It is well known that stroke is among the most common causes of disability in adults. Less well recognized, however, is how common psychiatric disorders are after stroke.

Poststroke Depression

According to the American Heart Association and American Stroke Association, poststroke depression affects approximately one-third of people after they have a stroke,1 with a peak incidence 3 to 6 months after stroke. A significant proportion of individuals with poststroke depression are undiagnosed or inadequately treated. Unfortunately, unrecognized psychiatric disorders are associated with a variety of poor outcomes, including but not limited to higher rates of mortality, long-term disability, hospital readmissions, and use of outpatient services.


The presumed pathophysiology of poststroke psychiatric disorders is complex, likely involving both biologic and environmental factors.1 Risk factors may include stroke severity (eg, whether there are impairments to activities of daily living, cognitive impairment, or social functioning, which can all be affected by aphasia when present. Other risk factors are genetics, previous history of depression and/or anxiety, and certain medications. In contrast, age and sex do not appear to be risk factors, nor is lesion location. Differences in study techniques regarding these factors limit generalizability to the population as a whole, and more research is needed.1

Screening and Diagnosis

Regardless of risk factors, some guidelines, such as the Canadian Stroke Best Practice Recommendations2 recommend that all persons who had a stroke be screened for depressive symptoms. The reasoning for this recommendation is the high prevalence of depression poststroke, a need for screening to detect depression, and strong evidence for the benefits of treating poststroke depression. Screening should be done with a validated tool and may take place at various stages throughout the continuum of stroke care, particularly at transition points (eg, transfer from an inpatient acute setting to a rehabilitation setting, before return to the community, and at follow-up appointments). The single question “Do you often feel sad or depressed?”, derived from the Personal Health Questionnaire (PHQ)-2, has a sensitivity of 86% and specificity of 78% for depression.3 When a person answers this question positively, further evaluation with the PHQ-9 should be done. For those with cognitive and/or communication impairments, other screening tools (eg, the Visual Analogue Mood Scale or Aphasia Depression Rating Scale) may be considered.


There is no definitive evidence to guide the specific choice of therapy for people with poststroke depression.1,4 Selective serotonin reuptake inhibitors (SSRIs) are commonly used as first-line treatment based on data extrapolated from the general population. Because SSRIs increase the risk of bleeding, however, they are contraindicated after a hemorrhagic stroke. If effective, SSRIs should be continued for 6 to 12 months. Potential side effects of SSRIs may include cardiovascular effects bleeding, interactions with other medications, falls, hyponatremia, and gastrointestinal disturbances, among others (Table).

Prophylactic treatment with SSRIs is not currently recommended. Studies that suggested SSRIs might have an independent positive effect on motor recovery5 have not been reproducible in larger-scale studies. A study that included more than 100 hospitals in which people who had strokes were followed for 4 to 5 years did not demonstrate any benefit on functional outcome of fluoxetine compared with placebo at 6 months.6 A study that examined citalopram’s effects on disability and mortality also did not demonstrate any benefit on functional outcome with citalopram compared with placebo at 6 months.7

Cognitive behavioral therapy (CBT) may or may not be useful for poststroke depression. Often used as a supplementary treatment to reduce feelings of helplessness, CBT targets thoughts and behaviors to improve mood. With CBT, practice focuses on increasing pleasurable activities, reducing negative thoughts, and improving assertiveness and problem-solving skills. Drawbacks include higher costs and the necessity of increased time and staff expertise. There are CBT programs specifically designed for poststroke depression (ie, the CALM trial in the United Kingdom8 or the Brainstorm program in Australia.9 For the communication-impaired, guided CBT self-help workbooks, therapists with education in art or music therapy, and mindfulness may be helpful. As adjustment issues emerge, CBT may become more effective.

Long-term Outcomes

Poststroke depression increases the risk for worse long-term outcomes, including increased mortality.1 A study of more than 1,000 patients using the Hospital Anxiety and Depression Scale (HADS) found that at 5-year follow-up, patients with a HADS score of 7 or more at 3 months poststroke had a hazard ratio of 1.41 for increased mortality compared with a normative control group.10 Other data suggests that those with poststroke depression are 3.4 times more likely to die within 10 years of a stroke than those without poststroke depression. People with few social contacts have an even more increased mortality rate.11 A few studies have also shown the negative effects poststroke depression has on quality of life as well as reduced treatment efficacy.

Other Poststroke Mood Disorders

A variety of other mood disorders can also occur more commonly after stroke.

Poststroke Anxiety

Poststroke anxiety affects approximately 20% of patients following stroke. Risk factors include comorbid poststroke depression and younger age. The HADS is a common screening tool. The SSRIs are first-line treatment, with data largely generalized from that used for generalized anxiety disorder. Psychotherapy also sometimes used. Weighing the benefit-to-risk ratio is important as there is no clear evidence-based data solely from the stroke population.

Poststroke Posttraumatic Stress Disorder

Posttraumatic stress disorder (PTSD) is also thought to affect 20% of people after stroke, and is associated with an increased risk for medication nonadherence.13 The American Psychiatric Association’s Diagnostic and Statistical Manual of Mental Disorders, 5th edition (DSM-5) defines PTSD as a “trauma and stressor-related disorder,” comprised of 4 core areas: intrusive thoughts, avoidance of triggering stimuli, negative alterations in mood and cognition, and hyperarousal.14 There have not yet been any controlled trials examining the efficacy of pharmacologic or psychotherapeutic interventions for poststroke PTSD.

Poststroke Anger

Poststroke anger proneness has been shown to affect up to 33% of people after stroke, both acutely and in the later periods following a stroke.15 Individuals can become irritable, impulsive, and hostile after stroke. They may show more aggressive behaviors including hurting others, or negative verbal behavior such as cursing or screaming, all of which can continue for years. A Cochrane review found weak evidence, based on a few small randomized controlled trials, that beta-blockers can improve aggression after acquired brain injury, but very large doses were used that are likely to produce significant adverse effects.15 For other classes of medication, randomized controlled trials have not been published, but there is reasonable anecdotal evidence (eg, case series reports) that antipsychotics, mood stabilizers, and antidepressants may also be effective.15

Poststroke Emotionalism

Poststroke emotionalism can involve easily provoked outbursts of laughter or tearfulness inappropriate to a situation with difficulty showing appropriate emotions at other times. Risk factors may include cognitive deficits and anterior lesions.16 Dextromethorphan/quinidine is approved by the Food and Drug Administration (FDA) for management of emotionalism. Tricyclic antidepressants (TCAs) and SSRIs may also be helpful as treatment, although this use is not in the FDA-approved indications.


In conclusion, poststroke mood disorders are common, disabling, underrecognized, and undertreated. Patients with these disorders are at higher risk for suboptimal recovery, recurrent vascular events, poor quality of life and mortality. More evidence-based research is required regarding optimal management. Future studies should examine pathophysiology, including relative contributions of biologic vs psychosocial factors. Large, multicenter, international randomized controlled trials should be conducted to identify safe and effective treatments for these disorders, and assess risks and benefits of routine screening to determine optimal timing, frequency, setting, and methods for diagnosis.

1. Towfighi A, Ovbiagele B, El Husseini N, et al. Poststroke depression: a scientific statement for healthcare professionals from the American Heart Association/American Stroke Association. Stroke. 2017;48(2):e30-e43.

2. Boulanger JM, Lindsay MP, Gubitz G, et al. Canadian stroke best practice recommendations for acute stroke management: prehospital, emergency department, and acute inpatient stroke care, 6th Edition, Update 2018. Int J Stroke. 2018;13(9):949-984.

3. Watkins C, Daniels L, Jack C, Dickinson H, van Den Broek M. Accuracy of a single question in screening for depression in a cohort of patients after stroke: comparative study. BMJ. 2001;323(7322):1159.

4. Hackett ML, Anderson CS, House A, Halteh C. Interventions for preventing depression after stroke. Cochrane Database Syst Rev. 2008;16(3):CD003689.

5. Chollet F, Tardy J, Albucher JF, et al. Fluoxetine for motor recovery after acute ischaemic stroke (FLAME): a randomised placebo-controlled trial. Lancet Neurol. 2011;10(2):123-130. Published correction appears in Lancet Neurol. 2011 Mar;10(3):205.

6. Kraglund KL, Mortensen JK, Grove EL, Johnsen SP, Andersen G. TALOS: a multicenter, randomized, double-blind, placebo-controlled trial to test the effects of citalopram in patients with acute stroke. Int J Stroke. 2015;10(6):985-987.

7. FOCUS Trial Collaboration. Effects of fluoxetine on functional outcomes after acute stroke (FOCUS): a pragmatic, double-blind, randomised, controlled trial. Lancet. 2019;393(10168):265-274.

8. Thomas SA, Walker MF, Macniven JA, Haworth H, Lincoln NB. Communication and low mood (CALM): a randomized controlled trial of behavioural therapy for stroke patients with aphasia. Clin Rehabil. 2013;27(5):398-408.

9. Ward SK, Turner A, A Hambridge J, et al. Group cognitive behavioural therapy for stroke survivors with depression and their carers. Top Stroke Rehabil. 2016;23(5):358-365.

10. Ayerbe L, Ayis S, Crichton SL, Rudd AG, Wolfe CD. Explanatory factors for the increased mortality of stroke patients with depression. Neurology. 2014;83(22):2007-2012.

11. Morris PL, Robinson RG, Andrzejewski P, Samuels J, Price TR. Association of depression with 10-year poststroke mortality. Am J Psychiatry. 1993;150(1):124-129.

12. Knapp P, Campbell Burton CA, Holmes J, et al. Interventions for treating anxiety after stroke. Cochrane Database Syst Rev. 2017;5(5):CD008860.

13. Garton AL, Sisti JA, Gupta VP, Christophe BR, Connolly ES Jr. Poststroke post-traumatic stress disorder: a review Stroke. 2017;48(2):507-512. Published correction appears in Stroke. 2017 Mar;48(3):e96.

14. American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders, 5th ed. APA Press; 2013.

15. Fleminger S, Greenwood RJ, Oliver DL. Pharmacological management for agitation and aggression in people with acquired brain injury. Cochrane Database Syst Rev. 2006;18(4):CD003299.

16. Allida S, Patel K, House A, Hackett ML. Pharmaceutical interventions for emotionalism after stroke. Cochrane Database Syst Rev. 2019;3(3):CD003690.

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