Headaches in Patients with Coexisting Psychiatric Disease

Donald Penzien

Richard C. Peatfield

Gay L. Lipchik

INTRODUCTION

Although most individuals with headache in the general population do not have comorbid psychiatric disorders, many patients presenting to specialty clinics do—especially those with chronic daily headache (24) and those with medication-overuse headache (35). Recent epidemiologic studies have identified a strong association between migraine and psychiatric disorders (11, 12, 13). For example, more than 30% of migraineurs compared with 10% of nonmigraineurs have a lifetime prevalence of major depression; similarly, 11% of migraineurs compared with 2% of nonmigraineurs have a lifetime prevalence of panic disorder (9). Migraine with comorbid depression is often complicated by the presence of an anxiety disorder, with the onset of the anxiety disorder typically preceding the onset of migraine and possibly present as early as childhood (33,51).

The exact nature of the relationship between migraine and mood disorders remains unclear. It is unlikely that depression results simply as a consequence of the burden of living with a recurrent painful condition. Several epidemiologic studies suggest the relationship is bidirectional, with the presence of major depression or anxiety increasing the likelihood of subsequently developing migraine (10, 11, 12). It is generally believed that the occurrence of comorbidity most likely arises from shared pathophysiology of migraine and mood disorders; this is discussed in detail by Drs. Merikangas Low, and Rasmussen in Chapter 26 of this volume.

Although one might expect psychiatric comorbidity to predispose headache patients to a poorer headache prognosis, this notion only rarely has been investigated. However, one recent longitudinal study revealed that the presence of psychiatric disorders (especially multiple disorders) foretold a poor headache treatment outcome (19). This 8-year prospective study of 100 young headache sufferers by Guidetti and colleagues (19) revealed that 86% of headache sufferers diagnosed with two or more comorbid psychiatric disorders in childhood or adolescence reported either no improvement or a deterioration in their migraine or tension-type headache (TTH) over time. In 62% of patients diagnosed with one comorbid psychiatric disorder, their headaches remained unchanged or worsened. Alternatively, the absence of psychiatric disorders was associated with remission of headaches after 8 years. Moreover, there is emerging evidence that a number of behavioral/psychologic risk factors are associated with progression of headache from episodic to chronic and daily (29,43) and that psychologic distress may play an even greater role in the transformation and chronification of headache than does analgesic overuse/abuse (47). Thus, the identification and treatment of psychiatric disorders in headache patients is essential beginning at an early age.

In this chapter we discuss the role of psychiatric illness in headache disorders. We briefly discuss the assessment of psychiatric illness in a nonpsychiatric medical setting. We also enumerate a number of opportunities as well as obstacles for the management of comorbid headache and psychiatric illness, and we close with an overview of a new diagnostic classification for headache symptoms attributable to a psychiatric disorder.

ASSESSMENT OF COMORBID PSYCHIATRIC DISORDERS

Given the frequent co-occurrence of recurrent headache and psychiatric disorders, depression and anxiety at a minimum merit a brief investigation during the clinical evaluation of migraine or TTH. This is particularly pertinent for patients presenting to specialty centers. There are a variety of well-validated and efficient screening tools designed to facilitate psychologic symptom assessment. The
presence and severity of depressive illness can be evaluated rapidly by the Beck Depression Inventory (BDI) (5,7) or the Hamilton Depression Inventory (HDI) (39). Likewise, the presence and severity of anxiety can be evaluated by the Beck Anxiety Inventory (6) or the Trait Anxiety Inventory (48).

The PRIME-MD (Primary Care Evaluation of Mental Disorders) (49) is yet another diagnostic tool designed for use in medical settings to assess the presence of a variety of comorbid psychiatric disorders. It is a 26-item self-administered symptom checklist designed to screen for common psychiatric disorders based on diagnostic criteria from the American Psychiatric Association’s Diagnostic and Statistical Manual of Mental Disorders, 4th edition (DSM-IV) (2). The list of disorders screened by the PRIME-MD includes mood disorders (depression, bipolar), anxiety disorders (panic disorder, generalized anxiety disorder), eating disorders, alcohol abuse or dependence, and somatization disorders. The PRIME-MD has been well utilized in a large number of published studies, including an increasing number addressing recurrent headache. Schriger and colleagues (44), for example, administered the PRIME-MD to 218 patients presenting to an emergency department with long-standing headache, abdominal pain, or back pain (patients with known psychiatric illness were excluded from the study). The authors reported that most patients willingly completed the PRIME-MD (median time of 7 minutes), which frequently yielded psychiatric diagnoses among these patients with primary complaints of pain (42% of patients overall).

TREATMENT OF PSYCHIATRIC COMORBIDITY

In the following sections we focus on depression, panic disorder, somatoform disorder, and selected personality disorders, as they are highly prevalent among head pain patients and can prove especially challenging for clinicians. We present recommendations for pharmacologic and nonpharmacologic interventions and suggest that in most instances, a combination of these two therapeutic strategies (often requiring a multidisciplinary intervention) generally is the preferred approach to treating headache complicated by psychiatric comorbidity. For additional details pertaining to management of these and other comorbid psychiatric disorders in headache patients, works by Lipchik and Rains (28), Saper and Lake (42), and Saper and Sheftell (35) are recommended reading.

Major Depression

Major depressive illness is a common disorder with a lifetime prevalence of at least 20% in women and 10% in men (26). It has been characterized as “the neglected major illness” because of the consistent underrecognition of the disorder and the tremendous costs it engenders (an estimated $44 billion annually in the United States) (18). The lion’s share of the cost of depression is a consequence of inadequate recognition and care of the illness, leading to lowered employment productivity. Although it can be a lifelong disorder, the majority of patients with depression can be treated successfully (1,18). On the other hand, efforts to manage head pain are considerably less likely to succeed if comorbid depression is not recognized and effectively treated.

The hallmark of major depressive illness is sad or depressed mood and a loss of interest or pleasure in previously enjoyed activities (anhedonia). The syndrome of depression is defined by a collection of symptoms that includes depressed mood and also results in significant functional impairment (see Table 137-1). Not everyone who is depressed experiences every symptom, with some patients experiencing only few symptoms and others many. The severity of symptoms varies considerably both between individuals and within patients over time. Depressive illness has a high rate of comorbidity with anxiety disorders and substance abuse.

Although full-blown depression with depressed affect, tearfulness, and psychomotor symptoms is not difficult to
diagnose, depression may not always be evident without systematic inquiry. Inquiry about all of the symptoms that constitute the criteria for major depression is essential for accurate diagnosis of depression.

TABLE 137-1 Symptoms of Major Depressive Episode

Five or more of the following symptoms have been present during the same 2-week period and represent a change from previous functioning. At least one symptom is either depressed mood or loss of interest or pleasure in previously enjoyed activities.
1. Depressed mood (feeling sad or empty, appears tearful; for children or adolescents, can be irritable mood)
2. Loss or interest or pleasure in most activities
3. Significant weight loss without dieting or decrease in appetite (with atypical depression—weight gain, increased appetite)
4. Insomnia or hypersomnia
5. Psychomotor agitation or retardation
6. Fatigue or loss of energy
7. Feelings of worthlessness or excessive, inappropriate guilt
8. Impaired concentration, slowed thinking, or indecision
9. Suicidal thoughts (with or without a plan) or a suicide attempt
Symptoms cause clinically significant distress or impairment in social, occupational, or other important areas of functioning.
The symptoms are not due to:
1. The direct physiologic effects of a substance (medication or drug of abuse)
2. A general medical condition (e.g., hypothyroidism)
3. A mixed episode of mania and depression
4. Bereavement

Excerpted from the Diagnostic and Statistical Manual of Mental Disorders, 4th edition (2).

Pharmacologic treatment of major depression focuses on the use of adequate doses of antidepressants. Tricyclic and related cyclic antidepressants (TCAs) can be effective in the prophylaxis of headache disorders (17,45), but they are now less often used in treatment of depression because of side effects associated with the high doses required to achieve an adequate clinical response. The newer selective serotonin reuptake inhibitors (SSRIs) have fewer side effects (e.g., less sedation, less likely to cause weight gain) than TCAs and have a lower risk for overdose. There is, however, less evidence of the effectiveness of fluoxetine and other SSRIs (e.g., fluvoxamine, paroxetine, sertraline, venlafaxine) for the prophylaxis of migraine and TTH (8,17,27,45). An SSRI may be worth considering if a tricyclic drug is poorly tolerated or has proved unsuccessful.

Because the overall efficacy of antidepressants does not vary dramatically from one medication choice to the next (within a class), the medication choice should be based on side effect profile and symptom target. For example, TCAs would be preferred for a patient with insomnia, while an SSRI might be preferred for an overweight or obese patient. SSRIs and TCAs are contraindicated when mania is present or suspected. The anticonvulsant valproate is effective in treating migraine and comorbid manic depression (bipolar disorder). The β-blockers, typically used in migraine prophylaxis, are relatively contraindicated when depression is also present. Researchers recently have begun to evaluate the benefits that may be achieved through use of an algorithmic approach to prescribing medications for patients with comorbid headache and psychiatric illness. Kaniecki (25) implemented an algorithm calling for use of SSRIs for migraineurs with depression and anxiety, TCAs for those with insomnia, and antiepileptic drugs (AEDs) for the remaining patients. Approximately two thirds of 367 patients experienced significant reductions in headache frequency and disability at 1 year, leading Kaniecki to conclude that the presence of these comorbidities may help rationally guide the selection of preventive agents for patients with migraine. Table 137-2 offers an overview of the therapeutic opportunities and limitations in treating comorbid migraine and psychiatric disorders.

The U.S. Agency for Healthcare Research and Quality (1) has developed guidelines for treating major depression. Once a diagnosis has been made, treatment should be monitored every few weeks. Response to treatment should be assessed at week 6, and if the patient shows clear improvement the treatment should be continued for an additional 6 weeks. If there is complete remission of symptoms, medication is continued for 4 to 9 months to prevent relapse. Maintenance treatment should be considered because after one episode of depression, the chance of recurrence is at least 50%. Increasing evidence supports ongoing treatment for a period of several years, if not indefinitely, to reduce the likelihood of relapse and recurrence. If a patient is only somewhat better at 6 weeks, a dose adjustment can be made. Treatment should be continued and monitored every 2 weeks. If at week 12 there is not a complete response to medication, a referral for psychotherapy, a referral to psychiatry for medication management, or a change in medication should be considered, although it may be more efficacious to augment SSRI antidepressant medication with bupropion than to switch SSRIs (34).

Only gold members can continue reading. Log In or Register to continue