of change in the Amyotrophic Lateral Sclerosis Functional Rating Scale Revised (ALSFRS-R), and survival. Comparisons were conducted in four stages, with predefined criteria for stopping at the end of stages one and two. We report interim analysis from the stage two results, which was done when 100 participants per group (excluding long survivors, defined as >8 years since diagnosis at baseline) completed a minimum of 12 months of follow-up for the candidate investigational medicinal products. The trial is registered on the European Clinical Trials Registry, 2019–000099–41, and ClinicalTrials.gov , NCT04302870 , and is ongoing. Between Feb 27, 2020, and July 24, 2023 (database lock for interim analysis two), 554 people with a motor neuron disease were randomly allocated to memantine (183 [33%]), trazodone (185 [33%]), or placebo (186 [34%]). The primary interim analysis population comprised 530 participants, of whom 175 (33%) had been allocated memantine, 175 (33%) had been allocated trazodone, and 180 (34%) had been allocated placebo. Over 12 months of follow-up, the mean rate of change per month in ALSFRS-R was –0·650 for memantine, –0·625 for trazodone, and –0·655 for placebo (memantine versus placebo estimated mean difference 0·033, one-sided 90% CI lower level –0·085; one-sided p=0·36; trazodone vs placebo: 0·065, –0·051; one-sided p=0·24). The one-sided p values were both above the significance threshold of 10%, indicating that neither memantine nor trazodone groups met the criteria for continuation. There were 483 participants with at least one adverse event (145 [77%] on placebo, 170 [91%] on memantine, and 168 [90%] on trazodone). There were 88 participants with at least one serious adverse event (37 [20%] on memantine, 27 [14%] on trazodone, and 24 [13%] on placebo). A total of 11 serious adverse event led to treatment discontinuation. There was no survival difference between comparisons, with 49 deaths in the memantine group, 52 deaths in the trazodone group, and 48 deaths in the placebo group. Neither memantine nor trazodone improved efficacy outcomes compared with placebo. This result is sufficiently powered to warrant no further testing of trazodone or memantine in motor neuron disease at the doses evaluated in this study. The multiarm multistage design shows important benefits in reducing the time, cost, and participant numbers to reach a definitive result. The Euan MacDonald Centre, MND Scotland, My Name'5 Doddie Foundation, and Baillie Gifford. [ABSTRACT FROM AUTHOR]

Published
2024
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18. Trazodone counteracts the response of microglial cells to inflammatory stimuli.

Author

Chelucci, Elisa, Daniele, Simona, Vergassola, Matteo, Ceccarelli, Lorenzo, Zucchi, Sara, Boltri, Luigi, and Martini, Claudia

Subjects
*NEUROGLIA, *NATURAL immunity, *HUMAN cloning, *QUINOLINIC acid, *TRAZODONE
Abstract

Microglia are resident brain cells that regulate neuronal development and innate immunity. Microglia activation participates in the cellular response to neuroinflammation, thus representing a possible target for pharmacological strategies aimed to counteract the onset and progression of brain disorders, including depression. Antidepressant drugs have been reported to reduce neuroinflammation by acting also on glial cells. Herein, the potential anti‐inflammatory and neuroprotective effects of trazodone (TRZ) on the microglial human microglial clone 3 (HMC3) cell line were investigated. HMC3 cells were activated by a double inflammatory stimulus (lipopolysaccharide [LPS] and tumour necrosis factor‐alpha [TNF‐α], 24 h each), and the induction of inflammation was demonstrated by (i) the increased expression levels of nuclear factor kappa‐light‐chain‐enhancer of activated B cells (NF‐kB) and ionized calcium‐binding adapter molecule 1 (IBA‐1), and (ii) the increased release of interleukin 6 (IL‐6) and transforming growth factor‐beta (TGF‐β). TRZ effects were evaluated by treating HMC3 cells for 24 h before (pre‐treatment) and after (post‐treatment) the double inflammatory stimulus. Notably, TRZ treatments significantly decreased the expression of NF‐kB and IBA‐1 and the release of the cytokines IL‐6 and TGF‐β. Moreover, TRZ prevented and reduced the release of quinolinic acid (QUIN), a known neurotoxic kynurenine metabolite. Finally, cellular supernatants collected from microglial cells pre‐treated LPS‐TNF‐α with TRZ were able to improve neuronal‐like cell viability, demonstrating a potential neuroprotective effect. Overall, this study suggests the anti‐inflammatory effects of TRZ on human microglia and strives for its neuroprotective properties. [ABSTRACT FROM AUTHOR]

Published
2024
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19. Evaluation of the sedative properties of oral trazodone, gabapentin or their combination in healthy cats.

Author

Tucker, Laura E, Sanchez, Andrea, Valverde, Alexander, Blois, Shauna, Monteith, Gabrielle, Longworth, Pamela, Downie, Alison, Gu, Yu, and Johnson, Ron

Abstract

Objectives: Sedation before veterinary visits is advocated to help reduce fear and anxiety in cats and facilitate safe handling. The aim of this study was to evaluate the effectiveness of trazodone, gabapentin and a trazodone/gabapentin combination for oral sedation in healthy feline patients before blood donation. Methods: A total of 21 cats were included in the study. Baseline sedation scores were obtained, and cats were randomly assigned to receive oral trazodone at 5 mg/kg (T), oral gabapentin at 10 mg/kg (G), their combination (TG) or placebo (control group). A sedation score was obtained 1 h after drug administration. A blood sample was obtained at the time of blood collection for quantification of drug plasma concentrations. Agreement between observers was tested with a Cohen's Kappa test. Sign tests to compare change within treatment and a Skilling–Mack rank ANOVA to test for differences between groups were performed to compare pre- and post-sedation scores as well as a magnitude of differences over time between the groups. A Spearman's rank correlation coefficient test was used to correlate sedation scores with drug plasma concentrations. Results: Post-sedation final scores were significantly higher only in the T (P = 0.022) and TG groups (P <0.001). The magnitude of change between pre- and post-sedation scores was larger in the TG (P <0.0032) and T groups (P <0.038) compared with the control group. There were no other significant differences between the groups. There was no correlation between drug plasma concentrations and sedation scores in any of the groups. Conclusions and relevance: Administration of oral trazodone alone at 5 mg/kg or in combination with gabapentin at 10 mg/kg resulted in significant sedation in healthy cats with no evident side effects. The degree of sedation was more profound when both drugs were combined, but a gabapentin dose of 10 mg/kg alone failed to provide significant sedation in this population. [ABSTRACT FROM AUTHOR]

Published
2024
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20. Effect of antidepressants on ejaculation dysfunction in patients with depression and anxiety: A systematic review and network meta‐analysis.

Author

Wang, Qihua, Xu, Zhunan, Chen, Xiangyu, Liu, Li, and Liu, Xiaoqiang

Subjects
*SEROTONIN uptake inhibitors, *MENTAL depression, *ANTIDEPRESSANTS, *TRAZODONE, *MEDICAL personnel
Abstract

Introduction Methods Results Conclusions Antidepressants may lead to a series of sexual adverse effects (SAEs), among which ejaculation dysfunction (EjD) is often overlooked by clinicians. The purpose of the present network meta‐analysis was to assist drug adjustment by comparing and ranking the incidence of EjD among various antidepressants.Relevant studies were retrieved from PubMed, Embase, Scopus, Web of Science, ClinicalTrials.gov, and other additional records. Eligible randomized controlled trials (RCTs) assessed the rate of EjD in patients with major depressive disorder (MDD) and anxiety disorder after taking anti‐depressants. The incidences of EjD, erectile dysfunction (ED), decreased libido (DL), adverse events (AE), withdrawal due to adverse events (WDAE) and withdrawal due to lack of efficacy (WDLE) were pooled using odds ratio (OR) with their 95% confidence intervals (CI). The values of surface under the cumulative ranking curve (SUCRA) helped to rank the risk of each outcome in different antidepressants.Thirty RCTs comprising 18,157 patients were included. Results of all node‐splitting analysis demonstrated no statistical inconsistency (all P > 0.05). Clomipramine (OR 42.11, 95% CI [9.90, 179.08]), WS5570 (OR 28.99, 95% CI [1.48, 568.97]) and paroxetine (OR 18.63, 95% CI [9.33, 37.23]) had significant risk of EjD comparing to placebo. Additionally, duloxetine (OR 7.37, 95% CI [2.61, 20.78]), clomipramine (OR 5.29, 95% CI [1.72, 16.25]), paroxetine (OR 3.75, 95% CI [1.37, 10.26]) and escitalopram (OR 3.04, 95% CI [1.20, 7.71]) presented higher risk of ED comparing to placebo. Agomelatine, levomilnacipran, vortioxetine, trazodone, vilazodone, fluvoxamine and imipramine exhibited similar incidence of EjD with placebo (all P > 0.05). Besides, trazodone, vilazodone and vortioxetine had the top‐five SUCRA values in each of SAEs (EjD, ED and DL), and agomelatine might be alternative in EjD and DL. Considering about AE, WDAE and WDLE, vilazodone appeared to offer more satisfactory performance across all these aspects.For patients undergoing SAEs following the administration of antidepressants, trazodone, vortioxetine, vilazodone and agomelatine are alternative antidepressants. [ABSTRACT FROM AUTHOR]

Published
2024
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21. Case report: Personalizing the use of trazodone in real-world patients: a study of three cases of depression with comorbidities.

Author

Rosso, Gianluca, Benatti, Beatrice, Pettorruso, Mauro, Sampogna, Gaia, and Tomasetti, Carmine

Subjects
MENTAL depression, SEROTONIN antagonists, PARKINSON'S disease, PHYSICIANS, TRAZODONE
Abstract

Depressive disorders are leading contributors to the global mental health-related burden, and they represent a challenge for real-world clinicians, due to the low rates of remission despite the high availability of treatments. Often, depression shows in the context of multiple chronic comorbidities, thus requiring precise and accurate management of pharmacological treatments to avoid interactions and side effects. These criticalities call for the need for new strategies of treatment, which may include new insights into the pharmacological properties of currently available antidepressant drugs, to enhance their efficacy in the different contexts in which depression may arise. Trazodone is the prototype serotonin antagonist/reuptake inhibitor antidepressant (SARI). Due to the malleability granted by its multiple formulations, trazodone is frequently used to treat depression, both as an add-on to other antidepressants and as a monotherapy, with satisfying results. Moreover, its tolerability makes it one of the most prescribed antidepressants in patients with poly-treated comorbid medical illnesses, especially in the elderly. Herein, a case series is presented regarding the use of trazodone in patients with complex comorbid diagnoses or distressing side effects. Each of the three cases has been discussed in three specific Round Tables, involving expert clinicians in the fields of Psychiatry, Neurology, General Practice, and Geriatrics using the Nominal Group Technique. The ideas collected have been used to integrate the cases and the discussion with the intent of facilitating accessibility to the widest audience of physicians and clinical workers in different clinical practice contexts. The final aim of this paper is to promote an increasingly personalized use of trazodone in realworld patients with depression. [ABSTRACT FROM AUTHOR]

Published
2024
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22. Use of transdermal trazodone before veterinary visit to reduce stress and anxiety in cats.

Author

Shih, Pei-Chi and Wang, Shang-Lin

Abstract

Trazodone hydrochloride is a tetracyclic antidepressant commonly used in human, gaining popularity in feline patients as a pre-appointment anxiolytic and sedative medication. However, the oral administration route in cats poses difficulties for owners and limits practicality. This study evaluated the efficacy and safety of transdermal trazodone in cats. At the first visit, the cat stress score (CSS), global sedation score (GSS), behavioral response score (BRS), and owner-assessed overall experience score (OES) were used to observe and record the behavior during transportation and examination. Thereafter, each cat was given 150 mg of transdermal trazodone before the second visit. The respiratory rate, heart rate, pulse rate, systolic blood pressure, blood test, adverse effects, and response time were compared between the two visits. Thirteen cats were enrolled in this study. Transdermal trazodone significantly lowered CSS of outward trip (P = 0.005) and return trip (P = 0.005) (Wilcoxon signed-rank test). No significant differences were observed in CSS and GSS during the examination. Moreover, the BRS was significantly low (P = 0.018), but the significance varied depending on the examination procedure and behavior. The OES questionnaire showed a significant reduction in stress during the outward trip (P = 0.002), return trip (P = 0.005), and examination (P = 0.003) (all Wilcoxin signed ranks test). Physiologic parameters and laboratory values were not significantly affected, and the adverse effects were few and mild. In conclusion, transdermal trazodone was well tolerated at a single dose of 150 mg/cat. It can reduce stress and anxiety before a veterinary visit, resulting in a better patient-owner experience. • Transdermal trazodone was well tolerated at a single dose of 150 mg/cat. • Transdermal trazodone significantly lower stress and anxiety during transportation. • Most owners give positive feedback to this method of trazodone administration. • Transdermal trazodone results in a better patient-owner experience. [ABSTRACT FROM AUTHOR]

Published
2024
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23. Cognitive dysfunction and owner-directed aggression in a 10-year-old neutered golden retriever: A case report.

Author

Perry, Pamela J.

Abstract

A 10-year-old, 38.5 kg, male neutered golden retriever was evaluated for a 2-year history of growling, baring teeth, and biting his owners. The dog also displayed disorientation, increased vocalization, altered interactions with the female owner, anxiety, and nighttime restlessness. A primary diagnosis of cognitive dysfunction syndrome and concurrent diagnosis of owner-directed aggression related to altered cognition or awareness, pain/discomfort, and impulse control/conflict was made based on the dog's age, behavioral signs, and exclusion of medical causes. The owners were provided with a treatment plan that included environmental and safety management, reward-based behavior modification, and an antioxidant-rich diet. After the addition of a selective serotonin reuptake inhibitor (fluoxetine) and a serotonin antagonist and reuptake inhibitor (trazodone), the dog's clinical signs were significantly improved within six months and sustained during a 2-year follow-up period. • A 10-year-old dog presented for aggression towards the owners, disorientation, increased vocalization, altered social interactions, anxiety, and nighttime restlessness. • A primary diagnosis of canine cognitive dysfunction and concurrent diagnosis of owner directed aggression related to altered cognition or awareness, pain/discomfort, and impulse control/conflict was made based on the dog's age and behavioral signs and exclusion of medical causes. • Treatment included management, reward-based behavior modification, an antioxidant-rich diet, a selective serotonin reuptake inhibitor (fluoxetine) and a serotonin antagonist and reuptake inhibitor (trazodone). • Improvement of clinical signs was noted within 6 months and sustained during a 2-year follow-up period. [ABSTRACT FROM AUTHOR]

Published
2024
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24. Evaluation of three doses of oral trazodone and their impact on handling, activity, and physiological parameters in rabbits: a prospective, blinded, randomized cross-over study.

Author

WATANABE, Ryota, GIBERT, Adalaïs, BENITO, Javier, GARBIN, Marta, KWONG, Grace P. S., DESMARCHELIER, Marion, and BENEDETTI, Inga-Catalina CRUZ

Subjects
BLOOD gases, VISUAL analog scale, TRAZODONE, CHI-squared test, RABBITS
Abstract

No study has determined the minimal effective dose of trazodone required to induce behavioral changes and its safety profile in rabbits. Therefore, this study aimed to determine the minimal effective dose of trazodone to improve compliance to handling, and to evaluate associated changes in motor activity, physiological and arterial blood gas parameters. Eight intact female New Zealand White rabbits (2-month-old; 1.66 ± 0.12 kg) were included in this prospective, blinded, randomized cross-over study. After a 10-day acclimation, rabbits randomly received placebo or trazodone 10, 20 or 30 mg/kg orally (PLAC, TRAZ10, TRAZ20, TRAZ30) with a 1-week wash-out period. Compliance scoring (dynamic interactive visual analog scale; DIVAS), activity levels measured with accelerometry (T0-T600), physiological parameters (temperature, heart, and respiratory rates), and arterial blood gas parameters (up to T240) were evaluated. Compliance scores, accelerometry, physiological and arterial blood gas parameters and hypoxemia prevalence (PaO2 <60 mmHg) were analyzed using linear mixed models and Chi-squared tests, respectively (P<0.05). When compared with PLAC, DIVAS scores were significantly higher at T80-120, T40-120 and T120-200 in TRAZ10, TRAZ20 and TRAZ30 post-administration, respectively. When compared with baseline, DIVAS scores were significantly higher from T80-160, T40-240 and T80-200 in TRAZ10, TRAZ20 and TRAZ30, respectively. All other parameters were not significantly different. In TRAZ30, hypoxemia was observed in 2/8 rabbits (P=0.104). In conclusion, oral trazodone improved rabbit compliance at all studied dosages, especially 20 mg/kg improved rabbit compliance without decreasing motor activity or causing hypoxemia. [ABSTRACT FROM AUTHOR]

Published
2024
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25. Effects of Trazodone and Dexmedetomidine on Fentanyl-Mediated Reduction of Isoflurane Minimum Alveolar Concentration in Cats

Author

Brosnan, Robert J, Pypendop, Bruno H, and Cenani, Alessia

Subjects
Veterinary Sciences, Agricultural, Veterinary and Food Sciences, anesthesia, dexmedetomidine, feline, fentanyl, isoflurane, trazodone, Veterinary sciences
Abstract

OBJECTIVE: To screen modulators of biogenic amine (BA) neurotransmission for the ability to cause fentanyl to decrease isoflurane minimum alveolar concentration (MAC) in cats, and to test whether fentanyl plus a combination of modulators decreases isoflurane MAC more than fentanyl alone. STUDY DESIGN: Prospective, experimental study. ANIMALS: A total of six adult male Domestic Short Hair cats. METHODS: Each cat was anesthetized in three phases with a 1 week washout between studies. In phase 1, anesthesia was induced and maintained with isoflurane, and MAC was measured in duplicate using a tail clamp stimulus and standard bracketing technique. A 21 ng mL-1 fentanyl target-controlled infusion was then administered and MAC measured again. In phase 2, a single cat was administered a single BA modulator (buspirone, haloperidol, dexmedetomidine, pregabalin, ramelteon or trazodone) in a pilot drug screen, and isoflurane MAC was measured before and after fentanyl administration. In phase 3, isoflurane MAC was measured before and after fentanyl administration in cats co-administered trazodone and dexmedetomidine, the two BA modulator drugs associated with fentanyl MAC-sparing in the screen. Isoflurane MAC-sparing by fentanyl alone, trazodone-dexmedetomidine and trazodone-dexmedetomidine-fentanyl was evaluated using paired t tests with p < 0.05 denoting significant effects. RESULTS: The MAC of isoflurane was 1.87% ± 0.09 and was not significantly affected by fentanyl administration (p = 0.09). In the BA screen, cats administered trazodone or dexmedetomidine exhibited 26% and 22% fentanyl MAC-sparing, respectively. Trazodone-dexmedetomidine co-administration decreased isoflurane MAC to 1.50% ± 0.14 (p < 0.001), and the addition of fentanyl further decreased MAC to 0.95% ± 0.16 (p < 0.001). CONCLUSIONS AND CLINICAL RELEVANCE: Fentanyl alone does not affect isoflurane MAC in cats, but co-administration of trazodone and dexmedetomidine causes fentanyl to significantly decrease isoflurane requirement.

Published
2023

28. Take It Easy! Serotonin Syndrome Precipitated by the Rapid Titration of Sertraline and Trazodone in the Setting of Risperidone Use.

Author

Martino, Julie, Elfessi, Zane, Szaflarska, Katarzyna, Suh, Melody, and Antonishina, Katerina

Subjects
*COMBINATION drug therapy, *MYOCLONUS, *MOUTH, *BENZODIAZEPINES, *NEUROMUSCULAR diseases, *SEROTONIN uptake inhibitors, *SERTRALINE, *RISPERIDONE, *TRANQUILIZING drugs, *VOLUMETRIC analysis, *BODY temperature, *HEART beat, *SEROTONIN syndrome, *TRAZODONE, *PSYCHOSOCIAL factors, *DISEASE risk factors
Abstract

Serotonin syndrome is a potentially life-threatening condition caused by a toxic excess of serotonin leading to overstimulation of the nervous system. Because it is a diagnosis of exclusion, it can be underrecognized, making the true incidence unknown. The classic triad of serotonin syndrome includes neuromuscular excitation, autonomic instability and altered mental status. If left unrecognized and untreated, patients are at a high risk of mortality. The most common class of medication that carries an increased risk of serotonin syndrome, when used in combination, is selective serotonin reuptake inhibitors (SSRIs); however, medications that increase serotonin production, increase serotonin release, inhibit serotonin metabolism and stimulate serotonin receptors can increase the possibility of serotonin syndrome. We report a case that details the presentation and treatment of a 25-year-old man who developed serotonin syndrome in the setting of rapid titration of risperidone, trazodone, and sertraline. The patient presented to the ED with acute agitation, diaphoresis, and altered mental status. He also had lower extremity myoclonus and was tremulous with an oral temperature of 100°F (37.8°C) and heart rate of 103 beats per minute. Serotonin syndrome was confirmed and the patient was treated successfully with benzodiazepines before being discharged from the hospital after 4 days. [ABSTRACT FROM AUTHOR]

Published
2024
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29. Efficacy and Safety of Trazodone and Gabapentin Fixed-Dose Combination in Patients Affected by Painful Diabetic Neuropathy: Randomized, Controlled, Dose-Finding Study

Author

Solomon Tesfaye, Ponnusamy Saravanan, Edvard Ehler, Karel Zinek, Ilona Palka-Kisielowska, Marcin Nastaj, Pierre Serusclat, Paola Lipone, Andrea Vergallo, Elisa Quarchioni, Fabrizio Calisti, Alessandro Comandini, and Agnese Cattaneo

Subjects
Trazodone, Painful diabetic neuropathy, Anesthesiology, RD78.3-87.3
Abstract

Abstract Introduction Up to 50% of diabetic patients with neuropathy suffer from chronic pain, namely painful diabetic neuropathy (PDN), an unmet medical need with significant impact on quality of life. Gabapentin is widely used for PDN, albeit with frequent dose-limiting effects. Trazodone, an antidepressant with multi-modal action, has shown promising results when given at low doses as an add-on to gabapentin. Upon previous clinical trials and experimental evidence, a fixed-dose combination (FDC) of both compounds, at low doses, was developed for neuropathic pain. Methods This was a phase II, randomized, double-blind, placebo and reference controlled, dose-finding, multicenter, international, prospective study. Male and female diabetic patients aged 18–75 years and affected by PDN were eligible for enrolment. Patients were randomized (1:1:1:1:2 ratio) to trazodone and gabapentin (Trazo/Gaba) 2.5/25 mg t.i.d. for 8 weeks, Trazo/Gaba 5/50 mg t.i.d. for 8 weeks, Trazo/Gaba 10/100 mg t.i.d. for 8 weeks, gabapentin (Gaba), or placebo (PLB). The aim of the study was to collect preliminary information on the effect of the 3 different FDCs of Trazo/Gaba on pain intensity based on the 11-point numeric rating score (NRS) after 8 weeks of treatment. The secondary objectives were the evaluation of the percentage of responders, neuropathic pain symptoms, anxiety, sleep, quality of life, safety, and tolerability. The primary efficacy endpoint was evaluated with last observation carried out forward (LOCF), using an analysis of covariance (ANCOVA), including treatment and centers as factors and baseline as covariate and applying linear contrast test, excluding the active treatment. Only if the linear contrast test was significant (p 0.05) among treatment groups. Consequently, the minimum effective dose against PLB was not determined. The multiple comparison with Dunnett adjustment did not show any statistically significant differences vs. PLB after 8 weeks of treatment: Trazo/Gaba 2.5/25 mg (95% confidence interval (CI) − 1.2739, 0.2026; p = 0.1539); Trazo/Gaba 5/50 mg (95% CI − 0.9401, 0.5390; p = 0.5931); Trazo/Gaba 10/100 mg (95% CI − 1.0342, 0.4582; p = 0.4471). However, patients receiving the lowest dose of Trazo/Gaba 2.5/25 mg showed a statistically significant difference to PLB after 6 weeks of treatment (95% CI − 1.6648, − 0.2126; p = 0.0116). Positive results were also found for responder patients, other items related to the pain, anxiety, depression, sleep, and quality of life, consistently in favor to the lowest Trazo/Gaba FDC. Two serious adverse events (SAEs) occurred but were judged unrelated to the study treatment. Treatment-emergent adverse events (TEAEs) were mainly mild-to-moderate in intensity and involved primarily nervous system, gastrointestinal disorders, and investigations. Conclusions The primary end point of the study was the change from baseline of the average daily pain score based on the 11-point NRS after 8 weeks of treatment. While the primary endpoint was not reached, patients treated with Trazo/Gaba 2.5/25 mg t.i.d. showed statistically significant improvement of pain and other scores after 6 weeks and reported consistent better results in comparison to PLB on primary and secondary endpoints for the overall study duration. According to these results, the lowest dose of Trazo/Gaba FDC may be the best candidate for further clinical development to confirm the potential benefits of the FDC drug for this condition. Clinical Trial Registration NCT03749642.

Published
2024
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30. Drugs associated with reversible cerebral vasoconstriction syndrome: A pharmacovigilance study in vigiBase ®.

Author

Favrelière, Sylvie, Mahé, Julien, Veyrac, Gwenaelle, Neau, Jean Philippe, Lafay-Chebassier, Claire, and Pérault-Pochat, Marie Christine

Subjects
*NASAL vasoconstrictors, *TRAZODONE, *MONOCLONAL antibodies, *MYCOPHENOLIC acid, *DRUG side effects
Abstract

Background: Data on drug-induced reversible cerebral vasoconstriction syndrome (RCVS) are scarce. We aimed to describe RCVS characteristics with drugs previously identified as associated with RCVS and investigate potential signals related to other drugs. Methods: VigiBase® was queried for all reports of RCVS until 31 May 2023. A descriptive study was performed on reports concerning drug classes known to precipitate RCVS. To identify new drugs, a disproportionality analysis was conducted. Results: In total, 560 reports were included. RCVS occurred in patients aged between 45–64 years (40%) and 18–44 years (35%), mainly in females (72.5%). Drugs were antidepressants (38.4%), triptans (6.4%), nasal decongestants (3.7%) and immunosupressants (8.7%). In 50 cases, antidepressants were in association with drugs known to precipitate RCVS. The median time to onset was 195 days for antidepressants and much shorter (1–10 days) for triptans, nasal decongestants and immunosuppressants. The outcome was favorable in 87% of cases, and fatal in 4.4%. We found a disproportionality signal with 14 drugs: glucocorticoids, bupropion, varenicline, mycophenolic acid, aripiprazole, trazodone, monoclonal antibodies (erenumab, ustekinumab and tocilizumab), leuprorelin and anastrozole. Conclusions: The present study confirms the role of vasoconstrictors in the onset of RCVS, particularly when used in combination and found potential signals, which may help clinicians envisage an iatrogenic etiology of RCVS. [ABSTRACT FROM AUTHOR]

Published
2024
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31. Efficacy and Safety of Trazodone and Gabapentin Fixed-Dose Combination in Patients Affected by Painful Diabetic Neuropathy: Randomized, Controlled, Dose-Finding Study.

Author

Tesfaye, Solomon, Saravanan, Ponnusamy, Ehler, Edvard, Zinek, Karel, Palka-Kisielowska, Ilona, Nastaj, Marcin, Serusclat, Pierre, Lipone, Paola, Vergallo, Andrea, Quarchioni, Elisa, Calisti, Fabrizio, Comandini, Alessandro, and Cattaneo, Agnese

Subjects
*DIABETIC neuropathies, *TRAZODONE, *TREATMENT effectiveness, *POSTHERPETIC neuralgia, *PATIENTS, *HEALTH facilities, *ANALGESIA
Abstract

Introduction: Up to 50% of diabetic patients with neuropathy suffer from chronic pain, namely painful diabetic neuropathy (PDN), an unmet medical need with significant impact on quality of life. Gabapentin is widely used for PDN, albeit with frequent dose-limiting effects. Trazodone, an antidepressant with multi-modal action, has shown promising results when given at low doses as an add-on to gabapentin. Upon previous clinical trials and experimental evidence, a fixed-dose combination (FDC) of both compounds, at low doses, was developed for neuropathic pain. Methods: This was a phase II, randomized, double-blind, placebo and reference controlled, dose-finding, multicenter, international, prospective study. Male and female diabetic patients aged 18–75 years and affected by PDN were eligible for enrolment. Patients were randomized (1:1:1:1:2 ratio) to trazodone and gabapentin (Trazo/Gaba) 2.5/25 mg t.i.d. for 8 weeks, Trazo/Gaba 5/50 mg t.i.d. for 8 weeks, Trazo/Gaba 10/100 mg t.i.d. for 8 weeks, gabapentin (Gaba), or placebo (PLB). The aim of the study was to collect preliminary information on the effect of the 3 different FDCs of Trazo/Gaba on pain intensity based on the 11-point numeric rating score (NRS) after 8 weeks of treatment. The secondary objectives were the evaluation of the percentage of responders, neuropathic pain symptoms, anxiety, sleep, quality of life, safety, and tolerability. The primary efficacy endpoint was evaluated with last observation carried out forward (LOCF), using an analysis of covariance (ANCOVA), including treatment and centers as factors and baseline as covariate and applying linear contrast test, excluding the active treatment. Only if the linear contrast test was significant (p < 0.05), the step-down Dunnett test would be used to determine the minimum effective dose significantly different from PLB. If linearity was not verified, an adjusted ANCOVA model and comparisons with Dunnett test were performed. Before the application of the ANCOVA model, the non-significance of interaction treatment per baseline was verified. Results: A total of 240 patients were included in the modified intention-to-treat (m-ITT) population: 39 in Trazo/Gaba 2.5/25 mg, 38 in Trazo/Gaba 5/50 mg, 37 in Trazo/Gaba 10/100 mg, 83 in PLB, and 43 in Gaba. After 8 weeks of treatment, changes of the average daily pain score based on the 11-point NRS from baseline were − 2.52 ± 2.31 in Trazo/Gaba 2.5/25 mg group, − 2.24 ± 1.96 in Trazo/Gaba 5/50 mg group, − 2.46 ± 2.12 in Trazo/Gaba 10/100 mg group, − 1.92 ± 2.21 in Gaba group, and − 2.02 ± 1.95 in the PLB group. The linear contrast test did not result in significant differences (p > 0.05) among treatment groups. Consequently, the minimum effective dose against PLB was not determined. The multiple comparison with Dunnett adjustment did not show any statistically significant differences vs. PLB after 8 weeks of treatment: Trazo/Gaba 2.5/25 mg (95% confidence interval (CI) − 1.2739, 0.2026; p = 0.1539); Trazo/Gaba 5/50 mg (95% CI − 0.9401, 0.5390; p = 0.5931); Trazo/Gaba 10/100 mg (95% CI − 1.0342, 0.4582; p = 0.4471). However, patients receiving the lowest dose of Trazo/Gaba 2.5/25 mg showed a statistically significant difference to PLB after 6 weeks of treatment (95% CI − 1.6648, − 0.2126; p = 0.0116). Positive results were also found for responder patients, other items related to the pain, anxiety, depression, sleep, and quality of life, consistently in favor to the lowest Trazo/Gaba FDC. Two serious adverse events (SAEs) occurred but were judged unrelated to the study treatment. Treatment-emergent adverse events (TEAEs) were mainly mild-to-moderate in intensity and involved primarily nervous system, gastrointestinal disorders, and investigations. Conclusions: The primary end point of the study was the change from baseline of the average daily pain score based on the 11-point NRS after 8 weeks of treatment. While the primary endpoint was not reached, patients treated with Trazo/Gaba 2.5/25 mg t.i.d. showed statistically significant improvement of pain and other scores after 6 weeks and reported consistent better results in comparison to PLB on primary and secondary endpoints for the overall study duration. According to these results, the lowest dose of Trazo/Gaba FDC may be the best candidate for further clinical development to confirm the potential benefits of the FDC drug for this condition. Clinical Trial Registration: NCT03749642. [ABSTRACT FROM AUTHOR]

Published
2024
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32. Impact of trazodone once‐a‐day on quality of life and functional recovery in adults with major depressive disorder: A prospective, observational study.

Author

Tellone, Valeria, Markovic, Oto, Strashimirova, Milena, Sani, Gabriele, Lenderking, William R., Margolis, Mary Kay, Fallone, Raffaella, Quarchioni, Elisa, Cattaneo, Agnese, and Comandini, Alessandro

Subjects
*SEROTONIN uptake inhibitors, *MENTAL depression, *SLEEP interruptions, *COGNITION disorders, *QUALITY of life, *DULOXETINE
Abstract

Background: Health‐related quality of life (HRQL) is an important goal for patients with major depressive disorder (MDD), but whether antidepressants improve HRQL in these patients is unclear. Here, we describe the real‐world effects of trazodone once‐a‐day (TzOAD) and selective serotonin reuptake inhibitor (SSRI) treatments on HRQL and functioning in adults with MDD. Methods: This 8‐week prospective, observational, open‐label, multicenter study was conducted in adults with moderate or severe MDD for whom TzOAD or SSRI were prescribed as monotherapy. The primary outcome was life enjoyment and satisfaction assessed via the patient‐reported Quality‐of‐Life Enjoyment and Satisfaction Questionnaire Short Form (Q‐LES‐Q‐SF) from baseline to week 8. Secondary outcomes included change in Q‐LES‐Q‐SF from baseline to weeks 1 and 2; severity of depressive symptoms using the Montgomery Åsberg Depression Rating Scale (MADRS) and sleep disturbance via the PROMIS SF‐SD 8b questionnaire at weeks 1, 2, and 8; and overall functioning via the Sheehan Disability Scale (SDS), hedonic capacity using the Snaith–Hamilton Pleasure Scale (SHAPS), and cognitive dysfunction using the Perceived Deficits Questionnaire (PDQ‐5) at baseline and week 8. Results: The study included 208 adults with MDD (mean [SD] age = 50.2 [14.3] years; 68.6% female; 98.4% White). Life enjoyment and satisfaction improved from baseline to week 8 for both treatment groups: Q‐LES‐Q‐SF mean (SD) scores were 27.5 (20.4) for the SSRI group and 39.0 (22.1) for the TzOAD group. Depressive symptoms and sleep disturbances also reduced from baseline to week 8: MADRS (SSRI, −15.7 [8.3]; TzOAD, −21.0 [9.8]); PROMIS SF‐SD 8b (SSRI, −9.9 [12.6]; TzOAD, −22.0 [12.6]). Mean change scores in Q‐LES‐Q‐SF, MADRS, and PROMIS SF‐SD 8b improved as early as week 1 in both groups. Mean scores also improved from baseline to week 8 on SDS (SSRI, −9.2 [7.4]; TzOAD, −14.3 [7.5]), SHAPS (SSRI, −6.6 [4.3]; TzOAD, −8.3 [4.4]), and PDQ‐5 (SSRI, −5.8 [4.5]; TzOAD, −7.7 [5.0]). Conclusions: In adults with MDD who received TzOAD or SSRIs, overall and individual HQRL domains improved rapidly and in parallel with improvements in depressive symptoms, with a slightly greater improvement observed in the TzOAD group. [ABSTRACT FROM AUTHOR]

Published
2024
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33. Rethinking the role of trazodone in the different depressive dimensions.

Author

Berardelli, Isabella, Amerio, Andrea, Bartoli, Francesco, Cuomo, Alessandro, Deste, Giacomo, Orsolini, Laura, Sampogna, Gaia, and Pompili, Maurizio

Abstract

The efficacy of trazodone for several psychopathologic dimensions of depression has been shown in the literature. Trazodone has been widely used in some clinical contexts (e.g. for insomnia and depression in the elderly). However, the role of trazodone in several aspects of depression is not well known. Eight experts from academic and medical centers across Italy met to identify the difficulties and barriers faced in daily clinical practice in the assessment and management of major depressive disorder and how the use of trazodone could address some unmet needs. The objective of the expert meetings and the present document was to increase knowledge of particular areas of treatment with trazodone. Evidence of the role of trazodone in patients affected by major depressive disorder with anxiety symptoms, insomnia, agitation, cognitive deficits, alcohol use disorders, physical comorbidities, and suicide risk has been identified, showing the effectiveness of trazodone in different presentations of major depressive disorder. The main characteristics of patients with depression for whom trazodone seems to be most effective have been identified, providing clinicians with information on possible uses of this drug in such population of patients. [ABSTRACT FROM AUTHOR]

Published
2024
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34. CURRENT ASPECTS ON THE USE OF TRAZODONE IN VARIOUS FIELDS, INCLUDING DENTAL MANAGEMENT.

Author

CRICLEVIT, Dragoş

Subjects
EFFECT of stress on animals, TRAZODONE, ORAL drug administration, PHYSIOLOGICAL stress, VETERINARY medicine
Abstract

Trazodone is the main anxiolytic used in veterinary medicine because it significantly reduces physiological stress in cats and dogs. In this case, the animals are prone to illness due to the body's decreased immunity. Four drugs from four different classes can be used to relieve acute situational fear and anxiety in dogs and cats: trazodone, gabapentin, alprazolam and oral dexmedetomidine. Of all of these, trazodone is the first choice for both veterinarians and humans, and the commonly chosen commercial product is Trittico. It is worth noting that trazodone can be administered both per os and intravenously. The oral route of administration has been chosen because side effects are rarer.,and the acceptable absolute bioavailability was 84.6%. Dosages were used according to behavioral or medical conditions. In anxiety the dose in dogs is: 1-16 mg/kg q24h for single daily medication or 1-19 mg/kg q24h in combination with other drugs, and in single administration the dose is between 2-14 mg/kg q24h. In behavioral stress in dogs the dose is 3.7 mg/kg alone/combined with NSAIDs, tramadol or other drugs. For sedation, the dose is 3.5 mg/kg q 12-24h.In cats no dose studies are reported. Only in case of accidental stress the dose of 7-15 mg/kg q 24h for 1-1,5h is mentioned.In behavioral stress in dogs the dose is 3.7 mg/kg alone/combined with NSAIDs, tramadol or other drugs. For sedation the dose is 3.5 mg/kg every 12-24h. In cats no studies on the dose administered are reported. In dogs in preoperative administration the dose is between 5-7 mg/kg combined with an opioid (Tramadol, Bupaq/Alvegesic). Postoperatively give 1-3 mg/kg in combination with tramadol for 3 days. Trazodone has a much higher risk of adverse reactions in geriatric patients including: callus, vomiting, colitis, sedation, sedation, increased appetite, paradoxical excitement and panting, hypersalivation and behavioral disinhibition in dogs, and hypersalivation, paradoxical excitement, ataxia, vomiting, diarrhea, callus in cats. [ABSTRACT FROM AUTHOR]

Published
2024

35. Treatment strategies for insomnia in Japanese primary care physicians' practice: A Web-based questionnaire survey.

Author

Takeshima, Masahiro, Sakurai, Hitoshi, Inada, Ken, Aoki, Yumi, Ie, Kenya, Kise, Morito, Yoshida, Eriko, Matsui, Kentaro, Utsumi, Tomohiro, Shimura, Akiyoshi, Okajima, Isa, Kotorii, Nozomu, Yamashita, Hidehisa, Suzuki, Masahiro, Kuriyama, Kenichi, Shimizu, Eiji, Mishima, Kazuo, Watanabe, Koichiro, and Takaesu, Yoshikazu

Subjects
*INSOMNIA treatment, *BENZODIAZEPINES, *PSYCHOTHERAPY, *SCALE analysis (Psychology), *CROSS-sectional method, *CHINESE medicine, *FAMILY medicine, *SEDATIVES, *RESEARCH funding, *DRUG therapy, *QUESTIONNAIRES, *TRANQUILIZING drugs, *DESCRIPTIVE statistics, *PROFESSIONS, *PHYSICIAN practice patterns, *GENERIC drug substitution, *COGNITIVE therapy, *COMPARATIVE studies, *DATA analysis software, *CONFIDENCE intervals, *TRAZODONE, *DRUG utilization, *RELAXATION techniques, *QUETIAPINE, *SLEEP hygiene
Abstract

Background: It is unclear how primary care physicians manage insomnia after the introduction of novel hypnotics such as orexin receptor antagonists and melatonin receptor agonists. This Web-based questionnaire survey aimed to examine treatment strategies for insomnia in Japanese primary care practice. Methods: One-hundred-and-seventeen primary care physicians were surveyed on the familiarity of each management option for insomnia on a binary response scale (0 = "unfamiliar"; 1 = "familiar") and how they managed insomnia using a nine-point Likert scale (1 = "I never prescribe/perform it"; 9 = "I often prescribe/perform it"). Physicians who were unfamiliar with a management option were deemed to have never prescribed or performed it. Results: Regarding medication, most physicians were familiar with novel hypnotics. Suvorexant was the most used hypnotic, followed by lemborexant and ramelteon. These novel hypnotics averaged 4.8–5.4 points and 4.0–4.7 points for sleep onset and sleep maintenance insomnia, respectively. By contrast, most benzodiazepines were seldom used below two points. Regarding psychotherapy, only approximately 40% of the physicians were familiar with cognitive behavioral therapy for insomnia (CBT-I) and they rarely implemented it, at an average of 1.5–1.6 points. More physicians were familiar with single-component psychotherapies (i.e., relaxation, sleep restriction therapy, and stimulus control) compared to CBT-I, and 48–74% of them implemented it slightly more often, with scores ranging from 2.6 to 3.4 points. Conclusion: This study suggests that Japanese primary care physicians seldom use CBT-I to treat insomnia. In addition, they use novel sleep medications more frequently than benzodiazepines in terms of pharmacotherapy. The use and availability of CBT-I in Japanese primary care might be facilitated by: educating primary care physicians, implementing brief or digital CBT-I, and/or developing collaborations between primary care physicians and CBT-I specialists. [ABSTRACT FROM AUTHOR]

Published
2024
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36. Statistical Design Approach for Optimizing the Spectrofluorimetric Method for Quantifying Trazodone Hydrochloride.

Author

Rahman, Nafisur, Sameen, Shahroora, Kashif, Mohammad, and Nasir, Mohd

Subjects
*TRAZODONE, *EXPERIMENTAL design, *RESPONSE surfaces (Statistics), *BUFFER solutions, *ION pairs, *FLUORESCENCE yield
Abstract

A sensitive spectrofluorimetric method was developed to determine trazodone hydrochloride in its formulation and urine sample. The principle of the developed method is based on the formation of an ion pair complex at a pH of 4.27 between the analyte drug and eosin Y, followed by its extraction into dichloromethane and subsequent fluorescence measurement. The fluorescence of the extracted trazodone-eosin Y complex was recorded at 450 nm with an excitation wavelength of 350 nm. Recording the fluorescence was utilized to construct the calibration plot, which was found to be linear in the range of 32.0–1.50 × 103 ng/mL of trazodone hydrochloride. The influences of experimental variables, namely pH, volumes of eosin Y (2.90 × 10–3 M), and buffer solution (pH 4.27), on the fluorescence intensity were examined and optimized by response surface methodology via Box−Behnken design. The limits of detection and the limit of quantitation of the reported method are 9.50 and 28.79 ng/mL, respectively. The accuracy of the proposed method was evaluated for intra-day and inter-day precision in the range of 0.46 to 0.77% RSD. The content of trazodone hydrochloride in its dosage forms was determined by the developed method using the standard addition technique, and the results showed good recovery between 96.50 and 99.25%, with a standard analytical error of 1.54 × 10–5 to 2.86 × 10–4. Interval hypothesis testing confirmed that it is lower than ±2%; hence, there was no bias between the developed and reference methods. No interference was observed from the common excipients present in tablet formulations. The developed method was also successfully applied for the determination of trazodone in urine samples, and recovery of the drug was observed in the range of 90–98%. [ABSTRACT FROM AUTHOR]

Published
2024
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37. Sage (Salvia officinalis) alleviates trazadone induced rat cardiotoxicity mediated via modulation of autophagy and oxidative stress.

Author

Al-Gholam, Marwa Abdel-Samad, Rasheed Hathout, Heba Moustafa, Safwat, Marwa Mohamed, and Essawy, Asmaa Saeed

Subjects
*SAGE, *OXIDATIVE stress, *DOXORUBICIN, *ASPARTATE aminotransferase, *OXIDANT status, *CARDIOTOXICITY, *AUTOPHAGY, *DNA damage
Abstract

The antidepressant drug trazodone (TRZ) is commonly used for treating depression, anxiety, and insomnia, however, it causes cardiotoxicity, which is one of its limitations. The objective of this work was to investigate the impact of sage (Salvia officinalis) in rats against cardiotoxicity induced by TRZ and to investigate the mechanisms involved in its cardio-protective properties through autophagy and oxidative stress. Fifty male albino rats were split randomly into five experimental groups: control group, sage oil group (100 mg/kg), TRZ group (20 mg/kg), protective group, and curative group. Cardiac function biomarkers (aspartate aminotransferase [AST], creatine kinase-MB [CK-MB], and cardiac troponin T [cTnI]) were assessed in serum. Oxidative stress and inflammatory biomarkers in cardiac tissue (total antioxidant capacity, malondialdehyde, and tumor necrosis factor-α) were evaluated. Heart tissues were subjected to histological, immunohistochemical, and ultrastructural evaluations. DNA damage also evaluated. Significant rise in the levels of AST, CK-MB, and cTnI were observed with enhanced autophagy along with marked histopathological changes in the form of interrupted muscle fibers with wide interstitial spaces with areas of hemorrhage and extravasated blood and interstitial mononuclear cellular infiltration in TRZ group. DNA damage was also significantly increased in TRZ group. However, administration of sage in both protective and curative groups show marked improvement of the cardiac alterations. In conclusion, sage ameliorated the alterations in the heart induced by trazadone through modulation of autophagy and oxidative stress. [ABSTRACT FROM AUTHOR]

Published
2024
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38. The Use of Trazodone for Insomnia and Other Sleep Disturbances.

Author

Mills, Jeremy

Subjects
*PSYCHOTHERAPY, *OFF-label use (Drugs), *BENZODIAZEPINES, *INSOMNIA, *PRIAPISM, *SEROTONIN uptake inhibitors, *TRANQUILIZING drugs, *PHYSICIAN practice patterns, *TRAZODONE, *DRUG prescribing, *PSYCHOPHARMACOLOGY, *SLEEP disorders, *BEHAVIOR therapy, *ACCIDENTAL falls
Abstract

The article offers information on the use of trazodone for insomnia and other sleep disturbances, highlighting its common prescription despite being an off-label use. Topics include the challenges of non-pharmacological options like cognitive behavioral therapy for insomnia (CBT-I) in rural areas, the limitations of sleep hygiene education, and the need for immediate sleep solutions in some cases.

Published
2024
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39. Dissolving microneedles loaded with nimodipine for prevention of sleep disorders at a high altitude.

Author

Wang, Chunqing, Huang, Xin, Tang, Ziyan, Zhang, Yizhi, Wei, Meng, Du, Shumin, Song, Xingshuang, Wu, Yanping, Chi, Qiang, Zhuang, Xiaomei, Lina, Du, and Jin, Yiguang

Subjects
SLEEP disorders, CALCIUM ions, NIMODIPINE, SLEEP quality, ALTITUDES, CALCIUM antagonists, TRAZODONE
Abstract

Sleep disorders are one of the most common acute reactions on the plateau, which can cause serious complications. However, there is no effective and safe treatment currently available. Nimodipine (NMD) is a dihydropyridine calcium channel blocker with neuroprotective and vasodilating activity, mainly used for the treatment of ischemic brain injury. Commercial oral or injectable NMD formulations are not a good option for central neuron diseases due to their poor brain delivery. In this study, nimodipine dissolving microneedles (NDMNs) were prepared for the prevention of sleep disorders caused by hypoxia. NDMNs were composed of NMD and polyvinyl pyrrolidone (PVP) K90 with a conical morphology and high rigidity. After administration of NDMNs on the back neck of mice, the concentration of NMD in the brain was significantly higher than that of oral medication as was confirmed by the fluorescent imaging on mouse models. NDMNs enhanced cognitive function, alleviated oxidative stress, and improved the sleep quality of mice with high-altitude sleep disorders. The blockage of calcium ion overloading may be an important modulation mechanism. NDMNs are a promising and user-friendly formulation for the prevention of high-altitude sleep disorders. [ABSTRACT FROM AUTHOR]

Published
2024
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40. A green micelle‐enhanced first derivative synchronous fluorescence approach for determination of donepezil HCl and trazodone HCl in their pure state, pharmaceutical dosage form and spiked human plasma.

Author

Abd El wahab, Mennah M., Saad, Samar, Sheribah, Zeinab A., and El‐Enany, Nahed

Abstract

The study's objective is to establish an eco‐friendly, sensitive and economical quantitative methodology for the concurrent analysis of donepezil HCl (DPZ) and trazodone HCl (TRZ) in raw materials, tablets and human plasma. The first derivative synchronous fluorescence spectroscopic (FDSFS) technique was applied at constant wavelength difference (∆λ = 120) for assessment of DPZ and TRZ at each other's zero‐crossing point at 279 nm and 297 nm, respectively. The submitted technique was validated in accordance with ICH Q2 R1 guidelines and the linearity of the standard calibration curve was observed over the concentration range of 10–500 ng/ml for DPZ and 20–1,000 ng/ml for TRZ. The detection limits (LOD) were found to be 2.65 and 5.4 ng/ml, and the limits of quantitation (LOQ) were 8.05 and 16.3 ng/ml for DPZ and TRZ, respectively. This technique was used further to quantify the studied medications in their laboratory‐prepared mixtures, commercial tablets and spiked plasma samples. The results obtained were not significantly different from those acquired from the comparison methods, indicating the high accuracy and precision of the proposed method. Furthermore, the ecological friendliness of the suggested method was evaluated and proven to be excellent using Green Analytical Procedure Index (GAPI) and Analytical GREEnness (AGREE) evaluation tools. [ABSTRACT FROM AUTHOR]

Published
2024
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44. Miscellaneous Psychotropic Drugs

Author

Masson, Sylvia, Bleuer-Elsner, Stéphane, Muller, Gérard, Médam, Tiphaine, Chevallier, Jasmine, Gaultier, Emmanuel, Masson, Sylvia, Bleuer-Elsner, Stéphane, Muller, Gérard, Medam, Tiphaine, Chevallier, Jasmine, and Gaultier, Emmanuel

Published
2024
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45. Treating depression in patients with borderline personality disorder: clinical clues on the use of antidepressants

Author

Carmine Tomasetti, G. Autullo, A. Ballerini, A. de Bartolomeis, B. Dell’Osso, A. Fiorentini, F. Tonioni, V. Villari, and D. De Berardis

Subjects
Serotonin antagonist/Reuptake inhibitors, Comorbidity, Psychiatric disorders, Trazodone, Neurobiology, Emotion, Psychiatry, RC435-571
Abstract

Abstract Personality disorders (PD) are described as enduring patterns of markedly deviant and pervasive inner experiences and behaviors, with onset in adolescence, which lead to severe distress or impairment. Patients suffering from major depressive disorder (MDD) display higher rates of comorbidity with personality disorders, often complicating the treatment, and worsening the outcomes. Borderline personality disorder (BPD) is the most common of PD and is frequently associated with MDD, with which shares several features. The most part of research agrees on the fact that comorbid BPD in MDD patients quite doubles the poor response to treatments. Moreover, no treatment strategy stands out currently to emerge as more effective in these cases, thus urging the call for the need of new approaches. Herein, we revise the current literature on BPD, its neurobiology and comorbidity with MDD, as well as the more recent treatment strategies used. Then, based on its pharmacology, we propose a possible role of trazodone as a valuable tool to approach comorbid BPD-MDD.

Published
2024
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46. Should Trazodone Be First-Line Therapy for Insomnia? A Clinical Suitability Appraisal

Author

Pelayo, Rafael, Bertisch, Suzanne M, Morin, Charles M, Winkelman, John W, Zee, Phyllis C, and Krystal, Andrew D

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Sleep Research, insomnia, trazodone, clinical appraisal, literature review, Biomedical and clinical sciences
Abstract

Trazodone is one of the most commonly used prescription medications for insomnia; however, some recent clinical guidelines do not recommend its use for treating insomnia. This clinical appraisal critically reviews the scientific literature on trazodone as a first-line treatment for insomnia, with the focus statement "Trazodone should never be used as a first-line medication for insomnia." In addition, field surveys were sent to practicing physicians, psychiatrists, and sleep specialists to assess general support for this statement. Subsequently, a meeting with a seven-member panel of key opinion leaders was held to discuss published evidence in support and against the statement. This paper reports on the evidence review, the panel discussion, and the panel's and healthcare professionals' ratings of the statement's acceptability. While the majority of field survey responders disagreed with the statement, the majority of panel members agreed with the statement based on the limited published evidence supporting trazodone as a first-line agent as they understood the term "first-line agent".

Published
2023

47. Trazodone affects periodic leg movements and chin muscle tone during sleep less than selective serotonin reuptake inhibitor antidepressants in children.

Author

DelRosso, Lourdes, Mogavero, Maria, Bruni, Oliviero, Schenck, Carlos, Fickenscher, Amy, and Ferri, Raffaele

Subjects
REM sleep without atonia, SSRI antidepressants, atonia index, children, chin EMG tone, leg movement activity during sleep, periodic leg movements during sleep, trazodone, Male, Female, Child, Humans, Selective Serotonin Reuptake Inhibitors, Trazodone, Muscle Tonus, Polysomnography, Chin, Leg, Antidepressive Agents, Sleep, Muscle Hypertonia, Muscle Hypotonia
Abstract

STUDY OBJECTIVES: To test the hypothesis that children taking trazodone have less leg movements during sleep (LMS) and higher rapid eye movement (REM) sleep atonia than children taking selective serotonin reuptake inhibitors (SSRIs) but more than normal controls. METHODS: Fifteen children (9 girls and 6 boys, mean age 11.7 years, standard deviation [SD] 3.42) taking trazodone (median dosage 50 mg/d, range 25-200 mg) for insomnia and 19 children (11 girls and 8 boys, mean age 13.7 years, SD 3.07) taking SSRIs for depression, anxiety, or both were consecutively recruited, as well as an age- and sex-matched group of 25 control children (17 girls and 8 boys, mean age 13.7 years, SD 3.11). LMS were scored and a series of parameters was calculated, along with the analysis of their time structure. The Atonia Index was then computed for each non-REM sleep stage and for REM sleep. RESULTS: Children taking trazodone exhibited slightly higher leg movement indices than controls but lower than those found in children taking SSRIs and their time structure was different. Chin electromyogram atonia in all sleep stages was not significantly altered in children taking trazodone but was decreased in children taking SSRIs, especially during non-REM sleep. CONCLUSIONS: In children, SSRIs but not trazodone are associated with a significantly increased number of LMS, including periodic LMS, and increased chin tone in all sleep stages. The assessment of periodic limb movement disorder and REM sleep without atonia might not be accurate when children are taking SSRIs because of their significant impact. CITATION: DelRosso LM, Mogavero MP, Bruni O, Schenck CH, Fickenscher A, Ferri R. Trazodone affects periodic leg movements and chin muscle tone during sleep less than selective serotonin reuptake inhibitor antidepressants in children. J Clin Sleep Med. 2022;18(12):2829-2836.

Published
2022

48. Treating depression in patients with borderline personality disorder: clinical clues on the use of antidepressants.

Author

Tomasetti, Carmine, Autullo, G., Ballerini, A., de Bartolomeis, A., Dell'Osso, B., Fiorentini, A., Tonioni, F., Villari, V., and De Berardis, D.

Subjects
*PSYCHOTHERAPY patients, *SEROTONIN uptake inhibitors, *EMOTIONS, *TREATMENT effectiveness, *BORDERLINE personality disorder, *ANTIDEPRESSANTS, *NEUROBIOLOGY, *TRAZODONE, *MENTAL depression, *PSYCHOSOCIAL factors, *COMORBIDITY
Abstract

Personality disorders (PD) are described as enduring patterns of markedly deviant and pervasive inner experiences and behaviors, with onset in adolescence, which lead to severe distress or impairment. Patients suffering from major depressive disorder (MDD) display higher rates of comorbidity with personality disorders, often complicating the treatment, and worsening the outcomes. Borderline personality disorder (BPD) is the most common of PD and is frequently associated with MDD, with which shares several features. The most part of research agrees on the fact that comorbid BPD in MDD patients quite doubles the poor response to treatments. Moreover, no treatment strategy stands out currently to emerge as more effective in these cases, thus urging the call for the need of new approaches. Herein, we revise the current literature on BPD, its neurobiology and comorbidity with MDD, as well as the more recent treatment strategies used. Then, based on its pharmacology, we propose a possible role of trazodone as a valuable tool to approach comorbid BPD-MDD. [ABSTRACT FROM AUTHOR]

Published
2024
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49. Cannabidiol Exerts Sedative and Hypnotic Effects in Normal and Insomnia Model Mice Through Activation of 5-HT1A Receptor.

Author

Liu, Yu-Meng, Li, Jin-Cao, Gu, Yong-Fang, Qiu, Ren-Hong, Huang, Jia-Ying, Xue, Rui, Li, Shuo, Zhang, Yang, Zhang, Kuo, and Zhang, You-Zhi

Subjects
*SLEEP latency, *SLEEP duration, *CANNABIDIOL, *CANNABIS (Genus), *INSOMNIA, *TRAZODONE
Abstract

Cannabis sativa has been used for improving sleep for long history. Cannabidiol (CBD) has drown much attention as a non-addictive psychoactive component in Cannabis sativa extract. However, the effects of CBD on sleep architecture and it's acting mechanism remains unclear. In the present study, we evaluated the sedative-hypnotic effect of cannabidiol (CBD), assessed the effects of CBD on sleep using a wireless physiological telemetry system. We further explored the therapeutic effects of CBD using 4-chloro-dl-phenylalanine (PCPA) induced insomnia model and changes in sleep latency, sleep duration and intestinal flora were evaluated. CBD shortened sleep latency and increases sleep duration in both normal and insomnia mice, and those effects were blocked by 5-HT1A receptor antagonist WAY100635. We determined that CBD increases 5-HT1A receptors expression and 5-HT content in the hypothalamus of PCPA-pretreated mice and affects tryptophan metabolism in the intestinal flora. These results showed that activation of 5-HT1A receptors is one of the potential mechanisms underlying the sedative-hypnotic effect of CBD. This study validated the effects of CBD on sleep and evaluated its potential therapeutic effects on insomnia. [ABSTRACT FROM AUTHOR]

Published
2024
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50. The screening and management of sleep disturbances in people living with HIV: Delphi consensus.

Author

Allavena, Clotilde, Bastides, Frédéric, Moroy, Anne, Occhipinti, Stéphanie, Durand, François, Barriere, Guillaume, Micoulaud‐Franchi, Jean‐Arthur, and Ghosn, Jade

Subjects
*DELPHI method, *HIV-positive persons, *SLEEP interruptions, *MEDICAL screening, *SLEEP duration, *SLEEP hygiene, *RESTLESS legs syndrome, *TRAZODONE
Abstract

Summary: Sleep disturbances in people living with HIV (PLHIV) are frequent but their management remains insufficient. In the absence of specific recommendations, a DELPHI consensus research project was conducted in France to establish best practice. A multidisciplinary Steering Committee (STC) undertook a literature review and used it with clinical expertise to create statements that were voted on. Two profiles of healthcare professionals with significant experience in monitoring PLHIV were selected for the voting: physicians and nurses/psychologists. Votes were collected electronically, independently, and anonymously. The STC created 27 statements covering six areas: Screening of sleep disturbances, Investigation, First‐line management, Referral to a specialist, Antiretroviral treatment (ARV), and Prevention. Two rounds of votes included 42 physicians and 32 nurses/psychologists. Consensus was reached for 24 out of 27 statements (89%) including: to assess quantity and quality of sleep among PLHIV at least annually, ideally using a common methodology within the medical department; to consider the temporary addition of a hypnotic treatment in cases of acute insomnia not improved by the rules of sleep hygiene, with full awareness of potential drug–drug interactions and risk of dependence; to correct ferritinaemia if <100 ng/mL before referral to a specialist when restless legs syndrome is suspected; to consider changing the time of ARV administration or an ARV switch within the same class when sleep disturbances are caused by an ARV. This DELPHI Consensus provides best practice for screening and managing sleep disturbances in PLHIV and optimising their quality of life. [ABSTRACT FROM AUTHOR]

Published
2024
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