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2. A complex psychosocial portrait of substance use disorders among Indigenous people in the United States: A scoping review.

Author

Edinoff, Amber N., Maudrie, Tara L., Chiwiwi, Carly, Kjerland, Tonya M., Contreras, Liz, and Gone, Joseph P.

Subjects
*NATIVE Americans, *ALCOHOLISM, *ALASKA Natives, *HISTORICAL trauma, *PSYCHOSOCIAL factors
Abstract

Background and Objectives: There has been a prevailing but erroneous belief in the medical community that there is a biological vulnerability in the American Indian/Alaskan Native (AI/AN) community to substance use disorders (SUDs), with alcohol use disorder (AUD) being the most prevalent. This scoping review aimed to examine what possible psychosocial issues could lead to the development of the perpetuation of SUDs in the AI/AN population. Methods: The protocol for this scoping review followed Arksey and O'Malley's methodological framework. There were 405 articles included for full‐text review. Further inclusion criteria were applied which included: Directly looking at participants who had a SUD, including either in the discussion or conclusion a statement linking their data to psychosocial issues as a possible explanation for their data, and having measured the psychosocial issue with a research device. The final review included 15 studies. Results: Four psychosocial themes were uncovered using an inductive process, where recurring words related to identity, prejudice, isolation, discrimination, and self‐concept in the literature. These themes were trauma/historical loss, mood, and discrimination/self‐esteem. All of these themes are interrelated, and all influence the development or sustainment of a SUD. Discussion and Conclusions: Complex psychosocial factors in the AI/AN community are associated with SUDs. This trauma and historical loss should be addressed with culturally tailored treatments. Scientific Significance: There are not many manuscripts that specifically look at the interplay of mood, trauma, self‐worth, and discrimination with SUD in the AI/AN community. This scoping review aims to highlight these issues as well as discuss how culture should play a part in treatment. Answer questions and earn CME credit [ABSTRACT FROM AUTHOR]

Published
2024
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4. Xylazine: A Drug Adulterant of Clinical Concern.

Author

Edinoff, Amber N., Sall, Saveen, Upshaw, William C., Spillers, Noah J., Vincik, LeighAnn Y., De Witt, Adalyn S., Murnane, Kevin S., Kaye, Adam M., and Kaye, Alan D.

Abstract

Purpose of Review: The opioid epidemic has been responsible for significant morbidity and mortality in the USA and worldwide. As a result, it is essential to recognize the threat these potent drugs can cause when illicitly used. Specifically, introducing fentanyl as a drug adulterant has been shown to impact overdose rates drastically. In this regard, the Drug Enforcement Agency recently released a public safety alert announcing the new threat of a new adulterant called xylazine. Xylazine is a powerful animal sedative with a different mechanism of action when compared to illicit opioids such as heroin and fentanyl. Xylazine is typically injected intravenously via a syringe, often in combination with multiple other drugs. One of the most common drugs, xylazine, is taken in combination with fentanyl, with users of this drug combination describing xylazine as prolonging the euphoric sensation produced by fentanyl. Recent Findings: Xylazine may cause adverse effects such as bradycardia, brief hypertension followed by hypotension, premature ventricular contractions, ataxia, slurred speech, sedation, and respiratory depression. Much of the recent literature on xylazine use in humans comes from case reports and review articles. Summary: Related to widespread use in veterinary medicine and increasing circulation in illicit drug markets, there is a critical need for public awareness and additional clinical-based studies to further increase understanding of mediated or modulated pharmacological effects of xylazine in humans. Further research is urgently needed to more clearly understand the implications of unregulated xylazine in the illicit drug market, to formulate public health interventions, and to implement harm reduction strategies. [ABSTRACT FROM AUTHOR]

Published
2024
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5. The possible clinical utility of the alcohol biomarker phosphatidylethanol for managing suspected alcohol withdrawal in hospitalized patients: A case report.

Author

Edinoff, Amber N., Hathaway, David B., Martinez Garza, David, Rosen, Jordan H., and Suzuki, Joji

Subjects
*HOSPITAL patients, *ALCOHOL withdrawal syndrome, *BIOMARKERS
Abstract

Background and Objectives: The decision to initiate pharmacotherapy for alcohol withdrawal is typically based on examining self‐reported use of alcohol and symptoms of withdrawal. Phosphatidylethanol (PEth) is a biomarker that could aim in clinical decision‐making in withdrawal management. Methods: This report describes three cases highlighting the potential clinical utility of PEth in caring for individuals at risk for alcohol withdrawal. Results: Two of the cases received phenobarbital when their PEth showed that the risk of withdrawal was low and one case where PEth could have shown this was needed. The results were only available in a delayed fashion, however, could have been useful in informing clinical care. Discussion and Conclusion: PEth can be a useful tool if available without delay. PEth can be used to quickly rule out alcohol withdrawal and avoid misdiagnoses and prolonged hospital stays. Scientific Significance: This is a clinical case study available looking at PEth and withdrawal in hospitalized patients. It proposes that PEth can be used as a way to quickly rule out alcohol withdrawal to avoid misdiagnoses and the possibility of a prolonged hospital stay. [ABSTRACT FROM AUTHOR]

Published
2024
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6. Tianeptine, an Antidepressant with Opioid Agonist Effects: Pharmacology and Abuse Potential, a Narrative Review.

Author

Edinoff, Amber N., Sall, Saveen, Beckman, Scott P., Koepnick, Andrew D., Gold, Logan C., Jackson, Eric D., Wenger, Danielle M., Cornett, Elyse M., Murnane, Kevin S., Kaye, Adam M., and Kaye, Alan D.

Subjects
*PHARMACOLOGY, *MENTAL depression, *CONTROLLED substances, *OPIOIDS, *CONVENIENCE stores
Abstract

Tianeptine is an antidepressant drug approved for the treatment of major depressive disorder in countries other than the US. It is classified as an atypical tricyclic antidepressant and has shown potential benefits in addressing anxiety and irritable bowel disease. However, it is important to note that tianeptine is not approved for any use by the United States Federal Drug Administration (FDA). Despite its lack of approval by the FDA, tianeptine has been distributed online and at small retail locations. The term "gas station drugs" refers to a wide range of substances typically available for purchase from gas stations, corner stores, bodegas, mini marts, smoke shops, and the Internet. These substances may be produced commercially by drug manufacturers or in clandestine laboratories to mimic the effects of more well-known illicit/controlled substances such as marijuana, cocaine, opioids, etc. Tianeptine has made its way to convenience stores and gas station shelves, branded as "Zaza" and "Tianna Red." It can also be obtained online from independent vendors without a prescription. Misuse of tianeptine can lead to euphoric, opioid-like highs with the potential for chronic users to develop dependence and tolerance. Overdose and use in suicide attempts have also been documented. This manuscript is a narrative review, highlighting the dangers of tianeptine and other gas station drugs and underscoring the urgent need to regulate these substances. [ABSTRACT FROM AUTHOR]

Published
2023
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7. Cebranopadol for the Treatment of Chronic Pain.

Author

Edinoff, Amber N., Flanagan, Chelsi J., Roberts, Logan T., Dies, Ross M., Kataria, Saurabh, Jackson, Eric D., DeWitt, Audrey J., Wenger, Danielle M., Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Abstract

Purpose of Review: Regardless of the etiology, if pain persists chronically, it can detrimentally impact multiple aspects of a patient's well-being. Both physical and psychological effects are significant in many chronic pain patients. In this regard, psychological consequences can alter a patient's quality of life, functionality, and social functioning. Opioids have been the long-established gold standard for acute pain treatment in settings such as the postoperative period. An alternative to opioids in pain management has been highly sought after. Through a non-selective mechanism, cebranopadol is a first-in-class oral drug which combines agonism of the mu and nociceptin opioid peptide (NOP) receptors to provide improved analgesia, while reducing the occurrence of many typically opioid side effects. This manuscript is a narrative review of the possible use of cebranopadol in pain management. Recent Findings: In pre-clinical studies, cebranopadol was similar to morphine in its pain control efficacy. In a phase IIa trial, cebranopadol was superior to placebo in reducing pain. In a randomized clinical trial, cebranopadol was superior to morphine. Another study concluded that cebranopadol had a lower misuse potential when compared to hydromorphone. Summary: In summary, cebranopadol offers new opportunities in treating chronic moderate to severe pain, while also countering risks of addiction. Additional studies are warranted to further evaluate the safety and efficacy of cebranopadol. In this regard, cebranopadol could prove to be a promising alternative to current pain treatment options. [ABSTRACT FROM AUTHOR]

Published
2023
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8. Low-Level Laser Therapy for Acute Pain: A Comprehensive Review.

Author

Lutfallah, Salim, Wajid, Irza, Sinnathamby, Evan S., Maitski, Rebecca J., Edinoff, Amber N., Shekoohi, Sahar, Cornett, Elyse M., Urman, Richard D., and Kaye, Alan D.

Abstract

Purpose of Review: An analysis of data conducted in 2015 by the National Health Interview Survey (NHIS) found that an estimated 25.3 million adults (11.2%) have experienced pain every day for the preceding 3 months, and nearly 40 million adults (17.6%) have experienced a severe level of pain. Recent Findings: Multiple reviews have analyzed the current management of acute pain; however, much of the current literature only focuses on pharmacological methods of analgesia, such as opiates, ketamine, or non-steroidal anti-inflammatory drugs (NSAIDs). Publications that discuss non-pharmacological options often criticize the limitations of available research for these therapies, making further exploration of this type of treatment necessary. Summary: The present investigation aims to summarize current knowledge on the use of low-level laser therapy (LLLT), a cold laser non-pharmacological approach, in managing acute pain and to discuss important clinical findings and considerations when it comes to utilizing this treatment option in patients. [ABSTRACT FROM AUTHOR]

Published
2023
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9. The Emerging Role of Ketamine in Acute Postoperative Pain Management.

Author

Edinoff, Amber N., Askins, Dorothy, Bobo, Elena, White, Kathryn L., Eswani, Zahaan, Jackson, Eric D., Wenger, Danielle M., Kaye, Aaron J., Cornett., Elyse M., Kaye, Adam M., and Kaye, Alan D.

Abstract

Purpose of Review: Postoperative pain (POP) is among the most unpleasant experiences that patients face after surgery. Interest in and use of N-methyl-D-aspartate (NMDA) receptor antagonists for the management of POP has increased over the years with ketamine being the most popular drug of this class. Recent Findings: Several randomized controlled trials found that the use of ketamine either alone or in combination with other medications leads to decreased postoperative pain and opioid consumption. However, there are other studies that have not found these benefits. The results as of now suggest that the role of intraoperative ketamine in postoperative pain control varies among different operative procedures. Summary: While some studies have shown promise in ketamine's potential use as a postoperative analgesic, there is still a great deal of proposed research and randomized controlled trials needed to deduce the most efficacious and tolerable form and dose of ketamine. [ABSTRACT FROM AUTHOR]

Published
2023
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11. Low-Dose Initiation of Buprenorphine: A Narrative Review.

Author

Edinoff, Amber N., Fahmy, Omar H., Spillers, Noah J., Zaheri, Alexa R., Jackson, Eric D., De Witt, Audrey J., Wenger, Danielle M., Cornett, Elyse M., Skidmore, Kimberly L., Kaye, Adam M., and Kaye, Alan D.

Abstract

Purpose of Review: Opioid use disorder (OUD) is a chronic disorder in which a person loses control over the use of opioids, develops a compulsive behavior, and defends the use despite knowing the negative consequences. There are numerous treatments for OUD, including buprenorphine. Since it is displacing a full agonist opioid, precipitated withdrawal can occur with standard inductions involving buprenorphine. Recent Findings: Case reports have noted success with a low-dose initiation of buprenorphine, which is different from typical protocols, relatively limited by adverse effects when patients were recently administered full agonists. A cohort investigation studied the use of a transdermal patch as part of the protocol, which was fairly well tolerated. Summary: While ongoing research is being conducted on this topic, recent case studies and smaller cohort studies have demonstrated the feasibility of a trial to treat OUD with low-dose initiation of buprenorphine. [ABSTRACT FROM AUTHOR]

Published
2023
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12. Treatment of Acute Pain in Patients on Naltrexone: A Narrative Review.

Author

Edinoff, Amber N., Flanagan, Chelsi J., Sinnathamby, Evan S., Pearl, Nathan Z., Jackson, Eric D., Wenger, Danielle M., Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Abstract

Purpose of Review: The tissue damage and trauma associated with surgery almost always result in acute postoperative pain. The intensity of postoperative pain can range from mild to severe. Naltrexone is suitable for patients who do not wish to be on an agonist treatment such as methadone or buprenorphine. However, naltrexone has been shown to complicate postoperative pain management. Recent Findings: Multiple studies have found that the use of naltrexone can increase the opioid requirement for postoperative pain control. Other modalities exist that can help outside of opioids such as ketamine, lidocaine/bupivacaine, duloxetine, and non-pharmacological management can help manage pain. Multimodal pain regiments should also be employed in patients. Summary: In addition to traditional methods for postoperative pain management, other methods of acute pain control exist that can help mitigate opioid dependence and help control pain in patients who use naltrexone for their substance use disorders. [ABSTRACT FROM AUTHOR]

Published
2023
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13. Proton Pump Inhibitors, Kidney Damage, and Mortality: An Updated Narrative Review.

Author

Edinoff, Amber N., Wu, Natalie W., Parker, Katelyn, Dudossat, Edwin, Linquest, Lauren, Flanagan, Chelsi J., Dharani, Anam, Patel, Hirni, Willett, Olga, Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Abstract

Since their approval by the Food and Drug Administration (FDA) in 1989, proton pump inhibitors (PPIs) have become one of the most highly utilized drugs in the United States, assuming a position as one of the top 10 most prescribed medications in the country. The purpose of PPIs is to limit the amount of gastric acid secreted by the parietal cells via irreversible inhibition of the H+/K+-ATPase pump, therefore maintaining an elevated gastric acid pH of greater than 4 for 15–21 h. Even though PPIs have many clinical uses, they are not without their adverse effects, mimicking achlorhydria. Besides electrolyte abnormalities and vitamin deficiencies, long-term use of PPIs has been linked to acute interstitial nephritis, bone fractures, poor COVID-19 infection outcomes, pneumonia, and possibly an increase in all-cause mortality. The causality between PPI use and increased mortality and disease risk can be questioned since most studies are observational. Confounding variables can greatly affect an observational study and explain the wide-ranging associations with the use of PPIs. Patients on PPIs are generally older, obese, sicker with a higher number of baseline morbidities, and on more medications than the compared PPI non-users. These findings suggest that PPI users are at a higher risk of mortality and complications based on pre-existing conditions. This narrative review aims to update readers on the concerning effects that proton pump inhibitor use can have on patients and give providers a resource to create informed decisions on appropriate PPI use. [ABSTRACT FROM AUTHOR]

Published
2023
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14. The Use of Oxytocin for the Treatment of Opioid Use Disorder.

Author

Edinoff, Amber N., Sall, Saveen, Honore, Lauryn G., Dies, Ross M., Zaheri, Alexa R., Kataria, Saurabh, Jackson, Eric D., Shekoohi, Sahar, Cornett, Elyse M., Murnane, Kevin S., Kaye, Adam M., and Kaye, Alan D.

Abstract

Nearly 27 million people have an opioid use disorder (OUD) according to the 2016 Global Burden of Disease study, most of which occur in the US where opioids are a common class of medication used to treat acute and chronic pain. In 2016 alone, more than 60 million patients had at least one prescription for opioids filled or refilled. Over the past decade, prescription rates have risen astronomically and have created an epidemic in the US dubbed the "opioid crisis." In this regard, there has been an increase in overdoses and OUD diagnoses. Several studies have found dysregulation of balance between several neurotransmitters involved in the neural circuitry that subserves several behavioral domains, such as reward recognition, motivation, learning, and memory, affect, stress, and executive function, that contribute to the manifestation of craving. On the horizon is a new treatment approach consisting of the neuropeptide oxytocin, which may be involved in the overlapping mechanisms of stable attachment formation and coping with stress. Through this mechanism, it can shift processing from novelty and reward-seeking to an appreciation of familiarity and thus reduce stress and increase resilience in the face of addiction. It has been hypothesized that there is a connection between the glutaminergic and oxytocinergic systems, making oxytocin a possible therapeutic agent in reducing drug-induced actions seen in OUD patients. This manuscript will review the potential and feasible use of oxytocin in treating OUD. [ABSTRACT FROM AUTHOR]

Published
2023
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15. New Synthetic Opioids: Clinical Considerations and Dangers.

Author

Edinoff, Amber N., Martinez Garza, David, Vining, Stephen P., Vasterling, Megan E., Jackson, Eric D., Murnane, Kevin S., Kaye, Adam M., Fair, Richard N., Torres, Yair Jose Lopez, Badr, Ahmed E., Cornett, Elyse M., and Kaye, Alan D.

Subjects
*POSITRON emission tomography, *OPIOID epidemic, *OPIOID receptors, *OPIOIDS, *ANIMAL anesthesia
Abstract

Since the early 2010s, synthetic opioids have significantly contributed to overall opioid-related overdose mortalities. For point of reference, of the 68,630 opioid-related deaths recorded in 2020, 56,516 involved synthetic opioids. During much of this period, fentanyl has been the most commonly used synthetic opioid. This time when fentanyl was the most popular opioid has been called the "third wave" of the opioid crisis, partly because it led to a sharp rise in deaths from overdoses. Other synthetic opioids, such as carfentanil, protonitazene, and isotonitazene, have also become more widely diverted for nonmedical used. Carfentanil is an even more potent fentanyl derivative that was initially used in the mid-1980s as a general anesthetic for large animals such as elephants. Related to its strong affinity for mu opioid receptors, carfentanil is still utilized in medicine and science today as a radiotracer for positron emission tomography imaging. Protonitazene and isotonitazene belong to a novel class of synthetic opioids called benzimidazoles that were manufactured in the 1950s as novel analgesics. These agents have come under recent scrutiny as designer synthetic opioids becoming more prevalent. However, to date, there is incomplete data regarding the prevalence of synthetic opioids, as traditional toxicology screenings may not be sensitive to detect these compounds at such low doses post-mortem, particularly when blood is drawn from the periphery instead of central tissues such as the brain, lung, or heart. This narrative review aims to highlight the clinical challenges presented by these new synthetic opioids. [ABSTRACT FROM AUTHOR]

Published
2023
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16. Tocilizumab for Severe COVID-19 Infection and Multisystem Inflammatory Syndrome in Adults and Children.

Author

Edinoff, Amber N., Alpaugh, Edward Sanders, Newgaard, Olivia, Wajid, Irza, Klapper, Rachel J., Cornett, Elyse M., Kaye, Adam M., Iyer, Praneet, and Kaye, Alan D.

Subjects
*MULTISYSTEM inflammatory syndrome in children, *COVID-19, *MULTISYSTEM inflammatory syndrome, *MIDDLE East respiratory syndrome, *COVID-19 pandemic
Abstract

Coronavirus disease 2019 (COVID-19) rapidly emerged as a global pandemic, placing imminent stress and burden on healthcare resources and workers worldwide. Many patients who present with a severe COVID-19 infection are at high risk of developing severe acute respiratory distress syndrome (ARDS), leading to a vast number of patients requiring mechanical ventilation and a high mortality rate. Similar to Middle East respiratory syndrome, COVID-19 demonstrates an initial viral replication phase that manifests as a variety of symptoms typically flu-like in nature, followed by a profound inflammatory response leading to rapid production of cytokines and uncontrolled inflammation. There have also been many cases of COVID-19 in pediatric patients presenting with elevated inflammatory markers and multisystem involvement labeled as a multisystem inflammatory syndrome (MIS-C) by the world health organization (WHO). The recent treatment of systemic inflammatory response to COVID-19 targets the secondary phase involving cytokine release syndrome. The detrimental effects of IL-6 can be profound and elevated levels are associated with a higher mortality rate and mechanical ventilation. Tocilizumab is an IL-6 inhibitor most widely investigated to target cytokine storm syndrome. Since June 2021, the FDA enacted an emergency use authorization for tocilizumab in the treatment of COVID-19. Several clinical trials have investigated tocilizumab combined with corticosteroids for treating severe ARDS associated with COVID-19. An increasing amount of evidence suggests that targeting the cytokine storm syndrome related to COVID-19 can lead to improved outcomes, especially in those patients requiring mechanical ventilation and with a critical illness. Additional studies are warranted to further look at the positive effects of tocilizumab in the COVID-19 population while additionally defining possible adverse effects. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Transcranial Stimulation for the Treatment of Stimulant Use Disorder.

Author

Edinoff, Amber N., Sall, Saveen, Roberts, T. Dean, Tomlinson, Henry H., Soileau III, Lenise G., Jackson, Eric D., Murnane, Kevin S., Wenger, Danielle M., Cornett, Elyse M., Toms, Jaime, Kumbhare, Deepak, Kaye, Adam M., and Kaye, Alan D.

Subjects
*COCAINE-induced disorders, *TRANSCRANIAL magnetic stimulation, *REWARD (Psychology), *STIMULANTS, *NERVE endings, *MENTAL illness, *DOPAMINE receptors
Abstract

The increasing prevalence of stimulant use disorder (StUD) involving methamphetamine and cocaine has been a growing healthcare concern in the United States. Cocaine usage is associated with atherosclerosis, systolic and diastolic dysfunction, and arrhythmias. Furthermore, approximately one of every four MIs is cocaine-induced among patients aged 18 to 45. Methamphetamine use has been associated with nerve terminal damage in the dopaminergic system resulting in impaired motor function, cognitive decline, and co-morbid psychiatric disorders. Current treatment options for StUD are extremely limited, and there are currently no FDA-approved pharmacotherapies. Behavioral interventions are considered first-line treatment; however, in a recent meta-analysis comparing behavioral treatment options for cocaine, contingency management programs provided the only significant reduction in use. Current evidence points to the potential of various neuromodulation techniques as the next best modality in treating StUD. The most promising evidence thus far has been transcranial magnetic stimulation which several studies have shown to reduce risk factors associated with relapse. Another more invasive neuromodulation technique being studied is deep-brain stimulation, which has shown promising results in its ability to modulate reward circuits to treat addiction. Results showing the impact of transcranial magnetic stimulation (TMS) in the treatment of StUD are limited by the lack of studies conducted and the limited understanding of the neurological involvement driving addiction-based diseases such as StUD. Future studies should seek to provide data on consumption-reducing effects rather than craving evaluations. [ABSTRACT FROM AUTHOR]

Published
2023
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18. Ketamine Evolving Clinical Roles and Potential Effects with Cognitive, Motor and Driving Ability.

Author

Edinoff, Amber N., Sall, Saveen, Koontz, Colby B., Williams, Ajah K., Drumgo, DeMarcus, Mouhaffel, Aya, Cornett, Elyse M., Murnane, Kevin S., and Kaye, Alan D.

Subjects
*KETAMINE abuse, *DRUGGED driving, *MOTOR ability, *KETAMINE, *DRUNK driving, *MOTOR vehicle driving
Abstract

While driving under the influence of drugs, drivers are more likely to be involved in and cause more accidents than drivers who do not drive under the influence. Ketamine is derived from phencyclidine and acts as a noncompetitive antagonist and allosteric modulator of N-methyl-D-aspartate receptors. Ketamine has been used to treat a variety of psychiatric disorders, with the most notable being treatment-resistant depression. With the rise of at-home ketamine treatment companies, the safety of unsupervised administration remains under evaluation. A study with ketamine and a ketamine-like medication, rapasitnel, showed that those who were given ketamine experienced more sleepiness and had decreased self-reported motivation and confidence in their driving abilities. Moreover, there seem to be significant differences in the acute versus persistent effects of ketamine, as well as the anesthetic versus subanesthetic doses, both in terms of effects and outcomes. These divergent effects complicate the clinical uses of ketamine, specifically involving driving, drowsiness, and cognitive abilities. This review aims to describe not only the various clinical uses of ketamine but also the potentially detrimental effects of driving under the influence, which should be understood to help with counseling the patients who use these substances, both for their well-being and to protect public safety. [ABSTRACT FROM AUTHOR]

Published
2023
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19. Chronic Administration of Melatonin: Physiological and Clinical Considerations.

Author

Givler, Donald, Givler, Amy, Luther, Patrick M., Wenger, Danielle M., Ahmadzadeh, Shahab, Shekoohi, Sahar, Edinoff, Amber N., Dorius, Bradley K., Jean Baptiste, Carlo, Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
CONTROLLED release preparations, MELATONIN, AUTISM spectrum disorders, ALZHEIMER'S disease, MILD cognitive impairment
Abstract

Background: Exogenous melatonin is commonly used to treat insomnia, other sleep problems, and numerous medical illnesses, including Alzheimer's disease, autism spectrum disorder, and mild cognitive impairment in adults and children. There is evolving information regarding issues with the use of chronic melatonin. Methods: The present investigation was a narrative review. Results: Melatonin usage has risen dramatically in recent years. Many countries only allow melatonin prescriptions. In the United States (U.S.), it is classified as a dietary supplement accessible over the counter and can be derived from animals, microorganisms, or, most commonly, made synthetically. No regulatory agency oversees its manufacturing or sale in the U.S. melatonin concentration of marketed preparations varies widely between product labels and manufacturers. Melatonin's ability to induce sleep is detectable. However, it is modest for most people. Sleep length appears to be less important in sustained-release preparations. The optimal dosage is unknown, and routinely used amounts vary substantially. Melatonin's short-term negative effects are minimal, resolve at medicine cessation, and do not usually prevent usage overall. Much research on long-term melatonin administration has found no difference between exogenous melatonin and placebo in terms of long-term negative effects. Conclusion: Melatonin at low to moderate dosages (approximately 5–6 mg daily or less) appears safe. Long-term usage appears to benefit certain patient populations, such as those with autism spectrum disorder. Studies investigating potential benefits in reducing cognitive decline and increased longevity are ongoing. However, it is widely agreed that the long-term effects of taking exogenous melatonin have been insufficiently studied and warrant additional investigation. [ABSTRACT FROM AUTHOR]

Published
2023
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25. Regenerative Medicine: Pharmacological Considerations and Clinical Role in Pain Management.

Author

Kaye, Alan D., Edinoff, Amber N., Rosen, Yale E., Boudreaux, Megan A., Kaye, Aaron J., Sheth, Meeta, Cornett, Elyse M., Moll, Vanessa, Friedrich, Claudia, Verhagen, Johan Sibrecht, Moser, Berthold, and Navani, Annu

Abstract

Purpose of Review: Low back pain affects at least 80% of individuals at some point in their lifetime and is the fifth most common reason for physician visits in the USA. Treatment of an acute episode of LBP generally includes rest, activity modification, physical therapy, NSAIDs, and patient education. Recent Findings: A small percentage of patients will develop chronic pain lasting > 6 months duration. Platelet-rich plasma (PRP) is one of the main pillars of regenerative medicine, as its release of bioactive proteins supports the aim of RM of restoring the anatomical function in degenerative conditions. Mesenchymal stem cells (MSCs) are multipotent stem cells, multipotent progenitor cells, or marrow stromal cells found in various body tissues, including bone marrow, lung, and adipose tissue. Evidence from well-designed case–control or cohort studies for the use of PRP and MSCs in lumbar facet joint, lumbar epidural, and sacroiliac joint injections is currently described as level IV evidence. PRP and MSCs are used autogenously to help facilitate the healing process, and their injection has been studied in the long-term management of discogenic low back pain. PRP has been compared to steroid injections in the sacroiliac joint for chronic low back pain, with favorable results. MSCs have also been shown to be useful in intervertebral disc regeneration and treatment of chronic low back pain associated with degenerative disc disease. Summary: Currently, the price for these treatments is extremely high, and thus the standard of care continues to be steroid injections and other treatments. This could change, however, with more robust data and research on the safety and long-term efficacy of biologics compared to other interventional management. [ABSTRACT FROM AUTHOR]

Published
2022
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26. Novel Designer Benzodiazepines: Comprehensive Review of Evolving Clinical and Adverse Effects.

Author

Edinoff, Amber N., Nix, Catherine A., Odisho, Amira S., Babin, Caroline P., Derouen, Alyssa G., Lutfallah, Salim C., Cornett, Elyse M., Murnane, Kevin S., Kaye, Adam M., and Kaye, Alan D.

Subjects
*DRUG accessibility, *BENZODIAZEPINES, *DRUG bioavailability, *DESIGNERS, *INTERNET marketing
Abstract

As tranquilizers, benzodiazepines have a wide range of clinical uses. Recently, there has been a significant rise in the number of novel psychoactive substances, including designer benzodiazepines. Flubromazolam(8-bromo-6-(2-fluorophenyl)-1-methyl-4H-[1,2,4]triazolo[4,3-a][1,4]benzodiazeZpine) is a triazolo-analogue of flubromazepam. The most common effects noted by recreational users include heavy hypnosis and sedation, long-lasting amnesia, and rapid development of tolerance. Other effects included anxiolysis, muscle-relaxing effects, euphoria, loss of control, and severe withdrawals. Clonazolam, or 6-(2-chlorophenyl)-1-methyl-8-nitro-4H-[1,2,4]triazolo[4,3-α]-[1,4]-benzodiazepine, is a triazolo-analog of clonazepam. It is reported to be over twice as potent as alprazolam. Deschloroetizolam (2-Ethyl-9-methyl-4-phenyl-6H-thieno[3,2-f][1,2,4]triazolo[4,3-a][1,4]diazepine) is part of the thienodiazepine drug class, which, like benzodiazepines, stimulates GABA-A receptors. Meclonazepam ((3S)-5-(2-chlorophenyl)-3-methyl-7-nitro-1,3-dihydro-1,4-benzodiazepin-2-one) is a designer benzodiazepine with additional anti-parasitic effects. Although it has proven to be an efficacious therapy for schistosomiasis, its sedative side effects have prevented it from being marketed as a therapeutic agent. The use of DBZs has been a subject of multiple recent clinical studies, likely related to increasing presence and availability on the internet drug market and lack of regulation. Many studies have aimed to identify the prevalence of DBZs and their effects on those using them. This review discussed these designer benzodiazepines and the dangers and adverse effects that the clinician should know. [ABSTRACT FROM AUTHOR]

Published
2022
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30. Alternative Options for Complex, Recurrent Pain States Using Cannabinoids, Psilocybin, and Ketamine: A Narrative Review of Clinical Evidence.

Author

Edinoff, Amber N., Fort, Juliana M., Singh, Christina, Wagner, Sarah E., Rodriguez, Jessica R., Johnson, Catherine A., Cornett, Elyse M., Murnane, Kevin S., Kaye, Adam M., and Kaye, Alan D.

Subjects
*PSILOCYBIN, *CANNABINOIDS, *PAIN management, *KETAMINE, *SEROTONIN receptors, *CANCER pain
Abstract

With emerging information about the potential for morbidity and reduced life expectancy with long-term use of opioids, it is logical to evaluate nonopioid analgesic treatments to manage pain states. Combinations of drugs can provide additive and/or synergistic effects that can benefit the management of pain states. In this regard, tetrahydrocannabinol (THC) and cannabidiol (CBD) modulate nociceptive signals and have been studied for chronic pain treatment. Psilocybin, commonly known as "magic mushrooms", works at the serotonin receptor, 5-HT2A. Psilocybin has been found in current studies to help with migraines since it has a tryptamine structure and works similarly to triptans. Psilocybin also has the potential for use in chronic pain treatment. However, the studies that have looked at alternative plant-based medications such as THC, CBD, and psilocybin have been small in terms of their sample size and may not consider the demographic or genetic differences in the population because of their small sample sizes. At present, it is unclear whether the effects reported in these studies translate to the general population or even are significant. In summary, additional studies are warranted to evaluate chronic pain management with alternative and combinations of medications in the treatment of chronic pain. [ABSTRACT FROM AUTHOR]

Published
2022
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33. The Possible Application of Ketamine in the Treatment of Depression in Alzheimer's Disease.

Author

Mohammad Shehata, Islam, Masood, Waniyah, Nemr, Nouran, Anderson, Alexandra, Bhusal, Kamal, Edinoff, Amber N., Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
KETAMINE abuse, ALZHEIMER'S disease, SEROTONIN uptake inhibitors, KETAMINE, SEROTONIN syndrome, ANTIDEPRESSANTS, MENTAL depression
Abstract

Depression is a leading cause of disability globally, with a prevalence of 3.8% among the whole population, 5% of the adult population, and 5.7% of the elderly population over 60 years of age. There is evidence that depression is linked to certain neurodegenerative diseases, one being Alzheimer's disease (AD). The efficacy of conventional antidepressants to treat depression in AD is conflicting, especially regarding selective serotonin reuptake inhibitors (SSRIs). A recent systemic review and meta-analysis of 25 randomized controlled trials including fourteen antidepressant medications showed no high efficacy in treating AD patients' symptoms. However, ketamine, a nonselective N-methyl-D-aspartate (NMDA) receptor antagonist, can mediate a wide range of pharmacological effects, including neuroprotection, anti-inflammatory and anticancer properties, multimodal analgesia, and treatment of depression, suicidal attempts, and status epilepticus. Esketamine, which is ketamine formulated as a nasal spray, was approved by the Federal Drug Administration (FDA) in March 2019 as an adjuvant drug to treat treatment-resistant depression. NMDA receptor antagonists treat AD through offsetting AD-related pathological stimulation of subtypes of glutamate receptors in the central nervous system. Recent clinical findings suggest that ketamine may provide neuroprotection and reduce neuropsychiatric symptoms associated with AD. In the present investigation, we evaluate the potential role of ketamine and its postulated mechanism in AD management. [ABSTRACT FROM AUTHOR]

Published
2022
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34. Transcranial Magnetic Stimulation for Post-traumatic Stress Disorder.

Author

Edinoff, Amber N., Hegefeld, Tanner L., Petersen, Murray, Patterson II, James C., Yossi, Christopher, Slizewski, Jacob, Osumi, Ashley, Cornett, Elyse M., Kaye, Adam, Kaye, Jessica S., Javalkar, Vijayakumar, Viswanath, Omar, Urits, Ivan, and Kaye, Alan D.

Subjects
TRANSCRANIAL magnetic stimulation, POST-traumatic stress disorder, EXECUTIVE function, SALIENCE network, CONTROL (Psychology)
Abstract

Post-traumatic stress disorder (PTSD) is a psychiatric disorder that causes significant functional impairment and is related to altered stress response and reinforced learned fear behavior. PTSD has been found to impact three functional networks in the brain: default mode, executive control, and salience. The executive control network includes the dorsolateral prefrontal cortex (DLPFC) and lateral PPC. The salience network involves the anterior cingulate cortex, anterior insula, and amygdala. This latter network has been found to have increased functional connectivity in PTSD. Transcranial Magnetic Stimulation (TMS) is a technique used in treating PTSD and involves stimulating specific portions of the brain through electromagnetic induction. Currently, high-frequency TMS applied to the left dorsolateral prefrontal cortex (DLPFC) is approved for use in treating major depressive disorder (MDD) in patients who have failed at least one medication trial. In current studies, high-frequency stimulation has been shown to be more effective in PTSD rating scales posttreatment than low-frequency stimulation. The most common side effect is headache and scalp pain treated by mild analgesics. Seizures are a rare side effect and are usually due to predisposing factors. Studies have been done to assess the overall efficacy of TMS. However, results have been conflicting, and sample sizes were small. More research should be done with larger sample sizes to test the efficacy of TMS in the treatment of PTSD. Overall, TMS is a relatively safe treatment. Currently, the only FDA- approved to treat refractory depression, but with the potential to treat many other conditions. [ABSTRACT FROM AUTHOR]

Published
2022
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35. Antipsychotic Polypharmacy-Related Cardiovascular Morbidity and Mortality: A Comprehensive Review.

Author

Edinoff, Amber N., Ellis, Emily D., Nussdorf, Laura M., Hill, Taylor W., Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
*ARRHYTHMIA, *VENTRICULAR arrhythmia, *CARDIAC arrest, *CONCOMITANT drugs, *DRUGS of abuse, *ANTIPSYCHOTIC agents, *BLOOD pressure
Abstract

Schizophrenia is a psychotic disorder that exists at the more extreme end of a spectrum of diseases, and significantly affects daily functioning. Cardiovascular adverse effects of antipsychotic medications are well known, and include changes in blood pressure and arrhythmias. Sudden cardiac death is the leading cause of death worldwide, and antipsychotic medications are associated with numerous cardiac side effects. A possible link exists between antipsychotic medications and sudden cardiac death. Common prescribing patterns that may influence cardiovascular events include the use of multiple antipsychotics and/or additional drugs commonly prescribed to patients on antipsychotics. The results of this review reflect an association between antipsychotic drugs and increased risk of ventricular arrhythmias and sudden cardiac death by iatrogenic prolongation of the QTc interval. QTc prolongation and sudden cardiac death exist in patients taking antipsychotic monotherapy. The risk increases for the concomitant use of specific drugs that prolong the QTc interval, such as opioids, antibiotics, and illicit drugs. However, evidence suggests that QTc intervals may not adequately predict sudden cardiac death. In considering the findings of this narrative review, we conclude that it is unclear whether there is a precise association between antipsychotic polypharmacy and sudden cardiac death with QTc interval changes. The present narrative review warrants further research on this important potential association. [ABSTRACT FROM AUTHOR]

Published
2022
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36. Oxytocin, a Novel Treatment for Methamphetamine Use Disorder.

Author

Edinoff, Amber N., Thompson, Elliot, Merriman, Chandler E., Alvarez, Mark R., Alpaugh, E. Saunders, Cornett, Elyse M., Murnane, Kevin S., Kozinn, Rachel L., Shah-Bruce, Mila, Kaye, Adam M., and Kaye, Alan D.

Subjects
*METHAMPHETAMINE, *OXYTOCIN, *METHAMPHETAMINE abuse, *SOCIAL anxiety, *SUBSTANCE abuse treatment, *DRUGS of abuse
Abstract

The treatment of substance abuse with oxytocin is a novel approach to a challenging public health issue that continues to contribute to a growing economic cost for societies worldwide. Methamphetamine addiction is one of the leading causes of mortality worldwide, and despite advances in understanding the neurobiology of methamphetamine addiction, treatment options are limited. There are no medications that the Food and Drug Administration currently approves for stimulant use disorder. Off-label use of therapies for stimulant misuse include antidepressants, anxiolytics, and milder stimulants as replacement agents. Due to the shortcomings of these attempts to treat a complicated psychiatric disorder, recent attention to oxytocin therapy (OT) has gained momentum in clinical studies as a possible therapy in the context of social stress, social anxiety, social cognition, and psychosis. Oxytocin produces enhanced connectivity between cortical regions. The results from studies in rodents with OT suggest that central neuromodulation of oxytocin may be beneficial across transition states of stimulant dependence and may alleviate intense withdrawal symptoms. Studies of oxytocin in the context of other drugs of abuse, including cocaine, cannabis, and alcohol, also support the potential of oxytocin to treat stimulant use disorder, methamphetamine type. Methamphetamine abuse continues to be a significant cause of distress and dysfunction throughout the world. The effects of oxytocin on methamphetamine use outlined in this review should act as a catalyst for further investigation into the efficacy of treating stimulant use disorder, methamphetamine type with oxytocin in humans. More human-based research should initiate studies involving the long-term efficacy, side effects, and patient selection. [ABSTRACT FROM AUTHOR]

Published
2022
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37. Bremelanotide for Treatment of Female Hypoactive Sexual Desire.

Author

Edinoff, Amber N., Sanders, Nicole M., Lewis, Kyle B., Apgar, Tucker L., Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
*LUST, *HYPOACTIVE sexual desire disorder, *SEXUAL intercourse, *MELANOCORTIN receptors, *SEXUAL fantasies
Abstract

Hypoactive sexual desire disorder (HSDD) is a persistent deficiency or absence of sexual fantasies and desire resulting in significant distress or interpersonal difficulty. Women with this disorder may display a lack of motivation for sexual activity, reduced responsiveness to erotic cues, a loss of interest during sexual activity, and avoidance of situations that could lead to sexual activity. The pathophysiology of HSDD is thought to be centered around inhibitory and excitatory hormones, neurotransmitters, and specific brain anatomy. Due to the multifactorial nature of HSDD, treatment can be complex and must attempt to target the biological and psychosocial aspects of the disorder. Bremelanotide is a melanocortin receptor agonist and has been recently approved by the FDA to treat HSDD. Bremelanotide is administered intranasally or as a subcutaneous injection. The recommended dosage of bremelanotide is 1.75 mg injected subcutaneously in the abdomen or thigh at least 45 min before sexual activity. Studies showed improvements in desire, arousal, and orgasm scores when 1.75 mg of bremelanotide was administered before sexual activity compared to a placebo. Bremelanotide is a promising way to treat HSDD. [ABSTRACT FROM AUTHOR]

Published
2022
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38. Antipsychotic Use in Pregnancy: Patient Mental Health Challenges, Teratogenicity, Pregnancy Complications, and Postnatal Risks.

Author

Edinoff, Amber N., Sathivadivel, Niroshan, McNeil, Shawn E., Ly, Austin I., Kweon, Jaeyeon, Kelkar, Neil, Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
*PREGNANCY complications, *FETAL growth disorders, *PEOPLE with mental illness, *MENTAL illness, *PREGNANT women, *FETAL surgery
Abstract

Pregnant women constitute a vulnerable population, with 25.3% of pregnant women classified as suffering from a psychiatric disorder. Since childbearing age typically aligns with the onset of mental health disorders, it is of utmost importance to consider the effects that antipsychotic drugs have on pregnant women and their developing fetus. However, the induction of pharmacological treatment during pregnancy may pose significant risks to the developing fetus. Antipsychotics are typically introduced when the nonpharmacologic approaches fail to produce desired effects or when the risks outweigh the benefits from continuing without treatment or the risks from exposing the fetus to medication. Early studies of pregnant women with schizophrenia showed an increase in perinatal malformations and deaths among their newborns. Similar to schizophrenia, women with bipolar disorder have an increased risk of relapse in antepartum and postpartum periods. It is known that antipsychotic medications can readily cross the placenta, and exposure to antipsychotic medication during pregnancy is associated with potential teratogenicity. Potential risks associated with antipsychotic use in pregnant women include congenital abnormalities, preterm birth, and metabolic disturbance, which could potentially lead to abnormal fetal growth. The complex decision-making process for treating psychosis in pregnant women must evaluate the risks and benefits of antipsychotic drugs. [ABSTRACT FROM AUTHOR]

Published
2022
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39. Naltrexone Implant for Opioid Use Disorder.

Author

Edinoff, Amber N., Nix, Catherine A., Orellana, Claudia V., StPierre, Samantha M., Crane, Erin A., Bulloch, Blaine T., Cornett, Elyse M., Kozinn, Rachel L., Kaye, Adam M., Murnane, Kevin S., and Kaye, Alan D.

Subjects
*OPIOID abuse, *NALTREXONE, *OPIOID peptides, *ORAL medication, *ADDICTIONS, *CANCER pain
Abstract

The continued rise in the availability of illicit opioids and opioid-related deaths in the United States has left physicians, researchers, and lawmakers desperate for solutions to this ongoing epidemic. The research into therapeutic options for the treatment of opioid use disorder (OUD) began with the introduction of methadone in the 1960s. The approval of oral naltrexone initially showed much promise, as the drug was observed to be highly potent in antagonizing the effects of opioids while producing no opioid agonist effects of its own and having a favorable side effect profile. Patients that routinely take their naltrexone reported fewer days of heroin use and had more negative drug tests than those without treatment. Poor outcomes in OUD patients treated with naltrexone have been directly tied to short treatment time. Studies have shown that naltrexone given orally vs. as an implant at the 6-month interval showed a higher non-compliance rate among those who used oral medications at the 6-month mark and a slower return to use rate. There were concerns that naltrexone could possibly worsen negative symptoms seen in opiate use disorder related to blockade of endogenous opioids that are important for pleasurable stimuli. Studies have shown that naltrexone demonstrated no increase in levels of anxiety, depression and anhedonia in participants and another study found that those treated with naltrexone had a significant reduction in mental health-related hospitalizations. The latter study also concluded that there was no increased risk for mental health-related incidents in patients taking naltrexone via a long-acting implant. Although not yet FDA approved in the United States, naltrexone implant has shown promising results in Europe and Australia and may provide a novel treatment option for opioid addiction. [ABSTRACT FROM AUTHOR]

Published
2022
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42. Viloxazine in the Treatment of Attention Deficit Hyperactivity Disorder.

Author

Edinoff, Amber N., Akuly, Haseeb A., Wagner, John H., Boudreaux, Megan A., Kaplan, Leah A., Yusuf, Shadman, Neuchat, Elisa E., Cornett, Elyse M., Boyer, Andrea G., Kaye, Adam M., and Kaye, Alan D.

Subjects
ATTENTION-deficit hyperactivity disorder, THERAPEUTICS, CHILD patients
Abstract

Attention deficit hyperactivity disorder (ADHD) is the most common neurodevelopmental disorder in children. Over the past twenty years, research on the disease and its characteristics and treatment options has grown exponentially. The first-line pharmacologic treatment of ADHD is stimulants, which have a response rate of ~70%. With the support of four phase 3 studies involving more than 1,000 pediatric patients 6–17 years old, the FDA has approved the non-stimulant, serotonin-norepinephrine modulating agent (SNMA) viloxazine in an extended-release capsule (viloxazine ER) for treatment of ADHD in children aged 6–17. Viloxazine modulates serotonergic activity as a selective 5-HT22B receptor antagonist and 5-HT2C receptor agonist and moderately inhibits norepinephrine transporter (NET), thus blocking the reuptake of norepinephrine. A phase 2 study by Johnson et al. found that once-daily dosing of viloxazine ER in 200, 300, or 400 mg dosages in children with ADHD for eight weeks resulted in a statistically significant reduction of ADHD-RS-IV total score. A post hoc analysis of data from four phase 3, randomized, placebo-controlled, double-blind, three-arm, clinical trials by Faraone et al. found that early response to viloxazine treatment, defined as a change in ADHD-RS-5 total score at week 2, best predicted the treatment response at week 6 [75% positive predictive power (PPP), 75% sensitivity]. Proper treatment of the symptoms and comorbidities associated with ADHD is crucial in improving a patient's quality of life, cognitive function, and overall therapeutic outcomes. Viloxazine's mechanism of action, clinical effects, and limited side effect profile point toward the drug's relevance in the treatment of ADHD. [ABSTRACT FROM AUTHOR]

Published
2021
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43. Benzodiazepines: Uses, Dangers, and Clinical Considerations.

Author

Edinoff, Amber N., Nix, Catherine A., Hollier, Janice, Sagrera, Caroline E., Delacroix, Blake M., Abubakar, Tunde, Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
*DRUG withdrawal symptoms, *CENTRAL nervous system depressants, *PSYCHIATRIC drugs, *BENZODIAZEPINES, *ALCOHOL withdrawal syndrome, *BLOOD-brain barrier, *EPILEPSY
Abstract

Benzodiazepines (BZDs) are among one of the most widely prescribed drug classes in the United States. BZDs are a class of psychoactive drugs known for their depressant effect on the central nervous system (CNS). They quickly diffuse through the blood–brain barrier to affect the inhibitory neurotransmitter GABA and exert sedative effects. Related to their rapid onset and immediate symptom relief, BZDs are used for those struggling with sleep, anxiety, spasticity due to CNS pathology, muscle relaxation, and epilepsy. One of the debilitating side effects of BZDs is their addictive potential. The dependence on BZDs generally leads to withdrawal symptoms, requiring careful tapering of the medication when prescribed. Regular use of BZDs has been shown to cause severe, harmful psychological and physical dependence, leading to withdrawal symptoms similar to that of alcohol withdrawal. Some of these withdrawal symptoms can be life threatening. The current treatment for withdrawal is through tapering with clonazepam. Many drugs have been tested as a treatment for withdrawal, with few proving efficacious in randomized control trials. Future research is warranted for further exploration into alternative methods of treating BZD withdrawal. This call to action proves especially relevant, as those seeking treatment for BZD dependence and withdrawal are on the rise in the United States. [ABSTRACT FROM AUTHOR]

Published
2021
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44. Catatonia: Clinical Overview of the Diagnosis, Treatment, and Clinical Challenges.

Author

Edinoff, Amber N., Kaufman, Sarah E., Hollier, Janice W., Virgen, Celina G., Karam, Christian A., Malone, Garett W., Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
*SINUS thrombosis, *CATATONIA, *ANTI-NMDA receptor encephalitis, *NEUROLEPTIC malignant syndrome, *ELECTROCONVULSIVE therapy, *GABA
Abstract

Catatonia is a syndrome that has been associated with several mental illness disorders but that has also presented as a result of other medical conditions. Schizophrenia and other psychiatric disorders such as mania and depression are known to be associated with catatonia; however, several case reports have been published of certain medical conditions inducing catatonia, including hyponatremia, cerebral venous sinus thrombosis, and liver transplantation. Neuroleptic Malignant Syndrome and anti-NMDA receptor encephalitis are also prominent causes of catatonia. Patients taking benzodiazepines or clozapine are also at risk of developing catatonia following the withdrawal of these medications—it is speculated that the prolonged use of these medications increases gamma-aminobutyric acid (GABA) activity and that discontinuation may increase excitatory neurotransmission, leading to catatonia. The treatment of catatonia often involves the use of benzodiazepines, such as lorazepam, that can be used in combination therapy with antipsychotics. Definitive treatment may be found with electroconvulsive therapy (ECT). Aberrant neuronal activity in different motor pathways, defective neurotransmitter regulation, and impaired oligodendrocyte function have all been proposed as the pathophysiology behind catatonia. There are many clinical challenges that come with catatonia and, as early treatment is associated with better outcomes, it becomes imperative to understand these challenges. The purpose of this manuscript is to provide an overview of these challenges and to look at clinical studies regarding the pathophysiology, diagnosis, and treatment of as well as the complications and risk factors associated with catatonia. [ABSTRACT FROM AUTHOR]

Published
2021
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45. Pharmacological Advances in Opioid Therapy: A Review of the Role of Oliceridine in Pain Management.

Author

Kaye, Alan D., Edinoff, Amber N., Babin, Katherine C., Hebert, Chance M., Hardin, Justin L., Cornett, Elyse M., Kaye, Aaron J., Kaye, Adam M., and Urman, Richard D.

Subjects
*PAIN management, *ALLERGY desensitization, *POSTOPERATIVE pain treatment, *ANALGESICS, *OPIOIDS, *NARCOTICS
Abstract

Problems with the treatment of acute pain may arise when a patient is opioid-tolerant, such as those on chronic therapy with opioids or opiate replacement therapy, those who misuse opioids, and those who are in recovery. While some of the adverse effects of opioid medications are well known, it is also important to recognize the roles of tolerance and hyperalgesia. Oliceridine can target and modulate a novel μ-receptor pathway. The G protein-biased agonism of oliceridine allows for effective re-sensitization and desensitization of the mu-opioid receptor, which decreases the formation of opioid tolerance in patients. Oliceridine has been demonstrated to be an effective and relatively safe intravenous analgesic for the treatment of postoperative pain and is generally well tolerated with a favorable side effect profile when compared to morphine. As the prevalence of pain increases, it is becoming increasingly important to find safe and effective analgesics. [ABSTRACT FROM AUTHOR]

Published
2021
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48. Paliperidone 3-Month Injection for Treatment of Schizophrenia: A Narrative Review.

Author

Edinoff, Amber N., Doppalapudi, Prithvi K., Orellana, Claudia, Ochoa, Caroline, Patti, Shelby, Ghaffar, Yahya, Cornett, Elyse M., Kaye, Aaron J., Viswanath, Omar, Urits, Ivan, Kaye, Adam M., and Kaye, Alan D.

Subjects
INJECTIONS, PATIENT compliance, ANTIPSYCHOTIC agents, SCHIZOPHRENIA, DISEASE relapse
Abstract

Given the typical age onset of schizophrenia, there are tremendous economic and social impacts that extend beyond the person and their families. One critical determinant of the diseases' impact is the patient's adherence to antipsychotic drug treatment. Approved in 2015 for the treatment of schizophrenia, paliperidone palmitate (Invega Trinza, a 3-month injection, noted as PP3M) is a second-generation long-acting injectable antipsychotic medication. Among the different formulations offered for palmitate paliperidone, including the 1 and 3-month formulations, the longer duration 3-month formulation was better at preventing relapse in schizophrenic patients. To date, different formulations of palmitate paliperidone that have been studied on relapse episodes of schizophrenia include once-daily extended-release oral paliperidone (ORAL paliperidone), once-monthly paliperidone palmitate (PP1M), and once-every-3-months paliperidone palmitate (PP3M). Post-hoc analyses show that patients who were withdrawn from PP1M paliperidone had the least risk of relapse, followed by patients withdrawn from PP3M and patients withdrawn from ORAL paliperidone. PP3M was better at preventing relapse compared to ORAL paliperidone. The results demonstrated that 50% of patients who were withdrawn from ORAL paliperidone, PP1M, or PP3M remained relapse-free for ~2, 6, and 13 months, respectively. Compared to PP1M, PP3M is just as safe and effective and has the added advantage of increased adherence related to a longer dose interval, decreasing the risk of relapse. [ABSTRACT FROM AUTHOR]

Published
2021
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49. Brexanolone, a GABAA Modulator, in the Treatment of Postpartum Depression in Adults: A Comprehensive Review.

Author

Edinoff, Amber N., Odisho, Amira S., Lewis, Kendall, Kaskas, Amir, Hunt, Grace, Cornett, Elyse M., Kaye, Alan D., Kaye, Adam, Morgan, John, Barrilleaux, P. Scott, Lewis, David, Viswanath, Omar, and Urits, Ivan

Subjects
POSTPARTUM depression, MENTAL depression, INTRAVENOUS therapy, DRUG approval, PUERPERIUM
Abstract

Postpartum depression (PPD) is one of the three major categories on the spectrum of postpartum psychiatric syndromes. Postpartum psychiatric syndromes are classified as either postpartum blues, postpartum depression, or postpartum psychosis. Postpartum depression is important to recognize clinically because of the effect it can have on the mother-child bond. The neurosteroid allopregnanolone, a progesterone derivative, is important for its role in positively modulating GABAA receptors. GABA-mediated signaling has been previously implicated in major depressive disorder. Allopregnanolone-mediated signaling has been identified as an important therapeutic target. Treatment with an allopregnanolone-analog, brexanolone, has been shown to improve depression scores in trials for the treatment of PPD. Brexanolone is a positive allosteric modulator of GABAA and is the first drug approved by the FDA to treat postpartum depression. Brexanolone enhances the inhibitory effects of GABAA, restores dysfunctional GABAA transmembrane channels, and mimics a naturally produced progesterone metabolite that fluctuates during pregnancy and postpartum. One open-label study and two phase two studies have some significant reduction in HAM-D scores after treatment and that the effect was still there 30 days post-treatment. Per the data reported, intravenous infusion of brexanolone could be efficacious and safe for the treatment of women suffering from postpartum depression. [ABSTRACT FROM AUTHOR]

Published
2021
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50. Selective Serotonin Reuptake Inhibitors and Clozapine: Clinically Relevant Interactions and Considerations.

Author

Edinoff, Amber N., Fort, Juliana M., Woo, Joshua J., Causey, Christopher D., Burroughs, Caroline R., Cornett, Elyse M., Kaye, Adam M., and Kaye, Alan D.

Subjects
*SEROTONIN uptake inhibitors, *CLOZAPINE, *MENTAL depression, *ANTIPSYCHOTIC agents, *MEDICAL personnel
Abstract

The monoamine hypothesis of depression attributes the symptoms of major depressive disorders to imbalances of serotonin, noradrenaline, and dopamine in the limbic areas of the brain. The preferential targeting of serotonin receptor (SERT) by selective serotonin reuptake inhibitors (SSRIs) has offered an opportunity to reduce the range of these side effects and improve patient adherence to pharmacotherapy. Clozapine remains an effective drug against treatment-resistant schizophrenia, defined as failing treatment with at least two different antipsychotic medications. Patients with schizophrenia who display a constellation of negative symptoms respond poorly to antipsychotic monotherapy. Negative symptoms include the diminution of motivation, interest, or expression. Conversely to the depressive symptomology of interest presently, supplementation of antipsychotics with SSRIs in schizophrenic patients with negative symptoms lead to synergistic improvements in the function of these patients. Fluvoxamine is one of the most potent inhibitors of CYP1A2 and can lead to an increase in clozapine levels. Similar increases in serum clozapine were detected in two patients taking sertraline. However, studies have been contradictory as well, showing no such increases, which are worrying. Clinicians should be aware that clozapine levels should be monitored with any coadministration with SSRIs. [ABSTRACT FROM AUTHOR]

Published
2021
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