Cognition and functioning in bipolar depression

Kapczinski, Natalia S.; Narvaez, Joana C.; Magalhães, Pedro V.; Bücker, Joana; Peuker, Ana C.; Loredo, Ana C.; Troiano, Federico; Czepielewski, Letícia; Rosa, Adriane; Fries, Gabriel R.; Gama, Clarissa S.

doi:10.1590/1516-4446-2014-1558

Abstract

Objectives:

Depressive symptoms are associated with worse outcomes in patients with bipolar disorder (BD). However, scarce data are available regarding neurocognitive profiles across different areas of functioning among BD patients with moderate and severe depression. Our objective was to assess cognition and global functioning in a group of patients with bipolar depression.

Methods:

Data were available for 100 patients with bipolar depression (78% female) and 70 controls (64% female) paired by age and education level. Cognitive function was assessed with a neuropsychological test battery. Functioning was assessed with the Functioning Assessment Short Test.

Results:

In patients, severe depression was associated with poorer cognitive performance on measures of executive function. Patients with severe depression showed worse global functioning than those with moderate depression (z = 2.54, p = 0.011). In patients with severe depression, lower global functioning was associated with lower scores in working memory (r = -0.200, p = 0.010), and executive function (r = -0.210, p = 0.007; and r = 0.293, p < 0.001).

Conclusion:

Our findings suggest cognitive impairment and global functioning impairment are associated with the severity of depressive symptoms in bipolar depression. Intensive treatment of depressive symptoms in patients with BD is crucial to improve cognitive functioning and, consequently, functional outcomes.

Memory; mood disorders, bipolar; tests/interviews, psychometric; cognitive neuroscience, outcome studies

Introduction

Bipolar disorder (BD) is a chronic, severe, and recurring mood disorder that may also affect cognitive performance and functioning.¹1. American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition, Text Revision (DSM-IV-TR). Porto Alegre: Artmed; 2002. 2. Chaves OC, Lombardo LE, Bearden CE, Woolsey MD, Martinez DM, Barrett JA, et al. Association of clinical symptoms and neurocognitive performance in bipolar disorder: a longitudinal study. Bipolar Disord. 2011;13:118-23. 3. Hellvin T, Sundet K, Simonsen C, Aminoff SR, Lagerberg TV, Andreassen OA, et al. Neurocognitive functioning in patients recently diagnosed with bipolar disorder. Bipolar Disord. 2012;14:227-38. 4. Leboyer M, Kupfer DJ. Bipolar disorder: new perspectives in health care and prevention. J Clin Psychiatry. 2010;71:1689-95. 5. Mann-Wrobel MC, Carreno JT, Dickinson D. Meta-analysis of neuropsychological functioning in euthymic bipolar disorder: an update and investigation of moderator variables. Bipolar Disord. 2011;13:334-42.-⁶6. Torres IJ, Boudreau VG, Yatham LN. Neuropsychological functioning in euthymic bipolar disorder: a meta-analysis. Acta Psychiatr Scand Suppl. 2007;434:17-26. More than 60% of patients with BD have difficulties in performing daily-life routines.⁷7. MacQueen GM, Young LT, Joffe RT. A review of psychosocial outcome in patients with bipolar disorder. Acta Psychiatr Scand. 2001;103:163-70. Presence of depressive symptoms is associated with worse outcomes.⁸8. Strejilevich SA, Martino DJ, Murru A, Teitelbaum J, Fassi G, Marengo E, et al. Mood instability and functional recovery in bipolar disorders. Acta Psychiatr Scand. 2013;128:194-202. Cognitive impairments in BD are consistently observed during mood episodes.⁹9. Robinson LJ, Thompson JM, Gallagher P, Goswami U, Young AH, Ferrier IN, et al. A meta-analysis of cognitive deficits in euthymic patients with bipolar disorder. J Affect Disord. 2006;93:105-15. 10. Iosifescu DV. The relation between mood, cognition and psychosocial functioning in psychiatric disorders. Eur Neuropsychopharmacol. 2012;22:S499-504. 11. Malhi GS, Ivanovski B, Hadzi-Pavlovic D, Mitchell PB, Vieta E, Sachdev P. Neuropsychological deficits and functional impairment in bipolar depression, hypomania and euthymia. Bipolar Disord. 2007;9:114-25.-¹²12. Martinez-Aran A, Vieta E, Colom F, Torrent C, Sanchez-Moreno J, Reinares M, et al. Cognitive impairment in euthymic bipolar patients: implications for clinical and functional outcome. Bipolar Disord. 2004;6:224-32. However, they can also be identified during euthymia. Cognitive deficits are associated with social impairment and worse course of illness,¹³13. Sachs G, Schaffer M, Winklbaur B. [Cognitive deficits in bipolar disorder]. Neuropsychiatr. 2007;21:93-101. and contribute significantly to functional disability, impacting global functioning.¹⁴14. Keefe RS, Fox KH, Davis VG, Kennel C, Walker TM, Burdick KE, et al. The Brief Assessment of Cognition In Affective Disorders (BAC-A): performance of patients with bipolar depression and healthy controls. J Affect Disord. 2014;166:86-92. 15. Depp CA, Mausbach BT, Harmell AL, Savla GN, Bowie CR, Harvey PD, et al. Meta-analysis of the association between cognitive abilities and everyday functioning in bipolar disorder. Bipolar Disord. 2012;14:217-26.-¹⁶16. Harvey PD, Wingo AP, Burdick KE, Baldessarini RJ. Cognition and disability in bipolar disorder: lessons from schizophrenia. Bipolar Disord. 2010;12:364-75.

Deficits in verbal and visual memory and in executive functioning have been demonstrated during depressive episodes,¹¹11. Malhi GS, Ivanovski B, Hadzi-Pavlovic D, Mitchell PB, Vieta E, Sachdev P. Neuropsychological deficits and functional impairment in bipolar depression, hypomania and euthymia. Bipolar Disord. 2007;9:114-25. whereas executive dysfunction and attention deficits have been reported in association with manic episodes.¹²12. Martinez-Aran A, Vieta E, Colom F, Torrent C, Sanchez-Moreno J, Reinares M, et al. Cognitive impairment in euthymic bipolar patients: implications for clinical and functional outcome. Bipolar Disord. 2004;6:224-32. A study by Buoli et al.¹⁷17. Buoli M, Caldiroli A, Caletti E, Zugno E, Altamura AC. The impact of mood episodes and duration of illness on cognition in bipolar disorder. Compr Psychiatry. 2014;55:1561-6. showed that patients with BD assessed during mixed or depressed states performed slightly better than manic patients. However, the data available in the literature are controversial. Other cross-sectional studies have found that depressed patients are the most compromised group in terms of cognition among bipolar patients, especially regarding executive function¹⁸18. Martínez-Arán A, Vieta E, Reinares M, Colom F, Torrent C, Sánchez-Moreno J, et al. Cognitive function across manic or hypomanic, depressed, and euthymic states in bipolar disorder. Am J Psychiatry. 2004;161:262-70. and motor abilities.¹¹11. Malhi GS, Ivanovski B, Hadzi-Pavlovic D, Mitchell PB, Vieta E, Sachdev P. Neuropsychological deficits and functional impairment in bipolar depression, hypomania and euthymia. Bipolar Disord. 2007;9:114-25. Severity of depressive symptoms has been positively correlated with cognitive dysfunction in non-BD samples.¹⁹19. Lawrence C, Roy A, Harikrishnan V, Yu S, Dabbous O. Association between severity of depression and self-perceived cognitive difficulties among full-time employees. Prim Care Companion CNS Disord. 2013;15(3). pii: PCC.12m01469. However, we were not able to find studies evaluating whether the severity of depressive symptoms can be associated with impaired functioning and cognitive deficits in BD.

The association between depressive episodes and impaired global functioning in dimensions such as work, social life, and family relationships is well documented. In recent studies, neurocognition and emotional regulation were shown to have an important impact on depressive symptoms, which influence psychosocial global functioning.²⁰20. Van Rheenen TE, Rossell SL. Objective and subjective psychosocial functioning in bipolar disorder: an investigation of the relative importance of neurocognition, social cognition and emotion regulation. J Affect Disord. 2014;162:134-41. A recent study of patients with type I and II BD (BD-I and BD-II) confirmed verbal memory as a mediator in the relationship between depressive symptoms and functioning. After a 1-year follow-up, subthreshold depressive symptoms predicted worse functional outcome mediated by verbal composite memory scores.²¹21. Bonnín Cdel M, González-Pinto A, Solé B, Reinares M, González-Ortega I, Alberich S, et al. Verbal memory as a mediator in the relationship between subthreshold depressive symptoms and functional outcome in bipolar disorder. J Affect Disord. 2014;160:50-4. However, the study included only euthymic patients with at least a moderate level of functional impairment, which may hinder generalization of these results.

Although BD-II is considered a less severe form of BD-I, it is known that the burden of disease does not differ between groups with respect to clinical severity, impairment, patterns of comorbidity, suicide attempts, family history, and treatment. It has also been suggested that patients with BD-II experience the same functional impairments subjects with BD-I may have. During euthymia, both subtypes present similar cognitive deficits with only subtle differences.²²22. Solé B, Bonnin CM, Mayoral M, Amann BL, Torres I, González-Pinto A, et al. Functional remediation for patients with bipolar II disorder: improvement of functioning and subsyndromal symptoms. Eur Neuropsychopharmacol. 2015;25:257-64. 23. Dittmann S, Hennig-Fast K, Gerber S, Seemüller F, Riedel M, Emanuel Severus W, et al. Cognitive functioning in euthymic bipolar I and bipolar II patients. Bipolar Disord. 2008;10:877-87.-²⁴24. Pålsson E, Figueras C, Johansson AG, Ekman CJ, Hultman B, Östlind J, et al. Neurocognitive function in bipolar disorder: a comparison between bipolar I and II disorder and matched controls. BMC Psychiatry. 2013;13:165. However, during acute depressive episodes, BD-I patients have shown more prominent cognitive impairment compared to unipolar and BD-II patients.²⁵25. Xu G, Lin K, Rao D, Dang Y, Ouyang H, Guo Y, et al. Neuropsychological performance in bipolar I, bipolar II and unipolar depression patients: a longitudinal, naturalistic study. J Affect Disord. 2012;136:328-39. This difference may be due to the fact that patients with BD-I report more psychosis than patients with BD-II.¹1. American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition, Text Revision (DSM-IV-TR). Porto Alegre: Artmed; 2002.

In brief, patients with BD experience impairments in various domains of cognition and global functioning, especially during mood episodes. However, whether severe depression confers additional cognitive and global functioning burdens in this population is unknown. To date, there have been no systematic reports describing neurocognitive profiles in relation to global functioning among BD patients with moderate and severe depression. We set out to study dimensions of cognition and global functioning among BD patients and paired healthy controls, with the hypothesis that cognitive and global functioning impairments would be associated with the severity of depressive symptoms in BD-I and BD-II patients with depression. In addition, we expected that patients with severe bipolar depression would exhibit worse cognitive impairment and global functioning when compared to those with moderate depression.

Methods

Patients with a diagnosis of BD-I or BD-II established by the Structured Clinical Interview for DSM-IV Axis I Disorders (SCID-I), between the ages of 20 and 71, were assessed and compared with healthy controls. Eligible patients were required to be experiencing a moderate to severe depressive episode, as determined by a minimum Montgomery-Åsberg Depression Rating Scale (MADRS) score of 12. We further subdivided the patients by severity of major depressive episode into severe and moderate subsets, based on the group median MADRS score. Although this has limitations, we believe it is a reasonable method for achieving a balance between having a high-scoring group and preserving maximum power. The SCID-I and MADRS were administered by experienced psychiatrists. Patients with intellectual disability, defined as an intelligence quotient (IQ) < 70 on the basis of estimates of intellectual functioning measured using the block design and vocabulary subtests of the Wechsler Intelligence Scale for Adults, 3rd edition (WAIS-III), were excluded, as were those with severe clinical illnesses (detected during clinical interviews or during review of medical records).

Controls were selected among blood donors attending a donation center or among chaperones of patients seen at other (non-psychiatric) outpatient units of Hospital de Clínicas de Porto Alegre (HCPA), Brazil; paired by age and sex; and screened using the SCID-I. Subjects with psychiatric symptoms and those who reported having first-degree relatives diagnosed with BD, schizophrenia, or other psychotic disorders were excluded.

The study protocol was approved by the HCPA Ethics Committee, and all participants signed an informed consent form prior to their inclusion in the study.

Assessment

Cognitive functioning was assessed using the WAIS-III digit span subtest²⁶26. Nascimento E. Adaptação, validação e normatização do WAIS-III para uma amostra brasileira. In: Wechsler D. WAIS-III: Manual para administração e avaliação. São Paulo: Casa do Psicólogo; 2004. p. 161-92. (both forward and backward). This test was chosen because it is established in the literature as a means of assessing attention and auditory working memory,²⁷27. Lera-Miguel S, Andres-Perpina S, Fatjo-Vilas M, Fanana L, Lazaro L. Two-year follow-up of treated adolescents with early-onset bipolar disorder: changes in neurocognition. J Affect Disord. 2014;172C:48-54. skills often impaired in BD. WAIS-III is fully validated in Brazil and has been standardized in our neuropsychiatric battery.²⁶26. Nascimento E. Adaptação, validação e normatização do WAIS-III para uma amostra brasileira. In: Wechsler D. WAIS-III: Manual para administração e avaliação. São Paulo: Casa do Psicólogo; 2004. p. 161-92. We also used the categories completed and perseverative errors parameters of the Wisconsin Card Sorting Test (WCST). This test has been also adapted and standardized to Brazilian Portuguese and can be used with children and adults.²⁸28. Heaton RK, Chelune GJ, Talley JL. Teste Wisconsin de classificação de cartas. São Paulo: Casa do Psicólogo; 1981. WCST and the WAIS-III digit span subtest evaluate executive function (working memory). Impairment in this cognitive domain has been reported as very relevant, and has been indicated by the International Society for Bipolar Disorders (ISBD) as a primary focus of research in patients with BD.²⁹29. Yatham LN, Torres IJ, Malhi GS, Frangou S, Glahn DC, Bearden CE, et al. The International Society for Bipolar Disorders-Battery For Assessment Of Neurocognition (ISBD-BANC). Bipolar Disord. 2010;12:351-63.

Global functioning was assessed using the Functioning Assessment Short Test (FAST). This instrument was developed to evaluate functional impairment and has been validated in patients with BD, showing excellent test-retest reliability and internal consistency, with a Cronbach’s alpha coefficient of 0.95 for the whole scale and excellent test-retest agreement for total FAST scores (r = 0.90; p < 0.001).³⁰30. Cacilhas AA, Magalhaes PV, Cereser KM, Walz JC, Weyne F, Rosa AR, et al. Validity of a short functioning test (FAST) in Brazilian outpatients with bipolar disorder. Value Health. 2009;12:624-7.,³¹31. Cacilhas AA, Magalhaes PV, Cereser KM, Walz JC, Weyne F, Rosa AR, et al. Bipolar disorder and age-related functional impairment. Rev Bras Psiquiatr. 2009;31:354-7. Previous studies have shown that patients with BD have lower FAST functioning scores compared with healthy controls, and that functional impairment is age-related in patients with BD.³¹31. Cacilhas AA, Magalhaes PV, Cereser KM, Walz JC, Weyne F, Rosa AR, et al. Bipolar disorder and age-related functional impairment. Rev Bras Psiquiatr. 2009;31:354-7.

Statistical analysis

Cognitive and global functioning variables were normalized with a Box-Cox data transformation³²32. Peltier MR, Wilcox CJ, Sharp DC. Technical note: application of the Box-Cox data transformation to animal science experiments. J Anim Sci. 1998;76:847-9. to enable use of parametric analyses. Analysis of variance (ANOVA) was used to compare group differences (BD vs. control and severe vs. moderate depression scores) in means. Chi-square tests were used to compare categorical group differences, and Pearson’s coefficient was used for correlations. A normal distribution could not be achieved for functioning scores, which were thus analyzed with nonparametric tests. Comparisons between mean results were adjusted for gender, the only variable significantly different between patients and controls. Effect sizes are described using Hedges’ g.³³33. Nakagawa S, Cuthill IC. Effect size, confidence interval and statistical significance: a practical guide for biologists. Biol Rev Camb Philos Soc. 2007;82:591-605. Results were considered statistically significant when p < 0.05 (two-tailed). As this is an exploratory investigation, an adjustment for multiple comparisons was not undertaken.

Results

A total of 100 patients with bipolar depression and 70 healthy controls were included in the sample. Sociodemographic and clinical characteristics of the sample are shown in Table 1. The median MADRS score in the BD group was 27; this score was used as a cutoff point to distinguish between moderate and severe depression.

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Table 1
Characteristics of the sample

Patients with bipolar depression showed worse working memory scores when compared with controls (F₁ = 3.93, p = 0.049). Executive functioning was also impaired in patients, who had a higher number of perseverative errors (F₁ = 10.66, p = 0.002), and a lower number of categories completed (F₁ = 3.92, p = 0.049) in the WCST compared with healthy controls. When patients were divided by median MADRS score (cutoff score = 27), the effect sizes of this difference were greater in patients with severe depression (Figure 1). Among patients with bipolar depression, no differences between severity groups were observed in use of lithium, other mood stabilizers, typical or atypical antipsychotics, benzodiazepines, or antidepressants.

Figure 1
Comparison between healthy controls, patients with moderate depression, and patients with severe depression in domains of cognition.

Global functioning scores were significantly different between patients and controls (z = 10.11, p < 0.001). Patients with severe depression showed greater impairment of global functioning than did those with moderate depression (z = 2.54, p = 0.011). Lower global functioning was associated with lower scores on the digit span scale (r = -0.200, p = 0.010), fewer categories completed (r = -0.210, p = 0.007), and more frequent perseverative errors (r = 0.293, p < 0.001). These associations were observed only in patients with severe depression (Figure 2).

Figure 2
Correlations between domains of cognition and functioning. The y axis represents functioning as measured by the Functioning Assessment Short Test (FAST; the higher the score, the poorer the functioning); the x axis represents standardized scores.

Discussion

The present study investigated cognition and global functioning in a group of patients with bipolar depression compared with healthy controls. Our main findings include impairment of global functioning among BD patients with severe depression and an association between lower global functioning and cognitive impairment in patients with severe depression. Our findings also confirmed previous research suggesting impairments in working memory and executive function among BD patients with depression when compared with healthy controls. The effect size of the differences in executive function was greater in patients with severe depression than in patients with moderate depression.

The present data also add to the notion that cognitive performance among bipolar patients varies as a function of the severity of depression, especially because only patients with severe depression showed impairment in executive function and working memory compared to healthy controls. The results of this study confirm previous findings that showed a role of depressive symptoms and cognitive impairment in global functioning in BD patients, and highlight the fact that depressive symptoms also affect cognitive performance.²¹21. Bonnín Cdel M, González-Pinto A, Solé B, Reinares M, González-Ortega I, Alberich S, et al. Verbal memory as a mediator in the relationship between subthreshold depressive symptoms and functional outcome in bipolar disorder. J Affect Disord. 2014;160:50-4. Our results are also partially consistent with a study by Bonnin et al.,³⁴34. Bonnin CM, Sanchez-Moreno J, Martinez-Aran A, Sole B, Reinares M, Rosa AR, et al. Subthreshold symptoms in bipolar disorder: impact on neurocognition, quality of life and disability. J Affect Disord. 2012;136:650-9. which showed that patients exhibiting low levels of subthreshold symptomatology (Hamilton Depression Rating Scale [HDRS] ≤ 3 and Young Mania Rating Scale [YMRS] ≤ 2), defined as asymptomatic, and those with higher levels of subthreshold symptomatology (HDRS ≥ 4 and YMRS ≥ 3), defined as subsyndromic, both scored low on cognitive measures when compared to healthy controls. The subsyndromic group also had poorer functional outcomes than the asymptomatic group and healthy controls. In our sample, patients showed impairment in executive function and working memory compared to healthy controls, and patients with higher MADRS scores also exhibited impairment in executive function and working memory as compared to those patients with lower MADRS scores. These findings and those of the aforementioned studies help clarify the role of depressive symptoms in global functioning and cognitive performance, and especially in executive function. Our hypothesis is that executive function impairment can cause loss of adaptive plasticity and ineffective responses of perseverance, which, in turn, may impact global functionality and intensify depressive symptoms.²⁰20. Van Rheenen TE, Rossell SL. Objective and subjective psychosocial functioning in bipolar disorder: an investigation of the relative importance of neurocognition, social cognition and emotion regulation. J Affect Disord. 2014;162:134-41.

These findings also can be interpreted in light of the potential impact of impaired attention, concentration, and flexibility as observed in these patients - abilities that are necessary to successfully engage in social and work interactions and to achieve adequate functional performance.¹¹11. Malhi GS, Ivanovski B, Hadzi-Pavlovic D, Mitchell PB, Vieta E, Sachdev P. Neuropsychological deficits and functional impairment in bipolar depression, hypomania and euthymia. Bipolar Disord. 2007;9:114-25. Furthermore, functional impairments are considered potential indicators of the chronicity and deterioration observed in BD.³⁵35. Rosa AR, Magalhães PV, Czepielewski L, Sulzbach MV, Goi PD, Vieta E, et al. Clinical staging in bipolar disorder: focus on cognition and functioning. J Clin Psychiatry. 2014;75:e450-6. However, in the present study, functional impairment was associated with deficits in working memory and executive function only in patients with severe depression. This finding may point to a possible heterogeneity of the mechanisms underlying functional impairment in BD.

A limitation of the present study is the fact that only patients experiencing a depressive episode were assessed. Future studies are warranted to investigate alterations specifically related with different phases of illness. Another important limitation is that duration of illness was not assessed in the protocol, which precluded investigation of whether cognitive impairment would be associated with the late stages of BD, as previously reported.³⁵35. Rosa AR, Magalhães PV, Czepielewski L, Sulzbach MV, Goi PD, Vieta E, et al. Clinical staging in bipolar disorder: focus on cognition and functioning. J Clin Psychiatry. 2014;75:e450-6. FAST is a valid instrument for evaluation of functioning in patients with BD.³⁰30. Cacilhas AA, Magalhaes PV, Cereser KM, Walz JC, Weyne F, Rosa AR, et al. Validity of a short functioning test (FAST) in Brazilian outpatients with bipolar disorder. Value Health. 2009;12:624-7.,³¹31. Cacilhas AA, Magalhaes PV, Cereser KM, Walz JC, Weyne F, Rosa AR, et al. Bipolar disorder and age-related functional impairment. Rev Bras Psiquiatr. 2009;31:354-7. However, it poses some limitations, such as the limited number of questions and the fact it is rated by a clinician. Another major limitation is that, as all patients were experiencing a depressive episode, their depressive symptoms may have affected vigilance and engagement during the cognitive assessment, thus impairing cognitive performance. Finally, the cross-sectional design of the study prevents the establishment of a causal relationship between global functioning and cognitive deficits. Cohort studies are needed to provide stronger evidence and establish whether such relationships exist. Strengths of the present study include the fact that results were not impacted by age or educational attainment in the comparisons between BD patients and controls, or by use of psychiatric medication between BD severity subgroups.

In summary, the present study demonstrated an association between severity of depressive symptoms and variation in global functioning and cognition, especially in working memory and executive function, among patients with bipolar depression. Within this context, an assessment of the pattern of cognitive performance and of its impact on global functioning may help improve treatment planning for patients with bipolar depression.

Acknowledgements

This study was partially funded by the Stanley Medical Research Institute. AR receives grants from Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq), Programa Ciência sem Fronteiras, Bolsa Atração de Jovens Talentos, Academia Brasileira de Ciências, and the Brazilian Commission of the L’Oréal-UNESCO For Women in Science program. CSG has received grant/research support from CNPq, Fundação de Amparo à Pesquisa do Estado do Rio Grande do Sul (FAPERGS), Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP), and Fundo de Incentivo à Pesquisa - Hospital de Clínicas de Porto Alegre (FIPE-HCPA).

References

¹
American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition, Text Revision (DSM-IV-TR). Porto Alegre: Artmed; 2002.
²
Chaves OC, Lombardo LE, Bearden CE, Woolsey MD, Martinez DM, Barrett JA, et al. Association of clinical symptoms and neurocognitive performance in bipolar disorder: a longitudinal study. Bipolar Disord. 2011;13:118-23.
³
Hellvin T, Sundet K, Simonsen C, Aminoff SR, Lagerberg TV, Andreassen OA, et al. Neurocognitive functioning in patients recently diagnosed with bipolar disorder. Bipolar Disord. 2012;14:227-38.
⁴
Leboyer M, Kupfer DJ. Bipolar disorder: new perspectives in health care and prevention. J Clin Psychiatry. 2010;71:1689-95.
⁵
Mann-Wrobel MC, Carreno JT, Dickinson D. Meta-analysis of neuropsychological functioning in euthymic bipolar disorder: an update and investigation of moderator variables. Bipolar Disord. 2011;13:334-42.
⁶
Torres IJ, Boudreau VG, Yatham LN. Neuropsychological functioning in euthymic bipolar disorder: a meta-analysis. Acta Psychiatr Scand Suppl. 2007;434:17-26.
⁷
MacQueen GM, Young LT, Joffe RT. A review of psychosocial outcome in patients with bipolar disorder. Acta Psychiatr Scand. 2001;103:163-70.
⁸
Strejilevich SA, Martino DJ, Murru A, Teitelbaum J, Fassi G, Marengo E, et al. Mood instability and functional recovery in bipolar disorders. Acta Psychiatr Scand. 2013;128:194-202.
⁹
Robinson LJ, Thompson JM, Gallagher P, Goswami U, Young AH, Ferrier IN, et al. A meta-analysis of cognitive deficits in euthymic patients with bipolar disorder. J Affect Disord. 2006;93:105-15.
¹⁰
Iosifescu DV. The relation between mood, cognition and psychosocial functioning in psychiatric disorders. Eur Neuropsychopharmacol. 2012;22:S499-504.
¹¹
Malhi GS, Ivanovski B, Hadzi-Pavlovic D, Mitchell PB, Vieta E, Sachdev P. Neuropsychological deficits and functional impairment in bipolar depression, hypomania and euthymia. Bipolar Disord. 2007;9:114-25.
¹²
Martinez-Aran A, Vieta E, Colom F, Torrent C, Sanchez-Moreno J, Reinares M, et al. Cognitive impairment in euthymic bipolar patients: implications for clinical and functional outcome. Bipolar Disord. 2004;6:224-32.
¹³
Sachs G, Schaffer M, Winklbaur B. [Cognitive deficits in bipolar disorder]. Neuropsychiatr. 2007;21:93-101.
¹⁴
Keefe RS, Fox KH, Davis VG, Kennel C, Walker TM, Burdick KE, et al. The Brief Assessment of Cognition In Affective Disorders (BAC-A): performance of patients with bipolar depression and healthy controls. J Affect Disord. 2014;166:86-92.
¹⁵
Depp CA, Mausbach BT, Harmell AL, Savla GN, Bowie CR, Harvey PD, et al. Meta-analysis of the association between cognitive abilities and everyday functioning in bipolar disorder. Bipolar Disord. 2012;14:217-26.
¹⁶
Harvey PD, Wingo AP, Burdick KE, Baldessarini RJ. Cognition and disability in bipolar disorder: lessons from schizophrenia. Bipolar Disord. 2010;12:364-75.
¹⁷
Buoli M, Caldiroli A, Caletti E, Zugno E, Altamura AC. The impact of mood episodes and duration of illness on cognition in bipolar disorder. Compr Psychiatry. 2014;55:1561-6.
¹⁸
Martínez-Arán A, Vieta E, Reinares M, Colom F, Torrent C, Sánchez-Moreno J, et al. Cognitive function across manic or hypomanic, depressed, and euthymic states in bipolar disorder. Am J Psychiatry. 2004;161:262-70.
¹⁹
Lawrence C, Roy A, Harikrishnan V, Yu S, Dabbous O. Association between severity of depression and self-perceived cognitive difficulties among full-time employees. Prim Care Companion CNS Disord. 2013;15(3). pii: PCC.12m01469.
²⁰
Van Rheenen TE, Rossell SL. Objective and subjective psychosocial functioning in bipolar disorder: an investigation of the relative importance of neurocognition, social cognition and emotion regulation. J Affect Disord. 2014;162:134-41.
²¹
Bonnín Cdel M, González-Pinto A, Solé B, Reinares M, González-Ortega I, Alberich S, et al. Verbal memory as a mediator in the relationship between subthreshold depressive symptoms and functional outcome in bipolar disorder. J Affect Disord. 2014;160:50-4.
²²
Solé B, Bonnin CM, Mayoral M, Amann BL, Torres I, González-Pinto A, et al. Functional remediation for patients with bipolar II disorder: improvement of functioning and subsyndromal symptoms. Eur Neuropsychopharmacol. 2015;25:257-64.
²³
Dittmann S, Hennig-Fast K, Gerber S, Seemüller F, Riedel M, Emanuel Severus W, et al. Cognitive functioning in euthymic bipolar I and bipolar II patients. Bipolar Disord. 2008;10:877-87.
²⁴
Pålsson E, Figueras C, Johansson AG, Ekman CJ, Hultman B, Östlind J, et al. Neurocognitive function in bipolar disorder: a comparison between bipolar I and II disorder and matched controls. BMC Psychiatry. 2013;13:165.
²⁵
Xu G, Lin K, Rao D, Dang Y, Ouyang H, Guo Y, et al. Neuropsychological performance in bipolar I, bipolar II and unipolar depression patients: a longitudinal, naturalistic study. J Affect Disord. 2012;136:328-39.
²⁶
Nascimento E. Adaptação, validação e normatização do WAIS-III para uma amostra brasileira. In: Wechsler D. WAIS-III: Manual para administração e avaliação. São Paulo: Casa do Psicólogo; 2004. p. 161-92.
²⁷
Lera-Miguel S, Andres-Perpina S, Fatjo-Vilas M, Fanana L, Lazaro L. Two-year follow-up of treated adolescents with early-onset bipolar disorder: changes in neurocognition. J Affect Disord. 2014;172C:48-54.
²⁸
Heaton RK, Chelune GJ, Talley JL. Teste Wisconsin de classificação de cartas. São Paulo: Casa do Psicólogo; 1981.
²⁹
Yatham LN, Torres IJ, Malhi GS, Frangou S, Glahn DC, Bearden CE, et al. The International Society for Bipolar Disorders-Battery For Assessment Of Neurocognition (ISBD-BANC). Bipolar Disord. 2010;12:351-63.
³⁰
Cacilhas AA, Magalhaes PV, Cereser KM, Walz JC, Weyne F, Rosa AR, et al. Validity of a short functioning test (FAST) in Brazilian outpatients with bipolar disorder. Value Health. 2009;12:624-7.
³¹
Cacilhas AA, Magalhaes PV, Cereser KM, Walz JC, Weyne F, Rosa AR, et al. Bipolar disorder and age-related functional impairment. Rev Bras Psiquiatr. 2009;31:354-7.
³²
Peltier MR, Wilcox CJ, Sharp DC. Technical note: application of the Box-Cox data transformation to animal science experiments. J Anim Sci. 1998;76:847-9.
³³
Nakagawa S, Cuthill IC. Effect size, confidence interval and statistical significance: a practical guide for biologists. Biol Rev Camb Philos Soc. 2007;82:591-605.
³⁴
Bonnin CM, Sanchez-Moreno J, Martinez-Aran A, Sole B, Reinares M, Rosa AR, et al. Subthreshold symptoms in bipolar disorder: impact on neurocognition, quality of life and disability. J Affect Disord. 2012;136:650-9.
³⁵
Rosa AR, Magalhães PV, Czepielewski L, Sulzbach MV, Goi PD, Vieta E, et al. Clinical staging in bipolar disorder: focus on cognition and functioning. J Clin Psychiatry. 2014;75:e450-6.

Corrigendum

We hereby inform that there was an error in the indexing of the 10th author’s name in the manuscript entitled “Cognition and functioning in bipolar depression” (doi: http://dx.doi.org/10.1590/1516-4446-2014-1558), by Natalia S. Kapczinski et al., published ahead of print in this journal: “Gabriel Fries” (Fries G) should read “Gabriel R. Fries” (Fries GR). This is how the letter should be cited: Kapczinski NS, Narvaez JC, Magalhaães PV, Bücker J, Peuker AC, Loredo AC, Troiano F, Czepielewski L, Rosa A, Fries GR, Gama CS. Cognition and functioning in bipolar depression. Rev Bras Psiquiatr. 2016 Feb 5. [Epub ahead of print]. http://dx.doi.org/10.1590/1516-4446-2014-1558.

Publication Dates

Publication in this collection
02 May 2016
Date of issue
Jul-Sep 2016

History

Received
10 Sept 2014
Accepted
29 Apr 2015

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

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	Bipolar depression (n=100)	Controls (n=70)
Age, mean ± SD	42.3±10.1	41.4±13.1
Female sex, %^* * p < 0.05.	78	64
Years of education, mean (range)	11 (9-14)	12 (8-15)
MADRS, mean ± SD	27.4±7.8	N/A
YMRS, mean (range)	0 (0-2)	N/A
Type I bipolar disorder, %	68	N/A
Current treatment, %
Lithium	52
Other mood stabilizers	59
Atypical antipsychotics	16
Typical antipsychotics	12
Antidepressants	20
Benzodiazepines	43