Hostname: page-component-8448b6f56d-m8qmq Total loading time: 0 Render date: 2024-04-24T10:34:21.031Z Has data issue: false hasContentIssue false
  • English
  • Français

Does bipolar disorder have a benign course?

Published online by Cambridge University Press:  16 September 2016

Osvaldo P. Almeida
Osvaldo P. Almeida*
Affiliation:
School of Psychiatry & Clinical Neurosciences and Western Australian Centre for Health & Ageing, University of Western Australia Department of Psychiatry, Royal Perth Hospital and Bentley Mental Health Services for Older Adults Perth, Western Australia, Australia Email: osvaldo.almeida@uwa.edu.au
Rights & Permissions [Opens in a new window]

Extract

Written records have been describing extreme states of emotions since ancient Greece (Angst and Marneros, 2001), but Aretaeus of Cappadocia (which is geographically located in modern Turkey) was probably the first to outline the close relationship between depression and mania nearly 2000 years ago: “I think that melancholia is the beginning and a part of mania. . . The development of mania is really a worsening of the disease rather than a change into another disease. . . In most of them the sadness became better after various lengths of time and changed into happiness; the patients then developed a mania” (Angst and Marneros, 2001). Limited progress in our understanding of these extreme states of affect occurred until the mid-1800s, when both German and French physicians suggested that the change from melancholia to mania was not only “usual,” but that the continuous cycle between depression, mania, and disease free intervals were the key features of a mental disorder. Jean Pierre Falret named the disorder “folie circulaire” (1851), while Jules Baillarger called it “folie a double-form” (1854).

Type
Guest Editorial
Information
International Psychogeriatrics , Volume 28 , Issue 11 , November 2016 , pp. 1755 - 1757
Copyright
Copyright © International Psychogeriatric Association 2016 

Written records have been describing extreme states of emotions since ancient Greece (Angst and Marneros, Reference Angst and Marneros2001), but Aretaeus of Cappadocia (which is geographically located in modern Turkey) was probably the first to outline the close relationship between depression and mania nearly 2000 years ago: “I think that melancholia is the beginning and a part of mania. . . The development of mania is really a worsening of the disease rather than a change into another disease. . . In most of them the sadness became better after various lengths of time and changed into happiness; the patients then developed a mania” (Angst and Marneros, Reference Angst and Marneros2001). Limited progress in our understanding of these extreme states of affect occurred until the mid-1800s, when both German and French physicians suggested that the change from melancholia to mania was not only “usual,” but that the continuous cycle between depression, mania, and disease free intervals were the key features of a mental disorder. Jean Pierre Falret named the disorder “folie circulaire” (1851), while Jules Baillarger called it “folie a double-form” (1854). Karl Kahlbaum, working in Germany, supported the French concept of “circular insanity” and his work played a key role in the classification of mental disorders put forward by Emil Kraepelin, which separated manic-depressive insanity from dementia praecox, paranoia, and paraphrenia (Angst and Marneros, Reference Angst and Marneros2001). According to Kraepelin, manic-depressive insanity was characterized by periods of melancholia, mania, and normal function. The concept of manic-depressive insanity evolved into that of bipolar disorder and was later incorporated into the Diagnostic and Statistical Manual of Mental Disorders (DSM) and the International Classification of Mental Disorders (ICD). At present, the diagnosis of bipolar disorder requires a current or past episode of mania or mixed state, and the assurance that the changes in mood are not due to other conditions such as schizophrenia (or dementia praecox, as Kraepelin called it) or other psychotic disorders. The underlying assumption of the modern concept of bipolar disorder is that the condition is characterized by nothing else but the episodes of mania and depression.

Function between mood episodes in people with bipolar disorder

In the late 1990s, several research papers described findings indicating that euthymic adults with bipolar disorder showed evidence of subtle impairments in cognitive function (Ferrier et al., Reference Ferrier, Stanton, Kelly and Scott1999). The concern, in this case, was that these cognitive deficits could potentially compromise the function of patients between the episodes of mood disturbance. Ten years ago, an American study followed adolescents presenting with their first ever hospital admission with mania or a mixed episode (DelBello et al., Reference DelBello, Hanseman, Adler, Fleck and Strakowski2007). The investigators found that about 50% of participants experienced syndromic recovery within 12–16 weeks and 86% within one year. In contrast, only about 17% of participants experienced functional recovery during the initial 12–16 weeks following admission and 43% by the end of one year (DelBello et al., Reference DelBello, Hanseman, Adler, Fleck and Strakowski2007). In other words, nearly 60% of the adolescents with bipolar disorder in this study failed to regain full functional capacity during the year following their first ever admission to hospital. Subsequently, a cross-sectional study that used the Functioning Assessment Short Test (FAST) found that 60% of the 71 euthymic adults with bipolar disorder were functionally impaired compared with 13% of the controls (Rosa et al., Reference Rosa2009), suggesting that the typical “disease free interval” of bipolar disorder may not necessarily be “impairment free.”

Cognitive function in bipolar disorder, and the risk of dementia and death

A recent meta-analysis of individual patient data compared the performance of euthymic adults with bipolar disorder with that of controls on 11 cognitive measures derived from tests of verbal learning, trail making, digit span, and/or the Wisconsin Card Sorting Test (Bourne et al., Reference Bourne2013). Bipolar disorder was associated with impairments in all measures, even after the analyses were controlled for the possible confounding effects of age, gender, and premorbid intelligence (Bourne et al., Reference Bourne2013). The authors of this meta-analysis also noticed that some cognitive deficits were associated with illness severity, and suggested that they seemed to track the progression of the disorder (Bourne et al., Reference Bourne2013). This raises the question of whether the cognitive and functional deficits observed among euthymic people with bipolar disorder are progressive in nature and may ultimately lead to the development of dementia.

We have recently reported the results of a population-based longitudinal study of men who were aged 65–85 years in 1996. Participants were free of dementia at the beginning of the follow-up period of 12 years (Almeida et al., Reference Almeida2016b). Of the 37,768 participants, 256 (0.7%) had a recorded diagnosis of bipolar disorder. Compared with other participants, men with bipolar disorder had five times greater prevalence of alcohol-related disorders and 70% greater odds of other substance use disorder (Almeida et al., Reference Almeida2016b). The hazard ratio of dementia during follow-up was 2.6 times greater in men with than without bipolar disorder (95% confidence interval: 2.0 to 3.3), and this increase in risk remained even after the analyses were adjusted for age and use of substances, and when death was used as a competing risk (Almeida et al., Reference Almeida2016b). The risk of dementia was particularly high for men with recent (i.e. < 5 years) history of bipolar disorder, suggesting that changes in the regulation of affect in later life may herald, in at least some cases, the early stages of dementia. A similarly high risk of dementia was observed among men with a longstanding history (i.e. ≥ 15 years), implying that prolonged exposure to the physiological concomitants of bipolar disorder may facilitate neuronal loss and the development of dementia (Moorhead et al., Reference Moorhead2007). Consistent with this idea, a Danish case-register study found that the risk of dementia in bipolar disorder increased with the number of affective episodes (Kessing and Andersen, Reference Kessing and Andersen2004), and was less marked among patients receiving continuous treatment with lithium (but not with other mood stabilizers) (Kessing et al., Reference Kessing, Forman and Andersen2010).

Bipolar disorder has also been associated with increased mortality (Almeida et al., Reference Almeida, Hankey, Yeap, Golledge, Norman and Flicker2014), including death by suicide (Schaffer et al., Reference Schaffer2015). A systematic review and meta-analysis of 31 studies that included over 300,000 people with bipolar disorder found that the condition more than doubled the risk of premature death both from natural and non-natural causes (such as suicide or accidents) (Hayes et al., Reference Hayes, Miles, Walters, King and Osborn2015).

Bipolar disorder: preparing for the future

One of the features that separated Kraepelin's manic-depressive illness (bipolar disorder) from dementia praecox (schizophrenia) was the recovery of function and absence of residual symptoms between episodes. However, recent data suggest that the euthymic periods are not entirely free of impairments, and that the long-term outcome of people with bipolar disorder is, in at least some cases, associated with cognitive deficits, poor function, and increased risk of dementia and death (Kessing et al., Reference Kessing, Olsen, Mortensen and Andersen1999; Bourne et al., Reference Bourne2013; Almeida et al., Reference Almeida, Hankey, Yeap, Golledge, Norman and Flicker2014; Almeida et al., Reference Almeida2016b).

The underlying causes associated with this restricted prognosis of bipolar disorder are not well understood, but could include lifestyle choices, concurrent comorbidities, psychosocial adversity, and sub-optimal access to supportive health services. Regardless of the causes, it is clear that the management of bipolar disorder should not be limited to the acute treatment of the affective episodes, particularly if we wish to improve the long-term outlook and function of these patients as they move toward old age.

As the world's population ages, mental health services for older adults will be responsible for the care on an increasingly larger number of people with bipolar disorder – these services should become actively engaged in the development of effective strategies to improve the clinical outcome of these patients. We will need to progress our understanding of the factors that mediate the age of onset of illness, the overlap between bipolar disorder and dementia in later life, as well as the protective and deleterious risk factors associated with good and poor functional outcomes. In practice, this will probably require the establishment of national and international collaborative networks that follow similar protocols for assessment, modification of risk factors (for example, Almeida et al., Reference Almeida, Hankey, Yeap, Golledge, McCaul and Flicker2013; Almeida et al., Reference Almeida, McCaul, Hankey, Yeap, Golledge and Flicker2016a), and treatment of adults with bipolar disorder (Sajatovic et al., Reference Sajatovic2015; Dols et al., Reference Dols2016). It is time to get moving!

Conflict of interest

None.

Funding

None.

References

Almeida, O. P., Hankey, G. J., Yeap, B. B., Golledge, J., McCaul, K. and Flicker, L. (2013). A risk table to assist health practitioners assess and prevent the onset of depression in later life. Preventive Medicine, 57, 878882.CrossRefGoogle ScholarPubMed
Almeida, O. P., Hankey, G. J., Yeap, B. B., Golledge, J., Norman, P. E. and Flicker, L. (2014). Mortality among people with severe mental disorders who reach old age: a longitudinal study of a community-representative sample of 37,892 men. PLoS One, 9, e111882.CrossRefGoogle Scholar
Almeida, O. P., McCaul, K., Hankey, G. J., Yeap, B. B., Golledge, J. and Flicker, L. (2016a). Risk of dementia and death in community-dwelling older men with bipolar disorder. British Journal of Psychiatry, 209, 121126 CrossRefGoogle ScholarPubMed
Almeida, O. P. et al. (2016b). Reducing depression during the menopausal transition with health coaching: results from the healthy menopausal transition randomised controlled trial. Maturitas, 92, 4148.CrossRefGoogle ScholarPubMed
Angst, J. and Marneros, A. (2001). Bipolarity from ancient to modern times: conception, birth and rebirth. Journal of Affective Disorders, 67, 319.CrossRefGoogle ScholarPubMed
Bourne, C. et al. (2013). Neuropsychological testing of cognitive impairment in euthymic bipolar disorder: an individual patient data meta-analysis. Acta Psychiatrica Scandinavica, 128, 149162.CrossRefGoogle ScholarPubMed
DelBello, M. P., Hanseman, D., Adler, C. M., Fleck, D. E. and Strakowski, S. M. (2007). Twelve-month outcome of adolescents with bipolar disorder following first hospitalization for a manic or mixed episode. American Journal of Psychiatry, 164, 582590.CrossRefGoogle ScholarPubMed
Dols, A. et al. (2016). Do current national and international guidelines have specific recommendations for older adults with bipolar disorder? A brief report. International Journal of Geriatric Psychiatry. doi:10.1002/gps.4534.CrossRefGoogle ScholarPubMed
Ferrier, I. N., Stanton, B. R., Kelly, T. P. and Scott, J. (1999). Neuropsychological function in euthymic patients with bipolar disorder. British Journal of Psychiatry, 175, 246251.CrossRefGoogle ScholarPubMed
Hayes, J. F., Miles, J., Walters, K., King, M. and Osborn, D. P. (2015). A systematic review and meta-analysis of premature mortality in bipolar affective disorder. Acta Psychiatrica Scandinavica, 131, 417425.CrossRefGoogle ScholarPubMed
Kessing, L. V. and Andersen, P. K. (2004). Does the risk of developing dementia increase with the number of episodes in patients with depressive disorder and in patients with bipolar disorder?. Journal of Neurology Neurosurgery & Psychiatry, 75, 16621666.CrossRefGoogle ScholarPubMed
Kessing, L. V., Forman, J. L. and Andersen, P. K. (2010). Does lithium protect against dementia?. Bipolar Disorder, 12, 8794.CrossRefGoogle ScholarPubMed
Kessing, L. V., Olsen, E. W., Mortensen, P. B. and Andersen, P. K. (1999). Dementia in affective disorder: a case-register study. Acta Psychiatrica Scandinavica, 100, 176185.CrossRefGoogle ScholarPubMed
Moorhead, T. W. et al. (2007). Progressive gray matter loss in patients with bipolar disorder. Biological Psychiatry, 62, 894900.CrossRefGoogle ScholarPubMed
Rosa, A. R. et al. (2009). Clinical predictors of functional outcome of bipolar patients in remission. Bipolar Disorder, 11, 401409.CrossRefGoogle ScholarPubMed
Sajatovic, M. et al. (2015). A report on older-age bipolar disorder from the international society for bipolar disorders task force. Bipolar Disorder, 17, 689704.CrossRefGoogle ScholarPubMed
Schaffer, A. et al. (2015). International society for bipolar disorders task force on suicide: meta-analyses and meta-regression of correlates of suicide attempts and suicide deaths in bipolar disorder. Bipolar Disorder, 17, 116.CrossRefGoogle ScholarPubMed