8 results on '"Cowen, Philip J."'
Search Results
2. Subchronic treatment with St John's wort produces a positive shift in emotional processing in healthy volunteers.
- Author
-
Warren, Matthew B., Cowen, Philip J., and Harmer, Catherine J.
- Subjects
- *
ANTIDEPRESSANTS , *MENTAL depression , *HYPERICUM , *CLINICAL trials , *SHORT-term memory , *COGNITION , *EMOTIONS , *HYPERICUM perforatum , *PLANT extracts , *BLIND experiment , *PHARMACODYNAMICS - Abstract
Background: The neurocognitive model of antidepressant treatment in depression states that antidepressants work by producing relatively immediate positive shifts in emotional processing, which translate into clinical improvement with time. St John's Wort has shown antidepressant potential in randomised controlled trials; however, its pharmacological actions are broad and it is unknown whether treatment also produces changes in emotional processing.Aims: We investigated whether short-term treatment with St John's wort has similar effects on emotional processing to those reported with other antidepressants such as selective serotonergic reuptake inhibitors.Methods: Forty-eight healthy participants were given St John's wort or placebo treatment for seven days. On day 7 they completed a battery of tasks to measure emotional processing and other elements of cognition.Results: St John's wort treatment produced similar changes to other antidepressants, for example reducing recognition of disgusted faces and attention to fearful faces, while increasing memory for positive words. We failed to find evidence for an effect of St John's wort on other aspects of cognition including working memory.Conclusions: These findings lend support to the theory that the production of early positive biases in emotional processing may be a common feature of all clinically effective antidepressants with diverse pharmacological mechanisms. [ABSTRACT FROM AUTHOR]- Published
- 2019
- Full Text
- View/download PDF
3. Overnight transdermal scopolamine patch administration has no clear effect on cognition and emotional processing in healthy volunteers.
- Author
-
Bukala, Bernard R., Browning, Michael, Cowen, Philip J., Harmer, Catherine J., and Murphy, Susannah E.
- Subjects
- *
SCOPOLAMINE , *MENTAL depression , *ANTIDEPRESSANTS , *SHORT-term memory , *EMOTIONAL intelligence - Abstract
There has been increasing interest in the antidepressant effects of the muscarinic cholinergic receptor antagonist scopolamine. Here we assess, for the first time, whether a transdermal scopolamine patch is sufficient to induce changes in cognition that are consistent with the reported cognitive and antidepressant effects of scopolamine. A scopolamine or placebo patch was administered to healthy volunteers ( n=33) for 17 h in a double-blind, between-subject procedure. There was no clear effect of scopolamine patch on emotional cognition, verbal or working memory, suggesting that the effective dose of scopolamine available through the patch is too low to represent a viable antidepressant mechanism. [ABSTRACT FROM AUTHOR]
- Published
- 2019
- Full Text
- View/download PDF
4. Tianeptine in an experimental medicine model of antidepressant action.
- Author
-
Cooper, Charlotte M, Whiting, Daniel A, Cowen, Philip J, and Harmer, Catherine J
- Subjects
- *
EXPERIMENTAL medicine , *NEUROPSYCHOLOGY , *SEROTONIN , *DRUG efficacy , *THERAPEUTICS ,PHYSIOLOGICAL effects of antidepressants - Abstract
Changes in emotional processing have been shown following acute administration of a range of monoaminergic antidepressants, and may represent an important common neuropsychological mechanism underpinning their therapeutic effects. Tianeptine is an agent that challenges the traditional monoaminergic hypothesis of antidepressant action, though its exact mode of action remains controversial. Healthy volunteers were randomised to receive a single dose of tianeptine (12.5 mg) or placebo, and subsequently completed a battery of tasks measuring emotional processing, including facial expression recognition, emotional memory and attentional vigilance, as well as working and verbal memory. Tianeptine-treated subjects were less accurate at identifying facial expressions, though this was not valence specific. The tianeptine group also showed reduced positive affective memory and reduced attentional vigilance to positive stimuli. There were no effects on emotional categorization or non-emotional cognition. The negative biases in aspects of emotional processing observed following acute tianeptine administration are at variance with the positive biases generally seen after acute administration of conventional antidepressant drugs, despite tianeptine’s putative antidepressant efficacy. This is an intriguing finding in the context of the lack of consensus regarding tianeptine’s mechanism of action; however, it may be consistent with the reported ability of acute tianeptine to increase the re-uptake of serotonin. [ABSTRACT FROM AUTHOR]
- Published
- 2015
- Full Text
- View/download PDF
5. The effects of atorvastatin on emotional processing, reward learning, verbal memory and inflammation in healthy volunteers: An experimental medicine study.
- Author
-
De Giorgi, Riccardo, Martens, Marieke, Rizzo Pesci, Nicola, Cowen, Philip J, and Harmer, Catherine J
- Subjects
- *
REWARD (Psychology) , *EXPERIMENTAL medicine , *VERBAL memory , *ATORVASTATIN , *EMOTIONAL conditioning , *NEUROPSYCHOLOGY , *ANTIDEPRESSANTS , *VERBAL learning , *ANTILIPEMIC agents - Abstract
Background: Growing evidence from clinical trials and epidemiological studies suggests that statins can have clinically significant antidepressant effects, potentially related to anti-inflammatory action on several neurobiological structures. However, the underlying neuropsychological mechanisms of these effects remain unexplored. Aims: In this experimental medicine trial, we investigated the 7-day effects of the lipophilic statin, atorvastatin on a battery of neuropsychological tests and inflammation in healthy volunteers. Methods: Fifty healthy volunteers were randomised to either 7 days of atorvastatin 20 mg or placebo in a double-blind design. Participants were assessed with psychological questionnaires and a battery of well-validated behavioural tasks assessing emotional processing, which is sensitive to putative antidepressant effects, reward learning and verbal memory, as well as the inflammatory marker, C-reactive protein. Results: Compared to placebo, 7-day atorvastatin increased the recognition (p = 0.006), discriminability (p = 0.03) and misclassifications (p = 0.04) of fearful facial expression, independently from subjective states of mood and anxiety, and C-reactive protein levels. Otherwise, atorvastatin did not significantly affect any other psychological and behavioural measure, nor peripheral C-reactive protein. Conclusions: Our results reveal for the first time the early influence of atorvastatin on emotional cognition by increasing the processing of anxiety-related stimuli (i.e. increased recognition, discriminability and misclassifications of fearful facial expression) in healthy volunteers, in the absence of more general effects on negative affective bias. Further studies exploring the effects of statins in depressed patients, especially with raised inflammatory markers, may clarify this finding and inform future clinical trials. [ABSTRACT FROM AUTHOR]
- Published
- 2021
- Full Text
- View/download PDF
6. Antidepressants, withdrawal, and addiction; where are we now?
- Author
-
Jauhar, Sameer, Hayes, Joseph, Goodwin, Guy M, Cowen, Philip J, Baldwin, David S, and Nutt, David J
- Subjects
- *
SEROTONIN uptake inhibitors , *ANTIDEPRESSANTS , *ADDICTIONS , *KNOWLEDGE gap theory , *DEBATE , *COMPARATIVE studies , *COMPULSIVE behavior , *DRUG withdrawal symptoms , *RESEARCH methodology , *MEDICAL cooperation , *RESEARCH , *EVALUATION research - Abstract
Controversy continues with regard to antidepressants and withdrawal. Recent debates have focused on the prevalence and length of withdrawal, and some continue to state that withdrawal from these compounds constitutes 'addiction'. In this editorial we examine the evidence underlying these recent debates. We acknowledge gaps in knowledge, and make suggestions for how the field can progress. [ABSTRACT FROM AUTHOR]
- Published
- 2019
- Full Text
- View/download PDF
7. The putative lithium-mimetic ebselen reduces impulsivity in rodent models.
- Author
-
Barkus, Chris, Ferland, Jacqueline-Marie N., Adams, Wendy K., Churchill, Grant C., Cowen, Philip J., Bannerman, David M., Rogers, Robert D., Winstanley, Catharine A., and Sharp, Trevor
- Subjects
- *
IMPULSE control disorders , *BIPOLAR disorder , *AFFECTIVE disorders , *MENTAL illness , *PSYCHOLOGY , *NEUROPROTECTIVE agents - Abstract
Background: Deficits in impulse control feature in many psychiatric conditions including bipolar disorder, suicidality and addictions. Lithium lowers impulsivity in clinical populations and decreases pathological gambling in experimental medicine studies, but suffers from adverse effects, poor compliance and a low therapeutic index.Aims: Recently we identified that the neuroprotective agent ebselen, which is reportedly safe in humans, inhibited inositol monophosphatase (IMPase), a candidate lithium mechanism. Ebselen also reduced 5-HT receptor (5-HT2A) function which predicts impulsivity lowering properties. Here we investigated the effect of ebselen in rat models of impulsive behaviour.Methods: Ebselen was tested in two models of impulsivity with human analogues: the five-choice serial reaction time task (5-CSRTT) and rodent gambling task (rGT). The main outcome measures were premature responses (5-CSRTT and rGT) and choice behaviour (rGT), which model motor impulsivity and choice impulsivity, respectively.Results: At doses that decreased 5-HT2A receptor function (DOI-induced wet dog shakes), ebselen decreased premature responding in the 5-CSRTT both in the absence and presence of cocaine. The 5-HT2A receptor antagonist MDL 100,907 also reduced premature responding in the 5-CSRTT although not in the presence of cocaine. In the rGT ebselen showed a tendency to reduce premature responding but had no effect on choice behaviour.Conclusions: These findings suggest that ebselen preferentially reduces motor impulsivity over choice impulsivity, and that inhibition of 5-HT2A receptor function is a contributing mechanism. Collectively, these data support the repurposing of ebselen as an anti-impulsive treatment and fast-tracking to clinical trials in patient groups characterised by poor impulse control. [ABSTRACT FROM AUTHOR]- Published
- 2018
- Full Text
- View/download PDF
8. Does melatonin treatment change emotional processing? Implications for understanding the antidepressant mechanism of agomelatine.
- Author
-
Pringle, Abbie, Bogdanovskaya, Maria, Waskett, Poppy, Zacharia, Sophie, Cowen, Philip J., and Harmer, Catherine J.
- Subjects
- *
MELATONIN , *EMOTIONS , *ANTIDEPRESSANTS , *SEROTONIN receptors , *DRUG synergism , *PLACEBOS , *SEROTONIN antagonists , *ACETIC acid , *CELL receptors , *CIRCADIAN rhythms , *RESEARCH funding , *HUMAN research subjects , *BLIND experiment , *THERAPEUTICS - Abstract
The antidepressant, agomelatine, has a novel pharmacological profile, with agonist properties at M1 and M2 receptors and antagonist properties at 5HT2C receptors. Whether the antidepressant effects of this treatment are mediated by the drug's effects at the M1 and M2 receptors or the 5HT2C receptor or a synergy between these actions remains unclear. In the present study, a healthy volunteer model of emotional processing, which discriminates between effective and non-effective antidepressant compounds, was used to assess the contribution of melatonin agonism to the efficacy of agomelatine. Fifty-eight healthy volunteers were randomised to receive 7 days of once daily treatment with either 1 mg melatonin, 3 mg melatonin or placebo. Seven days treatment with 3 mg melatonin resulted in earlier bedtimes consistent with a phase advance in circadian rhythm. Some marginal effects of melatonin were observed on emotional processing; however, these were neither consistent with nor comparable to those seen following conventional antidepressant treatment or with agomelatine itself. These data suggest that the antidepressant action of agomelatine cannot be accounted for solely by its action at the M1 and M2 receptors. [ABSTRACT FROM AUTHOR]
- Published
- 2015
- Full Text
- View/download PDF
Catalog
Discovery Service for Jio Institute Digital Library
For full access to our library's resources, please sign in.