Buspirone-associated Movement Disorder: A Literature Review

Rissardo, Jamir Pitton; Caprara, Ana Letícia Fornari

doi:10.14712/23362936.2020.1

Cited by 17 publications

(12 citation statements)

References 54 publications

(72 reference statements)

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“…When provided, we extracted author, department, year of publication, country of occurrence, number of patients affected, PGB indication, time from first PGB dose till MD onset, time from PGB withdrawal to symptom improvement, patient's status at follow-up, and important findings of clinical history and management. [ 11 12 13 ] Most of the cases did not report information about timeline events, neurological examination details, or electrodiagnostic studies. Data were extracted by two independent authors, double-checked to ensure matching, and organized by whether the MD was a side effect of the PGB use.…”

Section: Methodsmentioning

confidence: 99%

Pregabalin-associated movement disorders: A literature review

Rissardo

Caprara

2020

Brain Circ

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Central nervous system adverse effects are commonly reported with pregabalin (PGB). On the other hand, movement disorders (MDs) associated with this drug were rarely described. However, their occurrence could significantly affect the quality of life of PGB users. This literature review aims to evaluate the clinical epidemiological profile, pathological mechanisms, and management of PGB-associated MDs. Relevant reports in six databases were identified and assessed by two reviewers without language restriction. A total of 46 reports containing 305 cases from 17 countries were assessed. The MDs encountered were as follows: 184 individuals with ataxia, 61 with tremors, 39 with myoclonus, 8 with parkinsonism, 1 with restless legs syndrome, 1 with dystonia, 1 with dyskinesia, and 1 with akathisia. The mean age was 62 years (range: 23–94). The male sex was slightly predominant with 54.34%. The mean PGB dose when the MD occurred was 238 mg, and neuropathic pain was the most common indication of PGB. The time from PGB start to MD was < 1 month at 75%. The time from PGB withdrawal to recovery was < 1 week at 77%. All the individuals where the follow-up was reported had a full recovery. The most common management was PGB withdrawal. In the literature, the majority of the cases did not report information about timeline events, neurological examination details, or electrodiagnostic studies. The best management for all MDs is probably PGB withdrawal. If the patient is on dialysis program, perhaps an increased number of sessions will decrease recovery time. Furthermore, the addition of a benzodiazepine could accelerate recovery.

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Section: Methodsmentioning

confidence: 99%

Pregabalin-associated movement disorders: A literature review

Rissardo

Caprara

2020

Brain Circ

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“…Moreover, it was not as well-tolerated (nausea and dizziness) and less effective in those with past benzodiazepine use (22). A subsequent Cochrane review compared buspirone to placebo for PD and found buspirone to be less efficacious than placebo but the review was limited by the dearth of high-quality studies (23). Buspirone is generally dosed two to three times a day and has a gradual onset of action of around 10 days to 4 weeks.…”

Section: Current Treatments For Anxiety Disorders Serotonergic/norepinephrinergic Antidepressantsmentioning

confidence: 99%

Pharmacotherapy of Anxiety Disorders: Current and Emerging Treatment Options

et al. 2020

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Anxiety disorders are the most prevalent psychiatric disorders and a leading cause of disability. While there continues to be expansive research in posttraumatic stress disorder (PTSD), depression and schizophrenia, there is a relative dearth of novel medications under investigation for anxiety disorders. This review's first aim is to summarize current pharmacological treatments (both approved and off-label) for panic disorder (PD), generalized anxiety disorder (GAD), social anxiety disorder (SAD), and specific phobias (SP), including selective serotonin reuptake inhibitors (SSRIs), serotonin norepinephrine reuptake inhibitors (SNRIs), azapirones (e.g., buspirone), mixed antidepressants (e.g., mirtazapine), antipsychotics, antihistamines (e.g., hydroxyzine), alpha- and beta-adrenergic medications (e.g., propranolol, clonidine), and GABAergic medications (benzodiazepines, pregabalin, and gabapentin). Posttraumatic stress disorder and obsessive-compulsive disorder are excluded from this review. Second, we will review novel pharmacotherapeutic agents under investigation for the treatment of anxiety disorders in adults. The pathways and neurotransmitters reviewed include serotonergic agents, glutamate modulators, GABAergic medications, neuropeptides, neurosteroids, alpha- and beta-adrenergic agents, cannabinoids, and natural remedies. The outcome of the review reveals a lack of randomized double-blind placebo- controlled trials for anxiety disorders and few studies comparing novel treatments to existing anxiolytic agents. Although there are some recent randomized controlled trials for novel agents including neuropeptides, glutamatergic agents (such as ketamine and d-cycloserine), and cannabinoids (including cannabidiol) primarily in GAD or SAD, these trials have largely been negative, with only some promise for kava and PH94B (an inhaled neurosteroid). Overall, the progression of current and future psychopharmacology research in anxiety disorders suggests that there needs to be further expansion in research of these novel pathways and larger-scale studies of promising agents with positive results from smaller trials.

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“…These therapeutics are generally well tolerated with short-term adverse effects that include nausea, diarrhea, and constipation. However, more problematic adverse effects include sexual dysfunction ( Jing & Straw-Wilson, 2016 ), suicide ideation in pediatric patients ( Hammell et al, 2016 ), and serotonin syndrome ( Volpi-Abadie et al, 2013 ) with SSRIs and the development of buspirone induced movement disorders ( Rissardo & Caprara, 2020 ). While the utilization of THC in anxiolytic therapies is limited due to psychoactive sequelae, risk of abuse, and anxiogenic effects ( Kayser et al, 2020b ; García-Gutiérrez et al, 2020 ), CBD continues to draw increasing attention in its use as an anxiolytic as work continues in developing therapeutics that can mimic the beneficial effects of current first line anxiety therapeutics while having improved side effect profiles over SSRIs and buspirone.…”

Section: Cannabinoid Involvement In Central Nervous System Diseases A...mentioning

confidence: 99%

Medicinal Cannabis and Central Nervous System Disorders

2022

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Cannabinoids, including those found in cannabis, have shown promise as potential therapeutics for numerous health issues, including pathological pain and diseases that produce an impact on neurological processing and function. Thus, cannabis use for medicinal purposes has become accepted by a growing majority. However, clinical trials yielding satisfactory endpoints and unequivocal proof that medicinal cannabis should be considered a frontline therapeutic for most examined central nervous system indications remains largely elusive. Although cannabis contains over 100 + compounds, most preclinical and clinical research with well-controlled dosing and delivery methods utilize the various formulations of Δ9-tetrahydrocannabinol (THC) and cannabidiol (CBD), the two most abundant compounds in cannabis. These controlled dosing and delivery methods are in stark contrast to most clinical studies using whole plant cannabis products, as few clinical studies using whole plant cannabis profile the exact composition, including percentages of all compounds present within the studied product. This review will examine both preclinical and clinical evidence that supports or refutes the therapeutic utility of medicinal cannabis for the treatment of pathological pain, neurodegeneration, substance use disorders, as well as anxiety-related disorders. We will predominately focus on purified THC and CBD, as well as other compounds isolated from cannabis for the aforementioned reasons but will also include discussion over those studies where whole plant cannabis has been used. In this review we also consider the current challenges associated with the advancement of medicinal cannabis and its derived potential therapeutics into clinical applications.

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Buspirone-associated Movement Disorder: A Literature Review

Cited by 17 publications

References 54 publications

Pregabalin-associated movement disorders: A literature review

Pregabalin-associated movement disorders: A literature review

Pharmacotherapy of Anxiety Disorders: Current and Emerging Treatment Options

Medicinal Cannabis and Central Nervous System Disorders

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