937 results
Search Results
2. KEY PAPERS IN GERIATRIC PSYCHIATRY SERIES EDITOR: ALISTAIR BURNS.
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Burns, Alistair and Jacoby, Robin
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GERIATRIC psychiatry , *MENTAL health of older people , *GERIATRIC neuropsychiatry , *DEPRESSION in old age , *ANTIDEPRESSANTS , *CARE of people - Abstract
This article built on previous results of the author's experience in the treatment of elderly people with depression admitted under his care in 1949 and 1951. The article presents a followup investigation of a further consecutive series over the age of 60 receiving care in 1966 and 1967. The progress of 92 depressives over the age of 60 after discharge from hospital was compared with that of 81 subjects of an earlier follow up study. On account mainly of earlier and presumably often successful treatment in the community, the recent sample or hospital patients turned out to be more seriously and persistently ill. In spite of this, long-term results were similar to those obtained during an earlier period, possibly because of more effective aftercare and maintenance therapy with antidepressant drugs, which had in the meantime been introduced.
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- 1996
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3. Paper questions adult antidepressant use.
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ANTIDEPRESSANTS , *PLACEBOS , *DRUGS - Abstract
The article cites a paper on the use of antidepressants by adults, written by Joanna Moncrieff and Irving Kirsch, published in the "British Medical Journal." According to the authors of the paper, prescribing of antidepressants has increased 253 percent over the last ten years. They suggest that review data from the U.S. National Institute for Health and Clinical Excellence indicate that SSRIs show no clinically meaningful advantage over placebo, consistent with some recent metaanalyses. Furthermore, they assert that claims that antidepressants are more effective for treating severe conditions lack supporting evidence.
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- 2005
4. Interventions for adults with mild intellectual disabilities and mental ill-health: a systematic review.
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Osugo, M. and Cooper, S. ‐A.
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ANTIDEPRESSANTS ,MENTAL illness treatment ,MENTAL illness drug therapy ,ANTIPSYCHOTIC agents ,CINAHL database ,ELECTROCONVULSIVE therapy ,EXERCISE ,MEDICAL information storage & retrieval systems ,PSYCHOLOGY information storage & retrieval systems ,MEDLINE ,PEOPLE with intellectual disabilities ,SYSTEMATIC reviews ,TREATMENT effectiveness ,THERAPEUTICS - Abstract
Background People with intellectual disabilities have very high rates of mental ill health. Standard psychosocial interventions designed for the general population may not be accessible for people with mild intellectual disabilities, and drug usage tends to be modified - 'start low and go slow'. This systematic review aims to synthesise the evidence on psychological, pharmacological and electroconvulsive therapy (ECT) interventions for adults with mild intellectual disabilities and mental ill health. Method PRISMA guidelines were followed. Medline, Embase, PsycINFO and CINAHL were searched, as was grey literature and reference lists of selected papers. Papers were selected based on pre-defined inclusion and exclusion criteria. A proportion of papers were double reviewed. Data was extracted using a structured table. Study registration: PROSPERO 2015:CRD42015015218. Results Initially, 18 949 records were identified. Sixteen studies were finally selected for inclusion; seven on psychological therapies, two on group exercise, five on antipsychotics and two on antidepressants. They do not provide definitive evidence for effectiveness of psychosocial interventions, nor address whether starting low and going slow is wise, or causes sub-optimum therapy. Conclusions There are few evidence-based interventions for people with mild intellectual disabilities and mental ill-health; existing literature is limited in quantity and quality. Group cognitive-behavioural therapies have some supporting evidence - however, further randomised control trials are required, with longer-term follow-up, and larger sample sizes. [ABSTRACT FROM AUTHOR]
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- 2016
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5. Psilocybin‐assisted psychotherapy for treatment‐resistant depression: Which psychotherapy?
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Crowe, Marie, Manuel, Jenni, Carlyle, Dave, and Lacey, Cameron
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ANTIDEPRESSANTS , *BRIEF psychotherapy , *INTERPERSONAL psychotherapy , *SOCIAL support , *DRUG resistance , *TREATMENT effectiveness , *MENTAL depression , *PSYCHOTHERAPY , *HALLUCINOGENIC drugs , *COGNITIVE therapy - Abstract
This perspective paper explores the choice of psychotherapy for psilocybin‐assisted psychotherapy for treatment‐resistant depression. There is evidence to support the use of some psychotherapies in treating 'treatment‐resistant' depression, and emerging evidence for the efficacy of psilocybin. The next step which is the focus of this paper is to identify psychotherapies that are both effective and congruent with the psilocybin experience. The evidence for the efficacy of the psychotherapies is drawn from a Cochrane review and the analysis of their congruence with the psilocybin experience is drawn from a qualitative meta‐synthesis of the experience of psilocybin. The paper will examine whether three one‐to‐one psychotherapies identified as effective in the treatment of treatment‐resistant depression are compatible with the psilocybin experience. Each psychotherapy will be examined in relation to its congruence with the qualitative evidence that suggests the choice of psychotherapy needs to give priority to the subjective experience, facilitate emotional processing, support connectedness with others, acceptance of the self as emotional and support change based on the person's insights into their relationships with others and the world in which they live. We conclude that interpersonal psychotherapy and intensive short‐term dynamic psychotherapy align with that experience, although others are currently being trialled. [ABSTRACT FROM AUTHOR]
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- 2023
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6. Selective serotonin reuptake inhibitors, post‐treatment sexual dysfunction and persistent genital arousal disorder: A systematic review.
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Tarchi, Livio, Merola, Giuseppe Pierpaolo, Baccaredda‐Boy, Ottone, Arganini, Francesca, Cassioli, Emanuele, Rossi, Eleonora, Maggi, Mario, Baldwin, David S., Ricca, Valdo, and Castellini, Giovanni
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Purpose: Adverse effects of selective serotonin reuptake inhibitors (SSRIs) on sexual function have been an important area of research for many years. However, the duration of SSRI‐associated sexual adverse effects, and their possible persistence after treatment discontinuation, is still uncertain. The aims of the current systematic review were first to identify existing evidence of sexual dysfunction following SSRI discontinuation, and to provide an account of reported symptoms and proposed treatment options; and second, to establish whether current literature allows accurate estimates of the prevalence of such sexual dysfunction. Methods: A systematic review was conducted on PubMed, Embase, and Google Scholar; papers with clinical data regarding patients with persistent sexual dysfunction after SSRI treatment suspension were included. Results: Overall, two retrospective interventional studies, six observational studies and 11 case reports were judged eligible for inclusion. It was not possible to determine reliable estimates of prevalence. Similarly, a cause‐effect relationship between SSRI exposure and persistent sexual impairment could not be ascertained. Nonetheless, the potential for continued sexual disturbances despite discontinuation could not be entirely ruled out. Conclusions: There is a need to investigate a possible dose–response relationship between SSRI exposure and persistent sexual adverse effects. Treatment options for persistent dysfunctions remain limited, but novel therapeutic approaches may be required in order to address an otherwise neglected need for sexual well‐being. [ABSTRACT FROM AUTHOR]
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- 2023
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7. The discursive transformation of grief throughout history.
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Gravesen, Janni Dahlgaard and Birkelund, Regner
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GRIEF ,ANTIDEPRESSANTS ,NOSOLOGY ,LANGUAGE & languages ,DISCOURSE analysis ,PHILOSOPHY ,PSYCHOLOGICAL adaptation ,MENTAL illness ,BEREAVEMENT ,REFLECTION (Philosophy) - Abstract
In recent decades, the phenomenon of grief, when you lose a loved one, has been the subject of exploration and discussion among researchers. Because of this, prolonged grief is now recognized as a possible mental disorder as the latest version of the diagnosis manual; 'International Classification of Diseases' (ICD‐11) being published in 2018 is featuring a new diagnosis called 'prolonged grief disorder'. The commencement of this new disorder indicates a shift in the way grief is being articulated why the notion of rupture from the French philosopher Michel Foucault is applied as a philosophical approach in this paper. A Foucault‐inspired discourse analysis has been prepared and by considering the issue historically and tracing how the concept of grief has been articulated in different time periods throughout history, the aim is to map out the discursive transformation that has taken place and to gain insight into how the societal context has supported and enabled this transformation. This paper takes a historical look back from the 1800s to present and identifies when changes can be observed in the way grief is being articulated. These changes or ruptures are identified in the work of Søren Aabye Kierkegaard, Sigmund Freud and Margaret Stroebe & Henk Schut who all must be assumed to have contributed significantly to how grief is perceived in various historical time periods. The discourse analysis identifies how prominent thinkers have articulated grief in each period and how today's perception of grief, as a possible mental disorder, both relates to these prominent thinkers but also reflects dominant societal values and ideologies. [ABSTRACT FROM AUTHOR]
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- 2021
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8. Issue highlights.
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BEHAVIORAL sciences ,PHARMACOLOGY ,SEROTONIN uptake inhibitors ,DRUG development ,ANTIDEPRESSANTS - Abstract
Figures from the Editors selected issue highlights will be displayed each month in the journal image carousel on the BJCP homepage http://bpspubs.onlinelibrary.wiley.com/hub/journal/10.1111/(ISSN)1365-2125/. Treatment regimens for tuberculosis are lengthy and require a high number of combination drugs and unfortunately antitubercular drug development to date has not been very successful. In their paper, Morris Muliaditan M. and Oscar della Pasqua (London, UK), showed that drug-disease modelling may provide rationale for dose selection and companion drugs to treat tuberculosis. [Extracted from the article]
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- 2021
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9. Baseline data of a sequential multiple assignment randomized trial (STEP study).
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Hartmann, Jessica A., Nelson, Barnaby, Amminger, Günther Paul, Spark, Jessica, Yuen, Hok Pan, Kerr, Melissa J., Polari, Andrea, Wallis, Nicky, Blasioli, Julie, Dixon, Lisa, Carter, Cameron, Loewy, Rachel, Niendam, Tara A., Shumway, Martha, and McGorry, Patrick D.
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YOUNG adults ,OMEGA-3 fatty acids ,ANTIDEPRESSANTS ,MENTAL illness ,ANTIPSYCHOTIC agents - Abstract
Aim: Research has shown that preventative intervention in individuals at ultra‐high risk of psychosis (UHR) improves symptomatic and functional outcomes. The staged treatment in early psychosis (STEP) trial aims to determine the most effective type, timing and sequence of interventions in the UHR population by sequentially studying the effectiveness of (1) support and problem solving, (2) cognitive‐behavioural case management and (3) antidepressant medication with an embedded fast‐fail option of (4) omega‐3 fatty acids or low‐dose antipsychotic medication. This paper presents the recruitment flow and baseline clinical characteristics of the sample. Methods: STEP is a sequential multiple assignment randomized trial. We present the baseline demographics, clinical characteristics and acceptability and feasibility of this treatment approach as indicated by the flow of participants from first contact up until enrolment into the trial. Recruitment took place between April 2016 and January 2019. Results: Of 1343, help‐seeking young people who were considered for participation, 402 participants were not eligible and 599 declined/disengaged, resulting in a total of 342 participants enrolled in the study. The most common reason for exclusion was an active prescription of antidepressant medication. Eighty‐five percent of the enrolled sample had a non‐psychotic DSM‐5 diagnosis and symptomatic/functional measures showed a moderate level of clinical severity and functional impairment. Discussion: The present study demonstrates the acceptability and participant's general positive appraisal of sequential treatment. It also shows, in line with other trials in UHR individuals, a significant level of psychiatric morbidity and impairment, demonstrating the clear need for care in this group and that treatment is appropriate. [ABSTRACT FROM AUTHOR]
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- 2022
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10. Recent advances in synthesis of quinazoline‐2,4(1H,3H)‐diones: Versatile building blocks in N‐heterocyclic compounds.
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Gheidari, Davood, Mehrdad, Morteza, and Maleki, Saloomeh
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HETEROGENEOUS catalysts ,PHARMACEUTICAL chemistry ,ORGANIC chemistry ,CHEMISTS ,ANTIDEPRESSANTS ,ANTIMALARIALS - Abstract
Quinazoline‐2,4(1H,3H)‐dione is a significant class of N‐fused heterocyclic with a wide range of biological functions, including anti‐HIV, anticancer, antifungal, antibacterial, antimutagenic, anticoccidial, anticonvulsant, anti‐inflammatory, antidepressant, antimalarial, antioxidant, antileukemic, and antileishmanial activities, and other activities, and has attracted great attention in organic and medicinal chemistry. As a result, all chemists and pharmaceutical chemists must be aware of many methods to make quinazoline‐2,4(1H,3H)‐dione. This review paper focuses on various methods for producing quinazoline‐2,4(1H,3H)‐diones, such as green methods and homogeneous or heterogeneous catalysts from various precursors under varied conditions. [ABSTRACT FROM AUTHOR]
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- 2022
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11. Effects of central nervous system drugs on driving: speed variability versus standard deviation of lateral position as outcome measure of the on-the-road driving test.
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Verster, Joris C. and Roth, Thomas
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AUTOMOBILE drivers' tests ,CENTRAL nervous system depressants ,CENTRAL nervous system stimulants ,DISABILITIES ,AUTOMOBILE driving ,TRANQUILIZING drugs ,ANTIDEPRESSANTS ,ANTIHISTAMINES - Abstract
Background The on-the-road driving test in normal traffic is used to examine the impact of drugs on driving performance. This paper compares the sensitivity of standard deviation of lateral position (SDLP) and SD speed in detecting driving impairment. Methods A literature search was conducted to identify studies applying the on-the-road driving test, examining the effects of anxiolytics, antidepressants, antihistamines, and hypnotics. The proportion of comparisons (treatment versus placebo) where a significant impairment was detected with SDLP and SD speed was compared. Results About 40% of 53 relevant papers did not report data on SD speed and/or SDLP. After placebo administration, the correlation between SDLP and SD speed was significant but did not explain much variance ( r = 0.253, p = 0.0001). A significant correlation was found between ΔSDLP and ΔSD speed (treatment-placebo), explaining 48% of variance. When using SDLP as outcome measure, 67 significant treatment-placebo comparisons were found. Only 17 (25.4%) were significant when SD speed was used as outcome measure. Alternatively, for five treatment-placebo comparisons, a significant difference was found for SD speed but not for SDLP. Conclusions Standard deviation of lateral position is a more sensitive outcome measure to detect driving impairment than speed variability. Copyright © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]
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- 2014
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12. Pharmacological Treatment of Pain in Cancer Patients: The Role of Adjuvant Analgesics, a Systematic Review.
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Beuken ‐ van Everdingen, Marieke H.J., Graeff, Alexander, Jongen, Joost L.M., Dijkstra, Denise, Mostovaya, Irina, and Vissers, Kris C.
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PAIN management ,ANALGESICS ,ANTIDEPRESSANTS ,CANCER patients ,SYSTEMATIC reviews - Abstract
Context In patients with cancer, pain is one of the most feared and burdensome symptoms. Adjuvant analgesics are an important cornerstone on which treatment of pain in patients with cancer is based. Objectives To update our guidelines for the treatment of pain in patients with cancer, we performed a systematic review on the use of adjuvant analgesics in pain in cancer. Methods A systematic search of the literature was performed searching for articles that studied the effect of (1) antidepressants, (2) anti-epileptics, (3) N-methyl- d-aspartate ( NMDA) receptor antagonists, and (4) other adjuvant analgesics in patients with cancer pain and described their effects on pain intensity and/or side effects. Results Based on the keywords and after reading the full papers, we could include 12 papers on anticonvulsants, 10 papers on antidepressants, four on NMDA receptor antagonists, and 10 papers on other adjuvant analgesics. The methodological quality of the included papers was graded as low to very low. Overall, there was a low quality of evidence that gabapentin, pregabalin, amitriptyline, and venlafaxine were effective in reducing pain intensity in patients with cancer pain. There was insufficient evidence on the effectiveness of lamotrigine, levetiracetam, NMDA antagonists, cannabinoids, corticosteroids, and local anesthetics on reducing pain intensity in patients with cancer pain. Conclusion The quality of currently available evidence on the effectiveness of adjuvant analgesics in the treatment of cancer pain is low. The treatment of pain associated with cancer should be tailored to the patient's personal preferences. [ABSTRACT FROM AUTHOR]
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- 2017
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13. For veterans with comorbid disorders, more care may mean it's less adequate.
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Enos, Gary
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SUBSTANCE abuse treatment ,ANTIDEPRESSANTS ,MENTAL depression ,HEALTH services accessibility ,MEDICAL quality control ,MEDICAL protocols ,PSYCHOTHERAPY ,QUALITY assurance ,PSYCHOLOGY of veterans ,COMORBIDITY ,PSYCHIATRIC treatment - Abstract
Two recent research papers highlight ongoing deficiencies in the provision of addiction and mental health treatment services to veterans, though the report focusing on depression treatment for patients with substance use disorders (SUDs) suggests that shortcomings in treatment for co‐occurring disorders affect all populations. [ABSTRACT FROM AUTHOR]
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- 2020
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14. Capillary electrophoresis for the analysis of antidepressant drugs: A review.
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Abdul Keyon, Aemi Syazwani, Miskam, Mazidatulakmam, Ishak, Nur Syazwani, Mahat, Naji Arafat, Mohamed Huri, Mohamad Afiq, Abdul Wahab, Roswanira, Chandren, Sheela, Abdul Razak, Fazira Ilyana, Ng, Nyuk‐Ting, and Ali, Timothy Gandu
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CAPILLARY electrophoresis ,ANTIDEPRESSANTS ,MENTAL depression ,NEUROTRANSMITTERS ,METABOLITES - Abstract
Depression is a common mental disorder that may lead to major mental health problems, and antidepressant drugs have been used as a treatment of choice to mitigate symptoms of major depressive disorders by ameliorating the chemical imbalances of neurotransmitters in brain. Since abusing antidepressant drugs such as selective serotonin reuptake inhibitors and tricyclic antidepressant drugs can cause severe adverse effects, continuous toxicological monitoring of the parent compounds as well as their metabolites using numerous analytical methods appears pertinent. Among them, capillary electrophoresis has been popularly utilized since the method has a lot of advantages viz. using small amounts of sample and solvents, ease of operation, and rapid analysis. This review paper brings a survey of more than 30 papers on capillary electrophoresis of antidepressant drugs published approximately from 1999 until 2018. It focuses on the reported capillary electrophoresis techniques and their applications and challenges for determining antidepressant drugs and their metabolites. It is organized according to the commonly used capillary zone electrophoresis method, followed by non‐aqueous capillary electrophoresis and micellar electrokinetic chromatography, with details on breakthrough findings. Where available, information is given about the background electrolyte used, detector utilized, and sensitivity obtained. [ABSTRACT FROM AUTHOR]
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- 2019
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15. DSM-5 criteria for depression with mixed features: a farewell to mixed depression.
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Koukopoulos, A. and Sani, G.
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MENTAL depression ,AFFECTIVE disorders ,BIPOLAR disorder ,ANTIDEPRESSANTS ,SYSTEMATIC reviews - Abstract
Objective To review the DSM-5 proposed criteria for mixed depression in light of robust and consistent historical and scientific evidence. Method An extensive historical search, a systematic review of the papers used by DSM-5 as reference papers, and a PubMed search were performed. Results As Hippocrates, depressive mixed states have been described as conditions of intense psychic suffering, consisting of depressed mood, inner tension, restlessness, and aimless psychomotor agitation. In DSM-5, new criteria are proposed for a mixed features specifier, as part of depression either in major depressive disorder ( MDD) or bipolar disorder. Those criteria require, as diagnostically specific, manic/hypomanic symptoms that are the least common kinds of symptoms that actually arise in depressive mixed states. The DSM-5 proposal is based, almost entirely, on a speculative wish to avoid 'overlapping' manic and depressive symptoms. Mixed states are, in fact, nothing but overlapping manic and depressive symptoms. Conclusion In this article, we review the psychopathology and research on mixed depressive states, and try to demonstrate that the DSM-5 proposal has weak scientific basis and does not identify a large number of mixed depressive states. This may be harmful because of the different treatment required by these conditions. [ABSTRACT FROM AUTHOR]
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- 2014
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16. Misinformed, misconducted, misguided and misrepresented meta‐analyses. The use of antidepressants (AD) in major depressive disorders (MDD).
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Vinberg, Maj
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MENTAL depression ,ANTIDEPRESSANTS ,SEROTONIN uptake inhibitors - Abstract
The use of antidepressants (AD) in major depressive disorders (MDD) Keywords: antidepressants; depression; meta-analyses EN antidepressants depression meta-analyses 862 863 2 12/29/20 20201201 NES 201201 The often mud-throwing long-standing debate on the use of antidepressant was rebooted by a meta-analyses1 from a Danish group in 2017. In that paper, the authors successfully distorted the overall primary outcome (that selective serotonin reuptake inhibitors (SSRI) had a statistically significant effect in comparison with placebo). [Extracted from the article]
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- 2020
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17. Synergistic anti‐depressive effect of combination treatment of Brexpiprazole and selective serotonin reuptake inhibitors on forced swimming test in mice.
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Amada, Naoki, Hirose, Tsuyoshi, Suzuki, Mikio, Kakumoto, Yusuke, Futamura, Takashi, Maeda, Kenji, and Kikuchi, Tetsuro
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SEROTONIN uptake inhibitors ,ANTIDEPRESSANTS ,MENTAL depression ,OBSESSIVE-compulsive disorder ,SWIMMING ,SOCIAL anxiety - Abstract
Aim: Selective serotonin reuptake inhibitors (SSRIs) are used to treat major depressive disorder (MDD) and other psychiatric disorders (e.g., obsessive compulsive disorder, social anxiety disorder, and panic disorder). In MDD treatment, SSRIs do not show remission in approximately 30% of patients, indicating a need for a better treatment option. Forced swimming test (FST) is a behavioral assay to evaluate depression‐like behavior and antidepressant efficacy in rodents. In the present study, we evaluated the combination effect of brexpiprazole with SSRIs on FST in mice, in order to investigate their synergistic effect. Methods: Brexpiprazole (0.003 mg/kg) was intraperitoneally injected to mice 15 min before testing. Escitalopram (10 mg/kg), fluoxetine (75 mg/kg), paroxetine (10 mg/kg), or sertraline (15 mg/kg) were orally administered to mice 60 min before testing. Then, the mice were placed in water and immobility time was measured. Data from animals treated with escitalopram, fluoxetine, paroxetine, and sertraline were pooled as SSRI‐treated group data. Results: Combination treatment of brexpiprazole with SSRIs reduced immobility time in FST more than vehicle or each single treatment. A significant interaction effect was confirmed in the combination of brexpiprazole and SSRIs (p = 0.0411). Conclusion: Efficacy of adjunctive brexpiprazole has already been demonstrated in clinical trials in MDD patients not adequately responding to antidepressants including escitalopram, fluoxetine, paroxetine, and sertraline. The synergistic antidepressant‐like effect of brexpiprazole with SSRIs found in this study supports the already known clinical findings. [ABSTRACT FROM AUTHOR]
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- 2023
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18. The impact of lithium on bipolar disorder.
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Malhi, Gin S.
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BIPOLAR disorder ,ANTIDEPRESSANTS - Abstract
An introduction to the journal is presented in which the editor discusses the article on the key aspects of lithium in the clinical practice by Doctor Shorter, the research findings on the use of anticonvulsants in bipolar disorder by Bowden, and the psychosocial treatments in the management of bipolar disorder by Miklowitz and Scott.
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- 2009
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19. Is Placebo Response Responsible for Many Phase III Failures?
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Dumitrescu, Teodora Pene, McCune, Jeanine, and Schmith, Virginia
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PHARMACOGENOMICS ,NOCEBOS ,ANTIDEPRESSANTS ,PLACEBOS ,PERIAQUEDUCTAL gray matter - Abstract
The "gold standard" for demonstrating effectiveness of investigational drugs is through randomized, double-blinded, placebo-controlled (R-DB-PC) trials. This assertion is further supported by meta-analyses of antidepressant trials suggesting that high placebo response rather than low medication response explains most of the variability in drug-placebo differences.[3] Recent summaries of placebo and treatment effects for successful drugs in depression[5] and attention deficit hyperactivity disorder[6] have suggested that drug effects also increased over time. Placebome data described in the paper by Hall and Loscalzo[23] further support that the effects of placebo and active drugs are not additive, the tenant of our R-DB-PC trials. [Extracted from the article]
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- 2019
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20. Diagnosing latent bipolar disorder: A clinical dilemma.
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Gitlin, Michael J.
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BIPOLAR disorder ,MOOD stabilizers ,MENTAL depression ,META-analysis ,ANTIDEPRESSANTS ,PATIENTS - Abstract
Within the bipolar world, there is a chronic gnashing of teeth among experts, decrying clinicians' poor ability to diagnose bipolar disorder early in the course of the disorder. The feared consequence of this delayed diagnosis is risking a greater number of episodes early in adult life and increasing the likelihood of prescriptions of antide-pressants without mood stabilizers with their attendant risks when taken by those diagnosed as having unipolar depression but who are latently bipolar. These papers typically point to the long time frame from initial depressive symptoms to the proper bipolar diagnosis, usually measured in many years if not a decade or more. Clinicians are then usually urged to be more vigilant in ferreting out subtle hypomanic symptoms and looking for predictors of bipolar outcome. The treatment implication of making this earlier, accurate diagnosis of bipolar disorder would be to institute mood stabilizers and (presumably) to avoid antidepressants. Of course, in order to follow these recommendations, predictors of bipolar outcome among depressed patients must be established and validated across studies. [ABSTRACT FROM AUTHOR]
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- 2018
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21. An Eco‐friendly Pencil Graphite Sensor for Voltammetric Analysis of the Antidepressant Vilazodone Hydrochloride.
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Hussien, Emad M., Rizk, Mohamed S., Daoud, Amira M., and El‐Eryan, Rasha Th.
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ELECTRODE performance ,ELECTROCHEMICAL electrodes ,SQUARE waves ,PENCILS ,ANTIDEPRESSANTS - Abstract
A simple, eco‐friendly, accurate and inexpensive pencil graphite electrode (PGE) was utilized for the quantitative determination of Vilazodone hydrochloride (VLZ) by Square wave voltammetric (SWV) method. Optimum electrochemical performance of the electrode was achieved by optimizing the pH of the measuring solution, the rate of potential scan and the time of accumulation onto the electrode surface. The SWV showed linearity over the concentration range of 9.99×10−9 to 9.78×10−7 M, with LOD of 6.4×10−9 M. This method was applied to evaluate VLZ in pharmaceutical preparation and spiked plasma with %recovery± RSD of 99.99±0.41 and 99.40±1.36, respectively. [ABSTRACT FROM AUTHOR]
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- 2022
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22. Editorial: The rise and rise of developmental perspectives in child psychology and psychiatry.
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Jaffee, Sara R.
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ANTIDEPRESSANTS ,TREATMENT of behavior disorders in children ,RISK factors of attention-deficit hyperactivity disorder ,AUTISM risk factors ,ATTENTION-deficit hyperactivity disorder ,BEHAVIOR disorders in children ,CHILD development deviations ,CHILD psychiatry ,CHILD psychology ,MENTAL depression ,PATHOLOGICAL psychology ,SERIAL publications ,DIAGNOSIS - Abstract
When developmental psychopathology emerged as a discipline in the late 1970s and early 1980s, its proponents were as careful to explain what it was not, as they were to define what it was (e.g. Sroufe & Rutter, 1984). In particular, they differentiated developmental psychopathology from child psychiatry, which is primarily concerned with the differential diagnosis, prognosis, and treatment of childhood disorders. In contrast, developmental psychopathology was defined as 'the study of the origins and course of individual patterns of behavioral maladaptation, whatever the age of onset, whatever the causes, whatever the transformations in behavioral manifestation, and however complex the course of the developmental pattern may be' (Sroufe & Rutter, 1984, p. 18). [ABSTRACT FROM AUTHOR]
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- 2019
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23. Piperazine derivatives with central pharmacological activity used as therapeutic tools.
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Brito, Adriane F., Moreira, Lorrane K. S., Menegatti, Ricardo, and Costa, Elson A.
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PIPERAZINE ,MONOAMINE oxidase ,ANTIDEPRESSANTS ,NEUROTRANSMITTERS ,CLOZAPINE ,BENZYLPIPERAZINE - Abstract
Medicinal chemistry is a science applied to the search and discovery of new therapeutic agents for the treatment of various diseases. Therefore, promising structures have been identified; one of these structures is the piperazine moiety, a cyclic molecule containing two nitrogen atoms in positions 1 and 4 as well as four carbon atoms. Many piperazine derivatives have central pharmacological activity that mainly involves the activation of the monoamine pathway. Thus, piperazine derivatives have been the subject of research for many central therapeutic applications, including antipsychotic, antidepressant and anxiolytic applications. Benzylpiperazine is the prototype of piperazine derivatives; this substance is the main component of recreational drugs, partly due to its stimulant and euphoric effects. This paper describes some piperazine derivatives used therapeutically as antipsychotic (clozapine), antidepressant (vortioxetine) and anxiolytic (buspirone) drugs. [ABSTRACT FROM AUTHOR]
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- 2019
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24. Pharmacologic Prevention of Migraine: A Narrative Review of the State of the Art in 2018.
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Loder, Elizabeth and Rizzoli, Paul
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MIGRAINE prevention ,ANTICONVULSANTS ,ANTIDEPRESSANTS ,ANTIHYPERTENSIVE agents ,MIGRAINE ,OFF-label use (Drugs) ,PATIENTS' attitudes - Abstract
This paper describes current non‐antibody pharmacologic approaches to the prevention of migraine in adults. Preventive therapy should be considered for patients with migraine who routinely have more than 6 headache days per month or in other special circumstances. Choices for preventive therapy are based on patient preferences about side effects and evidence of efficacy. The evidence level and commonly used doses for selected categories of migraine preventive medication are reviewed, including antiepileptic drugs, antihypertensive drugs, and antidepressants. Propranolol, timolol, topiramate, and divalproex sodium are approved for migraine prevention by the US FDA. OnabotulinumtoxinA is approved for prevention of chronic migraine. Several off‐label drugs, especially lisinopril, candesartan, and amitriptyline also have good evidence of benefit. The spectrum of response to preventive therapy varies; in general, complete cessation of headaches is uncommon, although there are "super‐responders" to every therapy, as illustrated by patient reports of dramatic responses to treatment. Preventive treatment should be started at a low dose and doses increased slowly until therapeutic benefit is achieved or side effects preclude continued use. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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25. Flawed reviews of pediatric depression studies underestimate medication effects.
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ANTIDEPRESSANTS ,MENTAL depression ,CHILDREN'S health ,RESEARCH methodology ,META-analysis ,ADOLESCENT health ,EVIDENCE-based medicine ,STANDARDS - Abstract
Previous reviews of antidepressant treatment for children and adolescents that found minimal or no positive effects failed to account for critical methodological differences in studies, a new review concludes. The author of the review, published March 3 in the American Journal of Psychiatry, states that earlier reviews have drawn questionable conclusions because they categorized many flawed pharmaceutical industry-sponsored trials that found no benefits from antidepressants as negative trials, rather than as failed trials. Accounting for this distinction leads the author of the present paper to conclude that evidence for beneficial effects of antidepressants in children and adolescents is actually strong. [ABSTRACT FROM AUTHOR]
- Published
- 2017
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26. Staged Treatment in Early Psychosis: A sequential multiple assignment randomised trial of interventions for ultra high risk of psychosis patients.
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Nelson, Barnaby, Amminger, G. Paul, Yuen, Hok Pan, Wallis, Nicky, J. Kerr, Melissa, Dixon, Lisa, Carter, Cameron, Loewy, Rachel, Niendam, Tara A., Shumway, Martha, Morris, Sarah, Blasioli, Julie, and Mcgorry, Patrick D.
- Subjects
PSYCHOSES ,PSYCHOSES risk factors ,ANTIDEPRESSANTS ,PSYCHOTIC depression ,COGNITIVE therapy ,OXIDATIVE stress ,PATIENTS ,THERAPEUTICS - Abstract
Aim: Previous research indicates that preventive intervention is likely to benefit patients “at risk” of psychosis, in terms of functional improvement, symptom reduction and delay or prevention of onset of threshold psychotic disorder. The primary aim of the current study is to test outcomes of ultra high risk (UHR) patients, primarily functional outcome, in response to a sequential intervention strategy consisting of support and problem solving (SPS), cognitive‐behavioural case management and antidepressant medication. A secondary aim is to test biological and psychological variables that moderate and mediate response to this sequential treatment strategy. Methods: This is a sequential multiple assignment randomised trial (SMART) consisting of three steps: Step 1: SPS (1.5 months); Step 2: SPS vs Cognitive Behavioural Case Management (4.5 months); Step 3: Cognitive Behavioural Case Management + Antidepressant Medication vs Cognitive Behavioural Case Management + Placebo (6 months). The intervention is of 12 months duration in total and participants will be followed up at 18 months and 24 months post baseline. Conclusion: This paper reports on the rationale and protocol of the Staged Treatment in Early Psychosis (STEP) study. With a large sample of 500 UHR participants this study will investigate the most effective type and sequence of treatments for improving functioning and reducing the risk of developing psychotic disorder in this clinical population. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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27. Association between antidepressant medication use and epithelial ovarian cancer risk: a systematic review and meta‐analysis of observational studies.
- Author
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Huo, Yun‐Long, Qiao, Jia‐Ming, and Gao, Song
- Subjects
OVARIAN epithelial cancer ,ANTIDEPRESSANTS ,SEROTONIN uptake inhibitors ,CONFIDENCE intervals ,ODDS ratio ,CANCER treatment - Abstract
Aim: The aim of this paper is to clarify the inconsistent findings in the association between antidepressant use and the risk of epithelial ovarian cancer (EOC). Methods: This study is a meta‐analysis of observational studies retrieved from the PubMed, EMBASE, and Web of Science databases prior to August 15, 2017. Two researchers independently screened studies and extracted study characteristics and risk estimates. The odds ratios (OR) and 95% confidence intervals (CI) of EOC risk were summarized using an inverse variance weighted random‐effects model. Heterogeneity between studies was assessed with the I
2 statistic. Results: Eight case–control studies involving 7878 EOC cases and 73 913 controls were identified. Compared with non‐use, use of antidepressants was not significantly associated with EOC risk (summarized OR = 1.10, 95% CI: 0.91–1.32, I2 = 74.4%). Similar null results were also observed in the use of selective serotonin reuptake inhibitors (OR = 1.04, 95% CI = 0.80–1.35), tricyclic antidepressants (OR = 1.01, 95% CI = 0.79–1.30), and other antidepressant drugs (OR = 0.91, 95% CI = 0.74–1.12). Subgroup analyses of study characteristics, stratified by the type of control subjects, geographic location, exposure assessment, number of cases, and adjustment for potential confounders, showed that the ORs were broadly consistent across strata. The OR per 1 year‐increment of duration was 0.99 (95% CI = 0.94–1.05, I2 = 40.0%, P = 0.154). Additionally, the OR for the greatest intensity of antidepressant use compared with never use was 0.82 (95% CI = 0.70–0.98, I2 = 0%, P = 0.489). Furthermore, no evidence of publication bias was detected through Funnel plots as well as Egger's and Begg's tests. Conclusions: There is no association between antidepressant use and EOC risk. Further prospective studies are warranted to confirm these findings. [ABSTRACT FROM AUTHOR]- Published
- 2018
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28. A case study in identifying targeted patients population in major depressive disorder by enhanced enrichment design.
- Author
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Zhang, Peter, Carroll, Kevin, Hobart, Mary, Augustine, Carole, and Koch, Gary
- Subjects
ANTIDEPRESSANTS ,DRUG development ,CLINICAL trials ,PATIENT selection - Abstract
Despite advances in clinical trial design, failure rates near 80% in phase 2 and 50% in phase 3 have recently been reported. The challenges to successful drug development are particularly acute in central nervous system trials such as for pain, schizophrenia, mania, and depression because high‐placebo response rates lessen assay sensitivity, diminish estimated treatment effect sizes, and thereby decrease statistical power. This paper addresses the importance of rigorous patient selection in major depressive disorder trials through an enhanced enrichment paradigm. This approach led to a redefinition of an ongoing, blinded phase 3 trial algorithm for patient inclusion (1) to eliminate further randomization of transient placebo responders and (2) to exclude previously randomized transient responders from the primary analysis of the double blind phase of the trial. It is illustrated for a case study for the comparison between brexpiprazole + antidepressant therapy and placebo + antidepressant therapy. Analysis of the primary endpoint showed that efficacy of brexpiprazole versus placebo could not be established statistically if the original algorithm for identification of placebo responders was used, but the enhanced enrichment approach did statistically demonstrate efficacy. Additionally, the enhanced enrichment approach identified a target population with a clinically meaningful treatment effect. Through its successful identification of a target population, the innovative enhanced enrichment approach enabled the demonstration of a positive treatment effect in a very challenging area of depression research. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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- View/download PDF
29. Effectiveness of interpersonal psychotherapy in comparison to other psychological and pharmacological interventions for reducing depressive symptoms in women diagnosed with postpartum depression in low‐ and middle‐income countries: A systematic review
- Author
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Kang, Harmeet Kaur, Bisht, Bandana, Kaur, Manmeet, Alexis, Obrey, Worsley, Aaron, and John, Denny
- Subjects
PSYCHOTHERAPY ,MIDDLE-income countries ,MEDICAL information storage & retrieval systems ,LIFE change events ,INTERPERSONAL psychotherapy ,DRUG side effects ,SUICIDAL ideation ,CINAHL database ,POSTPARTUM depression ,TREATMENT effectiveness ,META-analysis ,DESCRIPTIVE statistics ,GROUP psychotherapy ,TREATMENT duration ,LONELINESS ,FAMILY relations ,SEVERITY of illness index ,ANTIDEPRESSANTS ,SYSTEMATIC reviews ,MEDLINE ,ODDS ratio ,TELEPSYCHOLOGY ,COMBINED modality therapy ,PSYCHOLOGY of mothers ,MEDICAL databases ,WOMEN'S health ,ONLINE information services ,CONFIDENCE intervals ,GRIEF ,PATIENT satisfaction ,LOW-income countries ,PSYCHOLOGY information storage & retrieval systems ,SOCIAL isolation - Abstract
Background: Postpartum depression (PPD) is a condition that can affect any woman regardless of ethnicity, age, party, marital status, income, and type of delivery. This condition is highly prevalent worldwide. PPD, if not treated timely, can affect the maternal‐child bond and can have a detrimental impact on the future cognitive, emotional, and behavioral development of the child. Interpersonal psychotherapy (IPT) has been reported as an effective treatment of PPD in previous studies as this focuses on relationship and social support issues. Previous reviews conducted in developed nations have reported the superior efficacy of IPT in comparison to other treatment options. There is no systematic review conducted in low to middle‐income countries on the efficacy of IPT on PPD. Therefore it was necessary to undertake a systematic review to assess the effectiveness of IPT in reducing the depression among postpartum women in low and middle‐income countries (LMICs). Objectives: The main aim of this systematic review was to assess the effectiveness of IPT alone or in conjunction with pharmacological therapy and/or other psychological and psychosocial interventions, in reducing depressive symptoms among women diagnosed with PPD residing in LMICs. Search Methods: The systematic search encompassed several prominent databases and grey literature. Furthermore, experts specializing in the field of IPT were consulted to identify any relevant studies conducted in LMICs that fulfilled the predetermined eligibility criteria. The most recent search update was performed in July 2022. Selection Criteria: The PICOS criteria were meticulously defined for this review as described. Participants: Postpartum women diagnosed with PPD in LMICs were included. Intervention: IPT either as a standalone treatment or in conjunction with pharmacological therapy was included. Comparison: any form of psychological therapy or pharmacological therapy, whether administered individually or in combination, was considered for comparison. Study designs: experimental and quasi‐experimental, factorial designs, and quantitative components (experimental, quasi‐experimental, factorial designs) of mixed methods designs were eligible to be included. Studies with single‐group study designs and qualitative studies were excluded from the review. Data Collection and Analysis: Two reviewers from our team conducted a rigorous screening process to determine the eligibility of articles for inclusion. This involved an initial evaluation of titles and abstracts, followed by a comprehensive assessment of the full text of selected articles. In instances where discrepancies arose between the two reviewers, resolution was achieved through discussion or consultation with a third author to establish a consensus. Following the screening process, two team members independently extracted pertinent information and data from the studies that met the inclusion criteria. The treatment effect of the intervention, in comparison to the control group, was subsequently analyzed utilizing the fixed effects model taking into account the small number of studies. Main Results: A total of 17,588 studies were identified from various databases, and 6493 duplicate studies were removed. Subsequently, 9380 studies underwent independent title and abstract screening resulting in the exclusion of 9040 studies. 345 full texts were thoroughly assessed leading to the exclusion of 341 studies, finally including 4 studies for review. The four included trials were randomized trials and comprised a total sample size of 188 women diagnosed with PPD residing in LMICs. Among these studies, three compared IPT with usual treatment, while one study compared IPT with antidepressant medications (ADMs). In terms of the providers of IPT, in one study, IPT was administered by nurses, while psychologists delivered IPT in another study. In one study, community health workers were responsible for providing IPT. However, in one study, information regarding the specific providers of IPT was not available or reported. The primary outcome measure reported in all four studies was depression, assessed using the Edinburgh Postnatal Depression Scale (EPDS). The geographical distribution of the studies included; one conducted in Zambia, one in Kenya, one in Pakistan, and one in Iran. Out of the four studies, three were included in the meta‐analysis, as missing data from one study could not be obtained. Based on the overall treatment effect, it was found that depression scores decreased significantly more in the IPT group compared to other interventions (usual treatment or ADMs) (standardized mean difference [SMD] −0.62, 95% confidence interval [CI] (−1.01, −0.23), Z = 3.13 (p = 0.002), χ2 = 49.49; df = 2; p < 0.00001; I2 = 96%; 3 studies, n = 136). Out of the three studies, two studies compared the effectiveness of IPT in reducing depression scores specifically when compared to the usual treatment, and in both studies, depression scores were reduced significantly in the IPT group as compared to the usual treatment group. Only one study directly compared the effectiveness of IPT with ADM, reporting that IPT was more effective than ADM in reducing depression scores among postpartum women. Regarding adverse outcomes, only one study reported suicidal ideation with one participant in the IPT group and two in the ADM group (RR 0.50, 95% CI (0.05, 5.30), p = 0.56, n = 78). The same study reported seven participants in the ADM group had adverse drug reactions as compared to none in the IPT group (RR 15.0, 95% CI (0.89, 254), p = 0.06, n = 78). Authors' Conclusions: Our comprehensive search yielded a limited number of four studies conducted in such settings. Despite the scarcity of available evidence, the findings collectively suggest that IPT is indeed an effective treatment for reducing PPD when compared to usual treatment and pharmacological therapy. However given the low certainty of evidence, there is a need for further research in the form of well‐designed randomized controlled trials with larger sample sizes and a reduced risk of bias. Such studies would greatly contribute to enhancing the strength and reliability of the evidence base regarding the effectiveness of IPT in the context of PPD in LMICs. The knowledge generated from future research endeavors would be highly valuable in guiding the development of more affordable and cost‐effective treatment approaches for PPD in resource‐limited settings. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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30. Post‐marketing surveillance of quetiapine fumarate extended‐release tablets in patients with bipolar depression.
- Author
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Kishi, Taro, Iwata, Nakao, Irie, Hiroyuki, and Aikawa, Masaru
- Subjects
BIPOLAR disorder ,MENTAL depression ,DRUG side effects ,QUETIAPINE ,ANTIDEPRESSANTS ,MOOD stabilizers ,OLANZAPINE ,SUMATRIPTAN - Abstract
Aim: This study aimed to verify the real‐world efficacy and safety of quetiapine fumarate extended‐release tablets (Bipresso® 50 mg and 150 mg; marketing authorization holder is KYOWA Pharmaceutical Industry Co., Ltd., Osaka, Japan) in patients with bipolar depression. Methods: We performed a post‐marketing surveillance with an observation period of 12 weeks. Results: In the safety analysis group (n = 345), adverse drug reactions (ADRs) occurred in 111 patients (32.17%). The most common ADRs (>1%) were somnolence in 55 patients (15.94%), akathisia in 11 (3.19%), dizziness in 10 (2.90%), weight increase in 6 (1.74%), thirst in 5 (1.45%), and hypersomnia, constipation, and nausea in 4 patients each (1.16%). The only severe ADR was one patient of suicidal ideation, and "longer time since the onset of the first episode" (p = 0.011) and "presence of complications" (p < 0.001) were identified as significant risk factors for the occurrence of ADRs. In the efficacy analysis group (n = 265), the average changes from baseline in the total Montgomery–Åsberg Depression Rating Scale (MADRS) score were −7.3 ± 8.8, −12.2 ± 10.7, −16.8 ± 12.7, and −13.2 ± 12.7 points after 4, 8, and 12 weeks, and at the last evaluation, respectively. The mean MADRS total score decrease had no significant association with maximum daily dose, diagnosis, and presence or absence of prior or concomitant treatment for bipolar disorder with mood stabilizers/antipsychotics/antidepressants. Conclusion: The efficacy of quetiapine fumarate extended‐release tablets was confirmed in clinical practice, and no new safety concerns or risks were identified. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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- View/download PDF
31. Hospital Pharmacy Dispensing Records for Pharmacoepidemiology Research into Late Gestation Exposure to Antidepressants.
- Author
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Grzeskowiak, Luke E., Gilbert, Andrew L., and Morrison, Janna L.
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ANTIDEPRESSANTS ,ANALYSIS of variance ,COMPUTER software ,CONFIDENCE intervals ,DRUG prescribing ,HOSPITAL pharmacies ,ELECTRONIC health records ,THIRD trimester of pregnancy ,PREGNANT women ,RESEARCH funding ,PHYSICIAN practice patterns ,DATA analysis ,RETROSPECTIVE studies ,PREGNANCY - Abstract
Aim: To determine the validity of electronic hospital pharmacy dispensing records as an indicator of late gestation exposure to antidepressants using medical records as the gold standard. Method:Medical records (gold standard) were reviewed for a consecutive sample of 400 women who delivered at a large maternity hospital during 2005. Data on antidepressants used in pregnancy from the medical records were compared with the electronic pharmacy dispensing records to ascertain sensitivity and specificity. Results: According to the medical records, 12 (3%) women were identified as taking antidepressants during late gestation. The electronic pharmacy dispensing records correctly identified 9 women as exposed to antidepressants (sensitivity score 75%; 95%CI 43-95). No women were classified as exposed according to pharmacy dispensing records and classified as not exposed according to the medical records (specificity score 100%; 95%CI 99-100). 7 (1.8%) women were identified in the medical records as taking antidepressants but had either stopped prior to pregnancy or on finding out that they were pregnant. These patients were not identified in the pharmacy dispensing records. Conclusion: Electronic hospital pharmacy dispensing records may provide an efficient alternative to paper records for identifying late gestation exposure to antidepressants, but will underestimate the exposure by 25%. [ABSTRACT FROM AUTHOR]
- Published
- 2010
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32. A validation analysis of two self-reported HAM-D6 versions.
- Author
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Bech, P., Wilson, P., Wessel, T., Lunde, M., and Fava, M.
- Subjects
- *
ANTIDEPRESSANTS , *MENTAL depression , *THERAPEUTICS , *AFFECTIVE disorders , *SEASONAL affective disorder , *PATHOLOGICAL psychology ,PSYCHIATRIC research - Abstract
Objective: The six items of the clinician-administrated Hamilton Depression Scale (HAM-D6) cover the core items of depressive states reflecting the antidepressive effect of medication. In this study, the two self-reported versions of the HAM-D6 have been psychometrically validated to ensure the unidimensionality of this administration form in patients with mild-to-moderate depression. Method: The item response theory analysis of Mokken was used to test the unidimensionality of both the Interactive Voice Recording System (IVRS) version of the HAM-D6 and a paper-and-pencil self-reported version (S-HAM-D6). Patients with typical major depression and with seasonal affective disorder were included. Results: The Mokken analysis showed that the two self-reported versions of the HAM-D6 obtained coefficients of homogeneity above 0.40, similar to the clinician-rated HAM-D6 and thus implying unidimensionality. By contrast, the full HAM-D17 versions (self-reported as well as clinician-rated) obtained coefficients of homogeneity below 0.40, implying that the HAM-D17 is a multidimensional scale. Conclusion: The analysis show that both the IVRS version and the S-HAM-D6 version are unidimensional self-rating scales for the measurement of depressive states. [ABSTRACT FROM AUTHOR]
- Published
- 2009
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33. Rapid cycling bipolar disorder – diagnostic concepts.
- Author
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Bauer, Michael, Beaulieu, Serge, Dunner, David L., Lafer, Beny, and Kupka, Ralph
- Subjects
BIPOLAR disorder ,AFFECTIVE disorders ,MOOD (Psychology) ,PSYCHOLOGICAL research ,NEUROPHYSIOLOGY - Abstract
Objectives: This paper reviews the literature to examine the DSM-IV diagnostic criteria for rapid cycling in bipolar disorder. Methods: Studies on the clinical characteristics of rapid cycling bipolar disorder were reviewed. To identify relevant papers, literature searches using PubMed and MEDLINE were undertaken. Results: First observed in the prepharmacologic era, rapid cycling subsequently has been associated with a relatively poor response to pharmacologic treatment. Rapid cycling can be conceptualized as either a high frequency of episodes of any polarity or as a temporal sequence of episodes of opposite polarity. The DSM-IV defines rapid cycling as a course specifier, signifying at least four episodes of major depression, mania, mixed mania, or hypomania in the past year, occurring in any combination or order. It is estimated that rapid cycling is present in about 12–24% of patients at specialized mood disorder clinics. However, apart from episode frequency, studies over the past 30 years have been unable to determine clinical characteristics that define patients with rapid cycling as a specific subgroup. Furthermore, rapid cycling is a transient phenomenon in many patients. Conclusions: While a dimensional approach to episode frequency as a continuum between the extremes of no cycling and continuous cycling may be more appropriate and provide a framework to include ultra-rapid and ultradian cycling, the evidence does not exist today to refine the DSM-IV definition in a less arbitrary manner. Continued use of the DSM-IV definition also enables comparisons between past and future studies, and it should be included in the next release of the ICD. Further scientific investigation into rapid cycling is needed. In addition to improving the diagnostic criteria, insight into neurophysiologic mechanisms of mood switching and episode frequency may have important implications for clinical care. [ABSTRACT FROM AUTHOR]
- Published
- 2008
- Full Text
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34. Iatrogenic sexual dysfunction and the protective withholding of information: in whose best interest?
- Author
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Higgins, A., Barker, P., and Begley, C. M.
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IATROGENIC diseases ,THERAPEUTIC complications ,SEXUAL dysfunction ,ANTIPSYCHOTIC agents ,DRUG therapy for psychoses ,ANTIDEPRESSANTS - Abstract
In recent years a growing body of evidence has highlighted the impact of neuroleptics and antidepressants on sexual function. Research from a service user’s perspective suggested that service users are dissatisfied with the information that they received on drugs, and would like more education, in particular, on the side effects of medication that impact on sexual function. This paper reports some of the findings of a grounded theory study that explored how psychiatric nurses responded to issues of sexuality in practice. Emphasis within the paper is given to how nursing staff addressed the side effects of drugs that impact on sexual function. Findings suggested that nurse addressed the issue of prescribed medication and sexual function in practice, using a ‘Veiling Sexualities Cycle’, which had three subcategories: ‘ Hanging the Veil’, ‘Lifting the Veil’ and ‘Re-veiling’. In the light of contemporary mental health policy, findings from the study are discussed and recommendations for practice and education made. [ABSTRACT FROM AUTHOR]
- Published
- 2006
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35. Should nortriptyline be used as a first-line aid to help smokers quit? Results from a systematic review and meta-analysis.
- Author
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Wagena, E. J., Knipschild, P., and Zeegers, M. P. A.
- Subjects
SMOKING cessation ,PLACEBOS ,SMOKING ,CLINICAL trials ,MEDICAL research ,MEDICAL care - Abstract
The objective of this paper is to evaluate the efficacy of nortriptyline for smoking cessation compared to placebo and bupropion sustained release.Randomized trials were identified by (1) checking electronic and (2) online publicly accessible registers of clinical trials; (3) searching references of identified studies and screening abstract books of conferences and symposia, and (4) personal communication with the first authors of identified papers.We included randomized trials in which nortriptyline was compared to placebo or bupropion hydrochloride SR. The main clinical outcome measure was (at least) 6-month prolonged abstinence, confirmed with a biochemical test. To investigate the efficacy of nortriptyline in time, we calculated the percentage of smokers who relapsed in time.We identified five randomized trials, including 861 smokers. Compared to placebo medication, nortriptyline resulted in significantly higher prolonged abstinence rates after at least 6 months[relative risk (RR) = 2.4, 95% CI 1.7–3.6; RD = 0.11, 95% CI 0.07–0.15]. The difference in efficacy between nortriptyline and placebo was highest in the first months after the target quit date. However, the number of people who remained abstinent decreased substantially and significantly faster over time in the nortriptyline group. Although bupropion resulted in higher abstinence rates compared with nortriptyline, the difference was not statistically significant (RR = 1.7, 95% CI 0.7–4.1).This systematic review and meta-analysis shows that the use of nortriptyline for smoking cessation resulted in higher prolonged abstinence rates after at least 6 months compared to placebo treatment. Furthermore, the use of nortriptyline for smoking cessation is well tolerated and safe. As a result, we believe health care professionals should be recommended to prescribe nortriptyline as a first-line therapy for smoking cessation, also because of the much lower cost of nortriptyline compared to bupropion SR. [ABSTRACT FROM AUTHOR]
- Published
- 2005
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36. The use of antidepressant drugs in dermatology.
- Author
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Gupta, MA and Gupta, AK
- Subjects
ANTIDEPRESSANTS ,DERMATOLOGY - Abstract
AbstractThis paper provides an updated review of the use of antidepressant drugs in dermatology. Some of the psychiatric disorders that are usually comorbid with dermatological disorders and respond to antidepressants include major depressive disorder, obsessive compulsive disorder, body dysmorphic disorder, social phobia and post-traumatic stress disorder usually secondary to trauma and abuse during early life. Cutaneous symptoms may be the feature of a primary psychiatric disorder, e.g. cutaneous body image problems, dermatitis artefacta, neurotic excoriations and trichotillomania, or psychiatric syndromes may be comorbid with a primary dermatological disorder such as the association of major depressive disorder or social phobia with psoriasis and obsessive compulsive disorder with acne excoriee. Some of the salient pharmacological properties of the tricyclic antidepressants (TCAs) and the selective serotonin reuptake inhibitor (SSRI) antidepressants are reviewed. The review indicates that the SSRI antidepressants are potentially beneficial in the management of all the major psychiatric syndromes that are encountered in dermatological disorders. The generally more favourable side-effect profile of the SSRIs, such as lower cardiotoxicity in contrast to the TCAs, has made them the first-line agents for the treatment of depression. Furthermore, some of the pharmacological properties of the antidepressant agents that are not related to their antidepressant activity, such as the histamine H1 blocking effect of TCAs, such as doxepin, amitriptyline and trimipramine, are of benefit in dermatological conditions such as urticaria and pruritus. This paper reviews the general guidelines for use of antidepressants and salient drug–drug interactions resulting mainly from the inhibition of the cytochrome P450 (CYP) 2D6 and 3A3/4 isoenzymes by some of the SSRI antidepressants. Before prescribing an antidepressant agent, the specific guidelines, side-effect profile,... [ABSTRACT FROM AUTHOR]
- Published
- 2001
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37. Surface, micellar, and thermodynamic properties of antidepressant drug nortriptyline hydrochloride with TX-114 in aqueous/urea solutions.
- Author
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Rub, Malik Abdul, Azum, Naved, Khan, Farah, and Asiri, Abdullah M.
- Subjects
MICELLES ,THERMODYNAMICS ,ANTIDEPRESSANTS ,NORTRIPTYLINE (Drug) ,HYDROCHLORIC acid ,AQUEOUS solutions - Abstract
This paper deals with a comprehensive study of the mixed micellization and adsorption behavior of mixed systems enclosing an amphiphilic antidepressant drug nortriptyline hydrochloride (NOT) and Triton X-114 (TX-114) (nonionic surfactant) in aqueous/urea (500 mmol·kg
−1 and 1000 mmol·kg−1 ) solutions by tensiometric method. The NOT is used for the cure of depression. For comparison purpose cmc value of pure drug NOT was also evaluated by conductimetric technique. Different theoretical models like Clint, Rubingh, and Rosen were used to get information about the nature of interaction between the components in bulk and at the interface. Because of the occurrence of urea increase in the surface charge of the micelles was obtained resulting a delay of the micelles formation. The cmc values of the mixed systems of NOT and TX-114 were found to be in between the cmc values of pure components, which signify nonideal mixed system having attractive interactions in the absence and presence of urea. Various parameters such as micellar mole fractions of TX-114 ( X1 m , X1 σ ) in solution and at interface, interaction parameter ( βm / βσ ) in solution and at interface, and activity coefficient in solution and at interface were evaluated and discussed using Rubingh's and Rosen's models. Surface excess ( Γmax ) increases that means minimum area per head group ( Amin ) decreases as mole fraction ( α1 ) of TX-114 increases in the absence/presence of urea. Different thermodynamic parameters have been calculated and discussed. The ∆ G0 m values achieved are all negative both in the absence and occurrence of urea. [ABSTRACT FROM AUTHOR]- Published
- 2017
- Full Text
- View/download PDF
38. Manic switches induced by antidepressants: an umbrella review comparing randomized controlled trials and observational studies.
- Author
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Allain, N., Leven, C., Falissard, B., Allain, J.‐S., Batail, J.‐M., Polard, E., Montastruc, F., Drapier, D., and Naudet, F.
- Subjects
BIPOLAR disorder ,THERAPEUTICS ,ANTIDEPRESSANTS ,SEROTONIN uptake inhibitors ,NORADRENALINE ,RANDOMIZED controlled trials ,PLACEBOS ,DISEASE prevalence - Abstract
Objective We aimed to explore whether the prevalence of manic switch was underestimated in randomized controlled trials ( RCTs) compared to observational studies ( OSs). Method Meta-analyses and simple and systematic reviews were identified by two reviewers in a blinded, standardized manner. All relevant references were extracted to include RCTs and OSs that provided data about manic switch prevalence after antidepressant treatment for a major depressive episode. The primary outcome was manic switch prevalence in the different arms of each study. A meta-regression was conducted to quantify the impact of certain variables on manic switch prevalence. Results A total of 57 papers (35 RCTs and 22 OSs) were included in the main analysis. RCTs underestimated the rate of manic switch [0.53 (0.32-0.87)]. Overestimated prevalence was related to imipraminics [1.85 (1.22-2.79)]; to serotonin-norepinephrine reuptake inhibitors [1.74 (1.06-2.86)]; and to other classes of drugs [1.58 (1.08-2.31)], compared to placebo treatment. The prevalence of manic switch was lower among adults than among children [0.2 (0.07-0.59)]; and higher [20.58 (8.41-50.31)] in case of bipolar disorder. Conclusion Our results highlight an underestimation of the rates of manic switch under antidepressants in RCTs compared to the rates observed in observational studies. [ABSTRACT FROM AUTHOR]
- Published
- 2017
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- View/download PDF
39. Allergic contact dermatitis due to 5% doxepin cream.
- Author
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Bilbao, Ibon, Aguirre, Antonio, Vicente, Jose Miguel, Raton, Juan Antonio, Zabala, Roberto, and Perez, Jose Luis Diaz
- Subjects
DOXEPIN ,ANTIDEPRESSANTS ,ANTIHISTAMINES ,ANTIALLERGIC agents ,ANXIETY ,DROWSINESS - Abstract
Doxepin is a tricyclic compound with antihistamine function, used orally for anxiety, depression and chronic urticaria. Topical application of 5% doxepin can relieve the itching associated with certain dermatoes. The most common adverse died of doxepin is transient stinging at the application site. Drowsiness secondary to significant systemic absorption is the second most common side-effect. Previous case reports of allergic contact dermatitis from doxepin all had positive patch tests to 5% pet. Featured hee is the first European case of allergic contact dermatitis due to topical doxepin and recommended patch testing it at 1% pet.
- Published
- 1996
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40. Lithium treatment in the era of personalized medicine.
- Subjects
THERAPEUTIC use of lithium ,INDIVIDUALIZED medicine ,LITHIUM carbonate ,BIPOLAR disorder ,MOOD stabilizers ,ANTIDEPRESSANTS - Abstract
In 1949, an Australian psychiatrist, John Cade, reported on the antimanic efficacy of lithium carbonate, which is regarded as an introduction of lithium into contemporary psychiatry. Since the 1960s, lithium has been a precursor of mood stabilizers and has become first‐choice drug for the prevention of affective episodes in mood disorders. For nearly four decades, lithium has also been used for the augmentation of antidepressant drugs in treatment‐resistant depression. The knowledge of clinical and biological factors connected with the capability of long‐term lithium treatment to prevent manic and depressive recurrences makes an important element of the personalized medicine of mood disorders. Excellent prophylactic lithium responders can be characterized by distinct mood episodes, with full remissions between them, the absence of other psychiatric morbidity, and the family history of bipolar illness. In recent years, many other clinical and biological factors connected with such a response have been identified, helping to select the best candidates for lithium prophylaxis. The antisuicidal effect of lithium during its long‐term administration has been demonstrated and should also be taken into account as the element of personalized medicine for the pharmacological prophylaxis of patients with mood disorders. Several studies pertaining to personalized medicine were also dedicated to lithium treatment of acute mood episodes. Lithium still has a value in the treatment of mania and bipolar depression. However, it seems that the more important indication would be the augmentation of antidepressant drugs in treatment‐resistant depression. The factors connected with the efficacy of lithium in these conditions are reviewed. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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41. The sequential treatment approach to resistant schizophrenia with risperidone and clozapine: results of an open study with follow-up.
- Author
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Cavallaro, R., Brambilla, P., and Smeraldi, E.
- Subjects
SCHIZOPHRENIA ,RISPERIDONE ,CLOZAPINE ,ANTIDEPRESSANTS ,PSYCHOPHARMACOLOGY - Abstract
In this paper we extend and test with long-term follow-up the results of a previous paper on the usefulness of a sequential treatment protocol with risperidone and clozapine in resistant schizophrenia. Twenty-four patients diagnosed as resistant schizophrenics according to DSM III R and Kane et al .'s (1988) criteria were treated with risperidone for 3 months. Eight patients responded (according to a priori criteria: improvement of basal BPRS, SAPS and SANS total scores over 20 per cent at 3 months observation), while of the remaining 16 patients two dropped out and nine responded to clozapine treatment within the next month. Five patients had partial or no response to clozapine. Follow-up lasting up to 37 months (mean 22·4 months for risperidone responders and 18·3 months for clozapine responders) showed good stability of response, no significant differences in relapses and re-hospitalizations between risperidone and clozapine responders and no tardive responses. © 1998 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]
- Published
- 1998
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42. PHARMACOLOGY OF PSYCHOTROPIC DRUGS USEFUL IN DERMATOLOGIC PRACTICE.
- Author
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Koblenzer, Caroline S.
- Subjects
PSYCHIATRIC drugs ,DERMATOLOGY ,PHARMACOLOGY ,SYNDROMES ,ANTIDEPRESSANTS ,TRANQUILIZING drugs - Abstract
The article focuses on the use of psychotropic drugs in dermatologic practice. In order to prescribe effectively and safely for these patients, the dermatologist must have a basic understanding of the pharmacology of psychotropic agents. This paper reviews the pharmacology of a selected group of these drugs. The individual syndromes for which the drugs are indicated will be outlined, describing psychopathology, as well as dermatologic patho-physiology and clinical phenomenology, in a companion paper. Integration of the information from these two papers will enable the dermatologist to treat appropriately, and with confidence. In order to treat a dermatosis effectively, an accurate dermatologic diagnosis is the "sine qua non." The same can be said for the cutaneous expressions of psychiatric disease.
- Published
- 1993
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43. What do we know about in‐utero antidepressant exposure, and are these medications safe to use during pregnancy?
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PRENATAL depression ,ANTIDEPRESSANTS ,SEROTONIN uptake inhibitors ,SEROTONIN syndrome ,PREGNANCY - Abstract
Though the discontinuer group was a better comparison group than pregnancies occurring in individuals who did not use antidepressants prior to pregnancy, the observed results could still be due to confounding by severity of symptoms of the condition that indicated antidepressant use. Dear Editor, More than 13% of pregnant individuals experience depression making depression during pregnancy a highly prevalent condition.1 In addition, anxiety is rather common during pregnancy with rates of specific anxiety disorders varying from 3% to 6% among pregnant individuals.2 Antidepressants, particularly selective serotonin reuptake inhibitors (SSRIs), are commonly prescribed to treat depression and anxiety.3 For example, a Canadian study found that 55% of antidepressants were prescribed for depression and 19% were prescribed for anxiety. We would expect individuals with more severe depression and anxiety symptoms to be more likely to continue antidepressant use during pregnancy than individuals who discontinue antidepressant use before pregnancy. [Extracted from the article]
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- 2022
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44. Locus Coeruleus‐Dorsolateral Septum Projections Modulate Depression‐Like Behaviors via BDNF But Not Norepinephrine.
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Zhang, Qian, Xue, You, Wei, Ke, Wang, Hao, Ma, Yuan, Wei, Yao, Fan, Yi, Gao, Lei, Yao, Hang, Wu, Fangfang, Ding, Xin, Zhang, Qingyu, Ding, Jianhua, Lu, Ming, and Hu, Gang
- Subjects
ANTIDEPRESSANTS ,BRAIN-derived neurotrophic factor ,GENETIC overexpression ,LOCUS coeruleus ,NORADRENALINE ,TYROSINE hydroxylase ,KETAMINE - Abstract
Locus coeruleus (LC) dysfunction is involved in the pathophysiology of depression; however, the neural circuits and specific molecular mechanisms responsible for this dysfunction remain unclear. Here, it is shown that activation of tyrosine hydroxylase (TH) neurons in the LC alleviates depression‐like behaviors in susceptible mice. The dorsolateral septum (dLS) is the most physiologically relevant output from the LC under stress. Stimulation of the LCTH‐dLSSST innervation with optogenetic and chemogenetic tools bidirectionally can regulate depression‐like behaviors in both male and female mice. Mechanistically, it is found that brain‐derived neurotrophic factor (BDNF), but not norepinephrine, is required for the circuit to produce antidepressant‐like effects. Genetic overexpression of BDNF in the circuit or supplementation with BDNF protein in the dLS is sufficient to produce antidepressant‐like effects. Furthermore, viral knockdown of BDNF in this circuit abolishes the antidepressant‐like effect of ketamine, but not fluoxetine. Collectively, these findings underscore the notable antidepressant‐like role of the LCTH‐dLSSST pathway in depression via BDNF‐TrkB signaling. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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45. Trends in the multiple prescriptions of hypnotic drugs in a university outpatient in Japan.
- Author
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Kato, Takao, Kotorii, Nozomu, Ozone, Motohiro, Murotani, Kenta, Ohshima, Hayato, Mori, Hiroyuki, Wasano, Kenjirou, Hiejima, Hiroshi, Habukawa, Mitsunari, and Uchimura, Naohisa
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HYPNOTICS ,DRUGS ,DRUG prescribing ,PSYCHIATRIC drugs ,PSYCHIATRIC clinics - Abstract
Aims: In Japan, the daily dosage of hypnotic drugs for insomnia treatment is increasing year by year, and over‐dependence on treatment with hypnotic drugs is a major problem. This study aimed to examine the factors related to the elimination of prescriptions of three or more hypnotic drugs within 1 year in our clinic. Methods: We conducted two surveys. Survey ① assessed the frequency of prescriptions of three or more hypnotic drugs by retrospectively reviewing the medical records of all patients who visited general and psychiatric outpatient clinics from January 2013 to March 2019. Survey ② assessed changes in prescriptions of hypnotic and psychotropic drugs within the subsequent year by retrospectively reviewing the medical records of all patients prescribed three or more hypnotic drugs who visited neuropsychiatric outpatient clinics multiple times between April 2013 and March 2019. Results: The frequency of prescribing three or more hypnotic drugs was six to nine times higher in psychiatry than in other departments. Flunitrazepam and brotizolam were the most common drugs prescribed and had the second lowest discontinuation rate after zolpidem. Conversely, eszopiclone, zopiclone, and suvorexant had the highest discontinuation rates. The success factors for drug reduction were age (odds ratio [OR]: 0.97, p < 0.0037), trazodone addition (OR: 12.86, p < 0.0194) and number of years of psychiatric experience. Conclusions: The characteristics and success factors in relation to drug reduction in patients with multiple prescriptions of hypnotic drugs identified in this study may contribute to solving the problem of multiple prescriptions of hypnotic drugs. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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46. Newer antidepressant for Japanese adults with major depressive disorder: A systematic review and meta‐analysis.
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Kishi, Taro, Sakuma, Kenji, Hatano, Masakazu, Matsuda, Yuki, Esumi, Satoru, Miyake, Nobumi, Miura, Itaru, Hori, Hikaru, Kato, Masaki, and Iwata, Nakao
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MENTAL depression ,JAPANESE people ,ANTIDEPRESSANTS ,UBIQUINONES - Abstract
Introduction: The question remains to be elucidated: "Is treatment with antidepressants at doses approved in Japan effective for Japanese patients with MDD?" It is crucial to confirm this in order to provide appropriate treatments for Japanese patients with major depressive disorder (MDD). Therefore, we conducted a systematic review and random‐effects pairwise meta‐analysis including these nine double‐blind, randomized, placebo‐controlled trials. Methods: We calculated the standardized mean difference (SMD) and risk ratio (RR) with a 95% confidence interval (95% CI). Results: Pooled newer antidepressants outperformed placebo regarding improvement of depressive symptom scale scores [SMD (95% CI) = −0.20 (−0.27, −0.12), p < 0.00001], response to treatment [RR (95% CI) = 1.23 (1.13, 1.32), p < 0.00001], and remission rate [RR (95% CI) = 1.30 (1.16, 1.45), p < 0.00001]. Although all‐cause discontinuation was not significantly different between the treatment groups, the pooled antidepressant group showed a higher discontinuation rate due to adverse event [RR (95% CI) = 1.60 (1.13, 2.26), p = 0.007] and a higher incidence of at least one adverse event than the placebo group [RR (95% CI) = 1.13 (1.08, 1.18), p < 0.00001]. Discussion: We concluded that newer antidepressants are effective for Japanese adults with MDD although the clinicians must monitor the health conditions of these individuals. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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47. The lived experience of withdrawal from Selective Serotonin Reuptake Inhibitor (SSRI) antidepressants: A qualitative interview study.
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Mahmood, Raqeeb, Wallace, Vuokko, Wiles, Nicola, Kessler, David, Button, Katherine S., and Fairchild, Graeme
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ANTIDEPRESSANTS ,COGNITION disorders ,SEROTONIN uptake inhibitors ,RESEARCH methodology ,INTERVIEWING ,MENTAL health ,EXPERIENCE ,QUALITATIVE research ,QUALITY of life ,SOUND recordings ,INTERPERSONAL relations ,RESEARCH funding ,TERMINATION of treatment ,THEMATIC analysis ,EMOTION regulation ,PSYCHOLOGICAL adaptation - Abstract
Background: Our knowledge of the broader impacts of antidepressant withdrawal, beyond physical side effects, is limited. Further research is needed to investigate the lived experiences of withdrawal, to aid clinicians on how to guide patients through the process. Aim: To explore antidepressant users' experiences and views on the withdrawal process and how it affected their quality of life across multiple life domains. Design and Setting: We conducted in‐depth qualitative interviews with 20 individuals from the community who had attempted to withdraw from Serotonin Reuptake Inhibitor antidepressants in the past year. Method: Semi‐structured interviews were conducted online. A topic guide was used to ensure consistency across interviews. The interviews were audio‐recorded and transcribed verbatim and analysed using inductive reflexive thematic analysis. Results: Five themes were generated. The first highlighted the challenges of managing the release from emotional blunting and cognitive suppression following antidepressant discontinuation. The second related to the negative impact of withdrawal on close relationships and social interactions. The third showed that concurrent with negative physical symptoms, there was a positive impact on health (exercise was reported by some as a coping mechanism). The fourth theme focused on support from GPs and families, emphasising the importance of mental health literacy in others. The final theme underscored the importance of gradual and flexible tapering in enabling a manageable withdrawal experience, and the consideration of timing. Conclusion: The lived experience of withdrawal significantly impacts individuals' well‐being. Participants emphasised that withdrawal is not just about physical side effects but also affects their emotional, cognitive, and social functioning. Patient and Public Involvement (PPI): Eight people attended individual online meetings to share their experiences of antidepressant withdrawal to help inform the study design and recruitment strategy. Insights from these meetings informed the development of the topic guide. Questions about GP involvement, family relationships, and mood and thinking changes were included based on this PPI work. This ensured the inclusion of topics important to antidepressant users and facilitated the researcher's questioning during the interviews. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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48. Patterns and correlates of new psychoactive substance use in a sample of Australian high school students.
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Champion, Katrina E., Teesson, Maree, and Newton, Nicola C.
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PSYCHIATRIC drugs ,ANTIDEPRESSANTS ,TRANQUILIZING drugs ,OPIOIDS ,CANNABIS (Genus) ,DRUGS of abuse ,STATISTICAL sampling ,SCHOOLS ,SELF-efficacy ,SELF-evaluation ,PSYCHOLOGICAL stress ,STUDENTS ,SUBSTANCE abuse ,RANDOMIZED controlled trials ,CROSS-sectional method - Abstract
Introduction and Aims: In recent years there has been growing concern about new psychoactive substances (NPS) designed to mimic the effects of established illicit drugs. This paper explores the patterns and correlates of NPS use in a sample of Australian students.Design and Methods: A cross-sectional survey was conducted in Australia in 2014. Data were collected from 1126 students (mean age: 14.9 years) from 11 secondary schools. Students completed a self-report questionnaire assessing NPS use and knowledge, beliefs and intentions to use these substances. NPS users were compared with non-users and illicit drug users, who had not used NPS, in terms of gender, binge drinking, tobacco use, psychological distress and self-efficacy to resist peer pressure.Results: Of the 1126 students, 3% reported having ever tried NPS, 2.4% had used synthetic cannabis and 0.4% had used a synthetic stimulant. Analyses revealed that NPS users were more likely to have had an episode of binge drinking in the past 6 months, tried tobacco and had higher levels of psychological distress and lower perceived self-efficacy to resist peer pressure than non-users, but did not significantly differ from users of other illicit drugs.Discussion and Conclusions: NPS use appears to be uncommon among Australian school students. Although adolescents that do use these substances did not differ from students that had used traditional illicit drugs, both appear to be higher-risk groups of students than non-users. Our findings suggest that universal education about NPS be incorporated into existing drug prevention programmes, and that targeted NPS prevention may also be warranted among high-risk adolescents. [Champion KE, Teesson M, Newton NC. Patterns and correlates of new psychoactive substance use in a sample of Australian high school students. Drug Alcohol Rev 2016;35:338-344]. [ABSTRACT FROM AUTHOR]- Published
- 2016
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49. Psychopharmacology and Bariatric Surgery.
- Author
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Roerig, James L. and Steffen, Kristine
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ANTIDEPRESSANTS ,LAPAROSCOPY ,OBESITY ,BARIATRIC surgery ,PSYCHOPHARMACOLOGY ,PSYCHIATRIC drugs ,GASTRIC bypass - Abstract
Currently, it has been demonstrated that psychotropic drugs, particularly antidepressants, are frequently prescribed for patients who seek bariatric surgery. Many bariatric surgery patients have a history of a mood disorder. Unlike medications for diabetes, hypertension or hyperlipidemia, which are generally reduced and at times discontinued, postsurgery antidepressants use is only slightly reduced. The Roux-en-Y procedure is most frequently associated with alteration in drug exposure. Medication disintegration, dissolution, absorption, metabolism and excretion have been found to be altered in postbariatric patients, although data are sparse at this time. This paper will review the current evidence regarding the effect of bariatric surgery on drug treatment including mechanism of interference as well as the extent of changes identified to date. Data will be presented as controlled trials followed by case series and reports. Copyright © 2015 John Wiley & Sons, Ltd and Eating Disorders Association. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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50. Determination of three antidepressants in urine using simultaneous derivatization and temperature-assisted dispersive liquid-liquid microextraction followed by gas chromatography-flame ionization detection.
- Author
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Alizadeh Nabil, Ali Akbar, Nouri, Nina, and Farajzadeh, Mir Ali
- Abstract
This paper presents a fast and simple method for the extraction, preconcentration and determination of fluvoxamine, nortriptyline and maprotiline in urine using simultaneous derivatization and temperature-assisted dispersive liquid-liquid microextraction (TA-DLLME) followed by gas chromatography-flame ionization detection (GC-FID). An appropriate mixture of dimethylformamide (disperser solvent), 1,1,2,2-tetrachloroethane (extraction solvent) and acetic anhydride (derivatization agent) was rapidly injected into the heated sample. Then the solution was cooled to room temperature and cloudy solution formed was centrifuged. Finally a portion of the sedimented phase was injected into the GC-FID. The effect of several factors affecting the performance of the method, including the selection of suitable extraction and disperser solvents and their volumes, volume of derivatization agent, temperature, salt addition, pH and centrifugation time and speed were investigated and optimized. Figures of merit of the proposed method, such as linearity ( r
2 > 0.993), enrichment factors (820-1070), limits of detection (2-4 ng mL−1 ) and quantification (8-12 ng mL−1 ), and relative standard deviations (3-6%) for both intraday and interday precisions (concentration = 50 ng mL−1 ) were satisfactory for determination of the selected antidepressants. Finally the method was successfully applied to determine the target pharmaceuticals in urine. Copyright © 2014 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]- Published
- 2015
- Full Text
- View/download PDF
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