Marjan M A Nielen’s research while affiliated with University of Groningen and other places

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Publications (25)


Figure 2. Task main effects and plot of effect sizes. (A) Task main effects for switching, superimposed on sagittal, transaxial and coronal slices from a canonical (MNI [Montreal Neurological Institute] compatible) T1 image as supplied by SPM. Enhanced BOLD responses are shown in the putamen bilaterally. (B) A plot of effect size in the left putamen is displayed for all three groups (MNI coordinates: x = 221, y = 6, z = 0), showing increased activation in this brain area for patients with obsessive-compulsive disorder (OCD) relative to patients with major depressive disorder (MDD) and the control group. doi:10.1371/journal.pone.0059600.g002
Figure 3. Group by condition (SE vs. RE) differences. (A) enhanced BOLD response in left anterior PFC (controls vs. OCD), (B) in dorsal ACC (OCD vs. controls), (C) in right inferior parietal cortex (controls vs. MDD) and (D) in left insula (OCD vs. MDD). doi:10.1371/journal.pone.0059600.g003
In this example (consecutive trials are running from top-left to bottom-right) the events-of-interest are displayed. Subjects are presented two stimuli on each trial, i.e. a letter and a digit, for 4000 ms maximally. Subjects select either stimulus by pressing the left or right button on a button box, after which a fixation cross is presented for 500 ms. Each letter/digit pair is presented in either blue or red color. The trial color cues the task to be performed. In the letter task, subjects indicate whether the letter presented is a vowel or a consonant. In the digit task, subjects indicate whether the digit presented is odd or even. Two consecutive trials never contain the same letter or digit. Trial color changes, and therefore task switching, occurs randomly after 4–6 trials to avoid predictability. The first trials immediately after task switching are defined ‘switch events’ (SEs), all other trials as ‘repeat events’ (REs). Color-task and stimulus-response associations were counterbalanced across participants.
(A) Task main effects for switching, superimposed on sagittal, transaxial and coronal slices from a canonical (MNI [Montreal Neurological Institute] compatible) T1 image as supplied by SPM. Enhanced BOLD responses are shown in the putamen bilaterally. (B) A plot of effect size in the left putamen is displayed for all three groups (MNI coordinates: x = −21, y = 6, z = 0), showing increased activation in this brain area for patients with obsessive-compulsive disorder (OCD) relative to patients with major depressive disorder (MDD) and the control group.
(A) enhanced BOLD response in left anterior PFC (controls vs. OCD), (B) in dorsal ACC (OCD vs. controls), (C) in right inferior parietal cortex (controls vs. MDD) and (D) in left insula (OCD vs. MDD).
Cognitive Inflexibility in Obsessive-Compulsive Disorder and Major Depression Is Associated with Distinct Neural Correlates
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April 2013

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244 Reads

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122 Citations

Peter L Remijnse

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Marjan M A Nielen

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Obsessive-compulsive disorder (OCD) and major depressive disorder (MDD) are frequently co-morbid, and dysfunctional frontal-striatal circuits have been implicated in both disorders. Neurobiological distinctions between OCD and MDD are insufficiently clear, and comparative neuroimaging studies are extremely scarce. OCD and MDD may be characterized by cognitive rigidity at the phenotype level, and frontal-striatal brain circuits constitute the neural substrate of intact cognitive flexibility. In the present study, 18 non-medicated MDD-free patients with OCD, 19 non-medicated OCD-free patients with MDD, and 29 matched healthy controls underwent functional magnetic resonance imaging during performance of a self-paced letter/digit task switching paradigm. Results showed that both patient groups responded slower relative to controls during repeat events, but only in OCD patients slowing was associated with decreased error rates. During switching, patients with OCD showed increased activation of the putamen, anterior cingulate and insula, whereas MDD patients recruited inferior parietal cortex and precuneus to a lesser extent. Patients with OCD and MDD commonly failed to reveal anterior prefrontal cortex activation during switching. This study shows subtle behavioral abnormalities on a measure of cognitive flexibility in MDD and OCD, associated with differential frontal-striatal brain dysfunction in both disorders. These findings may add to the development of biological markers that more precisely characterize frequently co-morbid neuropsychiatric disorders such as OCD and MDD.

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Functional MRI correlates of visuospatial planning in out-patient depression and anxiety

April 2011

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34 Reads

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42 Citations

Acta Psychiatrica Scandinavica

Major depressive disorder (MDD) has been associated with executive dysfunction and related abnormal prefrontal activity, whereas the status of executive function (EF) in frequently co-occurring anxiety disorders and in comorbid depression-anxiety is unclear. We aimed to study functional MRI correlates of (visuospatial) planning in MDD and anxiety disorders and to test for the effects of their comorbidity. Functional MRI was employed during performance of a parametric Tower of London task in out-patients with MDD (n = 65), MDD with comorbid anxiety (n = 82) or anxiety disorders without MDD (n = 64), and controls (n = 63). Moderately/severely depressed patients with MDD showed increased left dorsolateral prefrontal activity as a function of task load, together with subtle slowing during task execution. In mildly depressed and remitted MDD patients, in anxiety patients, and in patients with comorbid depression-anxiety, task performance was normal and no activation differences were observed. Medication use and regional brain volume were not associated with altered visuospatial planning. Prefrontal hyperactivation during high planning demands is not a trait characteristic, but a state characteristic of MDD without comorbid anxiety, occurring independent of SSRI use. Disturbances in planning or the related activation are probably not a feature of anxiety disorders with or without comorbid MDD, supporting the current distinction between anxiety disorders and depression.


Table 1 . Demographic Characteristics of the 89 Randomized Study Patients by Treatment Assignment
Scatterplots of individual patients' Hamilton Scale for Depression (HAM-D) scores at baseline (T0), after 3 weeks of treatment (T1) (A), and 3 weeks after discontinuation of treatment (T2) (B). Treatment consisted of bright light treatment (BLT) or placebo. Points that fall below the solid diagonal represent patients who improved. Points that fall below the dashed diagonal in the gray shaded area represent patients whose scores were reduced by 50% or more relative to baseline.
Bright Light Treatment in Elderly Patients With Nonseasonal Major Depressive Disorder A Randomized Placebo-Controlled Trial

January 2011

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317 Reads

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262 Citations

Archives of General Psychiatry

Major depressive disorder (MDD) in elderly individuals is prevalent and debilitating. It is accompanied by circadian rhythm disturbances associated with impaired functioning of the suprachiasmatic nucleus, the biological clock of the brain. Circadian rhythm disturbances are common in the elderly. Suprachiasmatic nucleus stimulation using bright light treatment (BLT) may, therefore, improve mood, sleep, and hormonal rhythms in elderly patients with MDD. To determine the efficacy of BLT in elderly patients with MDD. Double-blind, placebo-controlled randomized clinical trial. Home-based treatment in patients recruited from outpatient clinics and from case-finding using general practitioners' offices in the Amsterdam region. Eighty-nine outpatients 60 years or older who had MDD underwent assessment at baseline (T0), after 3 weeks of treatment (T1), and 3 weeks after the end of treatment (T2). Intervention Three weeks of 1-hour early-morning BLT (pale blue, approximately 7500 lux) vs placebo (dim red light, approximately 50 lux). Mean improvement in Hamilton Scale for Depression scores at T1 and T2 using parameters of sleep and cortisol and melatonin levels. Intention-to-treat analysis showed Hamilton Scale for Depression scores to improve with BLT more than placebo from T0 to T1 (7%; 95% confidence interval, 4%-23%; P = .03) and from T0 to T2 (21%; 7%-31%; P = .001). At T1 relative to T0, get-up time after final awakening in the BLT group advanced by 7% (P < .001), sleep efficiency increased by 2% (P = .01), and the steepness of the rise in evening melatonin levels increased by 81% (P = .03) compared with the placebo group. At T2 relative to T0, get-up time was still advanced by 3% (P = .001) and the 24-hour urinary free cortisol level was 37% lower (P = .003) compared with the placebo group. The evening salivary cortisol level had decreased by 34% in the BLT group compared with an increase of 7% in the placebo group (P = .02). In elderly patients with MDD, BLT improved mood, enhanced sleep efficiency, and increased the upslope melatonin level gradient. In addition, BLT produced continuing improvement in mood and an attenuation of cortisol hyperexcretion after discontinuation of treatment. clinicaltrials.gov Identifier NCT00332670.


Regional Brain Volume in Depression and Anxiety Disorders

October 2010

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321 Reads

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372 Citations

Archives of General Psychiatry

Major depressive disorder (MDD), panic disorder, and social anxiety disorder are among the most prevalent and frequently co-occurring psychiatric disorders in adults and may have, at least in part, a common etiology. To identify the unique and shared neuroanatomical profile of depression and anxiety, controlling for illness severity, medication use, sex, age of onset, and recurrence. Cross-sectional study. Netherlands Study of Depression and Anxiety. Outpatients with MDD (n = 68), comorbid MDD and anxiety (n = 88), panic disorder, and/or social anxiety disorder without comorbid MDD (n = 68) and healthy controls (n = 65). Volumetric magnetic resonance imaging was conducted for voxel-based morphometry analyses. We tested voxelwise for the effects of diagnosis, age at onset, and recurrence on gray matter density. Post hoc, we studied the effects of use of medication, illness severity, and sex. We demonstrated lower gray matter volumes of the rostral anterior cingulate gyrus extending into the dorsal anterior cingulate gyrus in MDD, comorbid MDD and anxiety, and anxiety disorders without comorbid MDD, independent of illness severity, sex, and medication use. Furthermore, we demonstrated reduced right lateral inferior frontal volumes in MDD and reduced left middle/superior temporal volume in anxiety disorders without comorbid MDD. Also, patients with onset of depression before 18 years of age showed lower volumes of the subgenual prefrontal cortex. Our findings indicate that reduced volume of the rostral-dorsal anterior cingulate gyrus is a generic effect in depression and anxiety disorders, independent of illness severity, medication use, and sex. This generic effect supports the notion of a shared etiology and may reflect a common symptom dimension related to altered emotion processing. Specific involvement of the inferior frontal cortex in MDD and lateral temporal cortex in anxiety disorders without comorbid MDD, on the other hand, may reflect disorder-specific symptom clusters. Early onset of depression is associated with a distinct neuroanatomical profile that may represent a vulnerability marker of depressive disorder.


S67-04 Double blind randomised clinical trial of bright light therapy in elderly subjects with nonseaonal major depressive disorder

December 2009

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33 Reads

European Psychiatry

Background The cause of depression is largely unknown, but several studies point to disturbances of biological rhythmicity. The functioning of the suprachiasmatic nucleus (SCN) is impaired, as evidenced by an increased prevalence of day-night rhythm perturbations, such as sleeping disorders. Moreover, the inhibitory SCN neurons on the hypothalamus-pituitary adrenocortical axis (HPA-axis) have decreased activity and HPA-activity is enhanced, when compared to non-depressed elderly. Using bright light therapy (BLT) the SCN can be stimulated. In addition, the beneficial effects of BLT on seasonal depression are well accepted. BLT is a potentially safe, nonexpensive and well accepted treatment option. But the current literature on BLT for depression is inconclusive. Methods/design RCT (ClinicalTrials.gov identifier: NCT00332670) in 89 subjects, of 60 years and older with a diagnosis of major depressive disorder. After inclusion subjects were randomly allocated to the active (BLT) vs. placebo (dim red light) condition. just before the start of light therapy, after completion of three weeks therapy period, and three weeks thereafter several endocrinological, psychophysiological, psychometrically, neuropsychological measures are performed: Results Main effect analyses on HADRS-17 scores revealed significant antidepressant effects from BLT. Primary results will be presented. Discussion BLT reduces nonseasonal depression in elderly patients. Additional lightning may easily be implemented in the homes of patients to serve as add-on treatment to antidepressants or as a stand-alone treatment in elderly depressed patients. Our data support the role of a dysfunctional biological clock in depressed elderly subjects, such a finding may guide further development of novel chronobiological oriented treatment strategies.


Distinct brain systems underlie the processing of valence and arousal of affective pictures

September 2009

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333 Reads

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108 Citations

Brain and Cognition

Valence and arousal are thought to be the primary dimensions of human emotion. However, the degree to which valence and arousal interact in determining brain responses to emotional pictures is still elusive. This functional MRI study aimed to delineate neural systems responding to valence and arousal, and their interaction. We measured neural activation in healthy females (N=23) to affective pictures using a 2 (Valence) x 2 (Arousal) design. Results show that arousal was preferentially processed by middle temporal gyrus, hippocampus and ventrolateral prefrontal cortex. Regions responding to negative valence included visual and lateral prefrontal regions, positive valence activated middle temporal and orbitofrontal areas. Importantly, distinct arousal-by-valence interactions were present in anterior insula (negative pictures), and in occipital cortex, parahippocampal gyrus and posterior cingulate (positive pictures). These data demonstrate that the brain not only differentiates between valence and arousal but also responds to specific combinations of these two, thereby highlighting the sophisticated nature of emotion processing in (female) human subjects.




Fig. 1. Accuracy of performance (hit rate expressed as percentage correct) for each of the five learning blocks in the reward (Rew) and the punishment (Cost) condition for the obsessive–compulsive disorder (OCD) group and the healthy volunteers (NC), averaged across sessions. Bars represent standard errors of the mean.  
Table 1 . Characteristics of participants and mean scores (standard deviation) on the YBOCS, HAMD and HAMA inventories (see text)
Fig. 2. Accuracy of performance (hit rate expressed as percentage correct) for each of the five learning blocks in the first and the second task sessions for obsessive–compulsive disorder (OCD) patients and healthy volunteers (NC), averaged across feedback conditions. Bars represent standard errors of the mean.  
Fig. 4. Averaged mean reaction times (RTs) in milliseconds (ms) for go responses of the obsessive–compulsive disorder (OCD) patients and healthy volunteers (NC) in each of the five learning blocks in the reward (Rew) and the punishment (Cost) condition, averaged across sessions. Bars represent standard errors of the mean.  
Patients with obsessive-compulsive disorder are impaired in associative learning based on external feedback

March 2009

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465 Reads

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52 Citations

Psychological Medicine

Patients with obsessive-compulsive disorder (OCD) have to repeat their actions before feeling satisfied that the action reached its intended goal. Learning theory predicts that this may be due to a failure in the processing of external feedback. We examined the performance of 29 OCD patients and 28 healthy volunteers on an associative learning task, in which initial learning is based solely on external feedback signals. Feedback valence was manipulated with monetary gains and losses. As predicted, OCD patients were impaired during initial, external feedback-driven learning but not during later learning stages. The emotional salience of the feedback modulated learning during the initial stage in patients and controls alike. During later learning stages, however, patients approached near-normal performance with rewarding feedback but continued to produce deficient learning with punishing feedback. OCD patients have a fundamental impairment in updating behavior based on the external outcome of their actions, possibly mediated by faulty error signals in response selection processes.


Fig. 1. The reversal learning task. In this example (consecutive trials are running from top-left to bottom-right) all events of interest are displayed. See Method section for details. 
Table 1 . Demographic and clinical data for patients with major depressive disorder (MDD), patients with obsessive-compulsive disorder (OCD), and for the healthy control group 
Table 2 . Behavioral data on the reversal learning task for the group of patients with major depressive disorder (MDD), with obsessive-compulsive disorder (OCD), and for the healthy control group 
Fig. 2. Across-group interaction effects for affective switching, superimposed on sagittal and transaxial slices from a canonical [Montreal Neurological Institute (MNI) compatible] T1 image as supplied by SPM2. Increasing blood oxygen level-dependent (BOLD) responses for patients with obsessive-compulsive disorder (OCD), major depressive disorder (MDD) and healthy controls respectively are shown in (a) the right dorsolateral prefrontal cortex (DLPFC) (upper left : x=48, y=3, z=18 ; upper middle : x=48, y=3, z=18 ; upper right : x=45, y=42, z=6) and (b) the left anterior PFC (lower left : x=x27, y=60, z=9 ; lower middle : x=x33, y=48, z=x6 ; lower right : x=x18, y=51, z=0). A plot of effect size in the left anterior PFC is displayed for all three groups (x=x27, y=60, z=9). 
Table 3 . Brain regions showing group interaction effects for reward (Correct Responses minus baseline trials), punishment [(Probabilistic Errors no Shift+Final Reversal Errors+Preceding Reversal Errors) minus baseline trials] and affective switching [Final Reversal Errors minus (Preceding Reversal Errors+Probabilistic Errors no Shift)] 
Differential frontal-striatal and paralimbic activity during reversal learning in major depressive disorder and obsessive-compulsive disorder

February 2009

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610 Reads

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128 Citations

Psychological Medicine

Several lines of research suggest a disturbance of reversal learning (reward and punishment processing, and affective switching) in patients with major depressive disorder (MDD). Obsessive-compulsive disorder (OCD) is also characterized by abnormal reversal learning, and is often co-morbid with MDD. However, neurobiological distinctions between the disorders are unclear. Functional neuroimaging (activation) studies comparing MDD and OCD directly are lacking. Twenty non-medicated OCD-free patients with MDD, 20 non-medicated MDD-free patients with OCD, and 27 healthy controls performed a self-paced reversal learning task in an event-related design during functional magnetic resonance imaging (fMRI). Compared with healthy controls, both MDD and OCD patients displayed prolonged mean reaction times (RTs) but normal accuracy. In MDD subjects, mean RTs were correlated with disease severity. Imaging results showed MDD-specific hyperactivity in the anterior insula during punishment processing and in the putamen during reward processing. Moreover, blood oxygen level-dependent (BOLD) responses in the dorsolateral prefrontal cortex (DLPFC) and the anterior PFC during affective switching showed a linear decrease across controls, MDD and OCD. Finally, the OCD group showed blunted responsiveness of the orbitofrontal (OFC)-striatal loop during reward, and in the OFC and anterior insula during affective switching. This study shows frontal-striatal and (para)limbic functional abnormalities during reversal learning in MDD, in the context of generic psychomotor slowing. These data converge with currently influential models on the neuropathophysiology of MDD. Moreover, this study reports differential neural patterns in frontal-striatal and paralimbic structures on this task between MDD and OCD, confirming previous findings regarding the neural correlates of deficient reversal learning in OCD.


Citations (16)


... A relative bias in favour of direct pathway activity over that of the indirect pathway may underlie the rigidity that is characteristic of obsessive-compulsive (OC) symptomology [70][71][72], although not all authors agree [73,74]. Nevertheless, dysregulated cortico-striatal signalling underlies among others, dysfunctional goal-directed outcome regulation on the level of reward feedback processing [75][76][77][78], action-outcome learning [79], response inhibition [78], habitual behaviour [80,81], and cognitive rigidity [1,82], all of which have been identified as neurocognitive underpinnings of OCD [83] (see Section 4). ...

Reference:

The deer mouse (Peromyscus maniculatus bairdii) as a model organism to explore the naturalistic psychobiological mechanisms contributing to compulsive-like rigidity: A narrative overview of advances and opportunities
Cognitive Inflexibility in Obsessive-Compulsive Disorder and Major Depression Is Associated with Distinct Neural Correlates

... In the studies performing the emotional processing tasks [21,25,40,45,50], abnormally increased activations were found in the right ventrolateral prefrontal cortex (vlPFC), OFC, the bilateral MTG, STG, and MFG in dlPFC, the amygdala, the striatum, the parahippocampal, the cerebellar, the fusiform and ACC, and abnormally decreased activation was found in the dACC. In the studies performing the reward learning and valuation tasks [27,33,47,51,58], abnormally increased activation was found in the dorsal medial prefrontal cortex (dmPFC) and MFG. ...

Functional MRI correlates of visuospatial planning in out-patient depression and anxiety
  • Citing Article
  • April 2011

Acta Psychiatrica Scandinavica

... A light therapy trial among patients with Parkinson's disease suffering from depression showed that self-reported sleep quality improved in both the BLT and the placebo group, with a larger improvement in patients treated with BLT (Rutten et al. 2019). Among elderly patients suffering from depression, BLT seemed to increase sleep efficiency, advance get-up time, and decrease total sleep time (Lieverse et al. 2011). In contrast, we found no improvement in any sleep parameters, indicating that the period of pregnancy might add additional barriers when comparing to clinical populations in which BLT was effective. ...

Bright Light Treatment in Elderly Patients With Nonseasonal Major Depressive Disorder A Randomized Placebo-Controlled Trial

Archives of General Psychiatry

... In another study, it was reported that the prevalence of depression was 20%-80% and the prevalence of anxiety was 13%-63% [10]. Major depressive disorder, generalized anxiety disorder and social anxiety disorder are among the most common and most frequently comorbid psychiatric disorders in adults [11]. Estimates of depression and anxiety comorbidity range from 10% to over 50% [12]. ...

Regional Brain Volume in Depression and Anxiety Disorders

Archives of General Psychiatry

... Specifically, the TOFC responded strongly to AAC agents, consistent with previous work showing heightened TOFC activation during decision-makings with ambiguous outcomes (Bach et al., 2009). In comparison, the OFG exhibited greater responses to aversive agents than to appetitive ones, supporting prior research demonstrating that part of the OFG is sensitive to affective valence (Nielen et al., 2009;Thakral et al., 2022). Lastly, the LOC activated more vigorously to non-AAC agents than to AAC ones, which corroborates existing studies showing LOC activation increases with the intensity of appetitive or aversive objects (Anderson, 2016;Kuniecki et al., 2018). ...

Distinct brain systems underlie the processing of valence and arousal of affective pictures
  • Citing Article
  • September 2009

Brain and Cognition

... Dysfunction or imbalance of valence processing systems contributes to many psychiatric disorders. Obsessive-compulsive disorder (OCD) (American Psychiatric Association, 2013) is one psychiatric condition in which alterations in both negative and positive valence processing may be characteristic of the disorder Apergis-Schoute et al., 2017;Figee et al., 2011;Kumari et al., 2001;Milad et al., 2013;Nielen et al., 2009;Simon et al., 2010;Tolin et al., 2003). Valence processing abnormalities may relate in fundamental ways to the behaviors characteristic of OCD. ...

Patients with obsessive-compulsive disorder are impaired in associative learning based on external feedback

Psychological Medicine

... Decreased putamen activity during reward processing is related to depressive symptoms generally (Gotlib et al., 2010;Gradin et al., 2011;Keren et al., 2018;Knutson et al., 2008;Pizzagalli et al., 2009;Robinson et al., 2012;Takamura et al., 2017;Yang et al., 2022;Zhang et al., 2016) and anhedonia specifically (Harvey et al., 2010;Keedwell et al., 2005). Note that putamen hyperreactivity to rewarding stimuli in MD is also reported Mitterschiffthaler et al., 2003;Remijnse et al., 2009), but the overall evidence points towards decreased striatal (including putamen) reward processing in MD, as demonstrated in recent meta-analyses (Keren et al., 2018;Yang et al., 2022;Zhang et al., 2016). Interestingly, several reports emphasize decreased DS volume specifically in MD (Beyer & Krishnan, 2002;Kempton et al., 2011;Koolschijn et al., 2009), and populations at-risk for MD (Pagliaccio et al., 2020;Talati et al., 2022), and decreased putamen volume is related to higher self-reported anhedonia (Auerbach et al., 2017;Sachs-Ericsson et al., 2017;Schaub et al., 2021). ...

Differential frontal-striatal and paralimbic activity during reversal learning in major depressive disorder and obsessive-compulsive disorder

Psychological Medicine

... Furthermore, manipulations of light exposure or sleep that affect the circadian clock are now known to affect mood as well (3,4). Bright light, the primary resetting stimulus for the clock, is an effective antidepressant in both MDD and seasonal affective disorder (5,6), and sleep deprivation or shifting sleep onset to an earlier time temporarily alleviates depression (7,8). ...

Bright light in elderly subjects with nonseasonal major depressive disorder: A double blind randomised clinical trial using early morning bright blue light comparing dim red light treatment

Trials

... Meta-analyses have found that individuals with OCD tend to perform worse on measures of neurocognitive functioning, including aspects of memory and executive functioning, compared to healthy controls (Abramovitch et al., 2013;Bora, 2020;Shin et al., 2014;Snyder et al., 2015), and that symptom severity is associated with worse cognitive functioning (Abramovitch et al., 2019). Findings appear to be most consistent for set shifting ability and cognitive flexibility (Abbruzzese et al., 1997;Deepthi et al., 2021;Martínez-Esparza et al., 2021;Okasha et al., 2000;Veale et al., 1996), impaired response inhibition (Bora, 2020;Chamberlain et al., 2006), decision making (Cavedini et al., 2006;Nielen et al., 2002), planning and processing speed (Burdick et al., 2008;Kuelz et al., 2006), and memory dysfunction (Bora, 2020;Chamberlain et al., 2005;Kuelz et al., 2004;Rao et al., 2008). These deficits in cognitive flexibility, set-shifting, and motorinhibition have been shown to extend to unaffected first-degree relatives along with OCD patient probands in a number of subsequent studies (Bora, 2020;Cavedini et al., 2010;Lennertz et al., 2012;Rajender et al., 2011;Viswanath et al., 2009), suggesting that these cognitive deficits may be potential endophenotypes or brain markers for the illness that may reflect the underlying genetic basis of the illness. ...

Decision making performance in obsessive compulsive disorder
  • Citing Article
  • June 2002

Journal of Affective Disorders

... For the current exploratory analyses, to minimize multiple comparisons, we included neurocognitive outcomes where patients performed significantly worse than controls pre-to post-chemotherapy (T1 to T2) in our previous research (Janelsins et al., 2018. Computerized cognitive assessments included items from the Cambridge Neuropsychological Test Battery (CANTAB) (Vardy et al., 2015;Russo et al., 2003;Fray and Robbins, 1996;Robbins et al., 1994;Sahakian and Owen, 1992): the Verbal Recognition Memory (VRM) task (Verbal Recognition Memory (VRM), n.d.) and the One Touch Stockings of Cambridge (OTS) (One Touch Stockings of Cambridge (OTS), n.d.). ...

Neuropsychological investigation into the carcinoid syndrome

Psychopharmacology