Natural History of Illness/Comorbidity

Diagnostic Criteria for PD

         Recurrent unexpected panic attacks with four or more of the symptoms listed below (not including culture-specific symptoms such as uncontrollable screaming, crying, headache).

         At least one of the attacks has been followed by one or more of the following for at least 1 month:

                Persistent concern about having additional attacks

                Worry about the implications of the attack

                A significant maladaptive change in behavior to avoid future attacks

         The disturbance is not better explained by another type of mental disorder.

         The disturbance does not occur in relationship to the physiological effects of a substance, or other medical condition.

Symptomatology of Panic Attacks

         Shortness of breath/smothering sensations

         Dizziness, unsteady feelings, or faintness

         Palpitations/tachycardia

         Trembling/shaking

         Sweating

         Feelings of choking

         Nausea/abdominal distress

         Depersonalization (being detached from oneself)

         Derealization (feelings of unreality)

         Paresthesias (numbness or tingling sensations)

         Flushes/chills

         Chest pain or discomfort

         Fear of dying

         Fear of going crazy or doing something uncontrolled

Treatment Options, Expected Outcomes, and Comprehensive Management

COGNITIVE-BEHAVIORAL THERAPY

CBT teaches patients to anticipate the situations and bodily sensations associated with their panic attacks. This awareness sets the stage for helping the patient to control the attacks. Specially trained therapists tailor CBT to the specific needs of each patient. The therapy usually includes the following components:

CBT is a short-term treatment, typically lasting 12 to 15 sessions over several months. It is thought that patients who undergo CBT demonstrate a high maintenance of treatment gains over time. Family members and others may participate by encouraging the patient to complete individual counseling or group activities, and become a monitor of behaviors that may suggest the need for medical and psychiatric intervention. In some locations, CPT may not be available due to the absence of providers skilled in this intervention. The use of phone and Internet contact between the therapist and the patient are increasing (Donegan & Dugas, 2012).

PHARMACOTHERAPY

Anxiety-disorder patients tend to be sensitive to medication and often experience exacerbation of their symptoms with medication, especially if too large an initial dose is used. It is generally recommended that low starting doses of selective SSRIs, selective norepinephrine reuptake inhibitors (SNRIs), and TCAs be used and that low doses be maintained for several days and gradually increased to a full therapeutic dose as the patient tolerates (APA, 2010, 2013; Marchesi, 2008). Insufficient evidence exists to recommend any of these pharmacological agents as superior to the others (APA, 2010, 2013). It is important to note that not advancing to full therapeutic dosages is common in treatment of PDs and is a frequent source of patient partial or nonresponse (APA, 2010, 2013). It is recommended that patients be informed of a time frame for positive response to avoid premature abandonment of treatment. There are limited data on optimum length of treatment after patient response to therapy has been achieved (Bandelow et al., 2012).

The concern for potential treatment-related increases in self-harming or suicidal behaviors associated with antidepressant medications requires clarification. Data primarily from studies on children and adolescents resulted in Food and Drug Administration (FDA) warnings applied to all antidepressants indicating the risk of increased suicidal thinking and behavior in patients younger than 25 years. In adults, antidepressant treatment does not appear to be associated with an increase in suicide risk (APA, 2010, 2013).

Pharmacological agents with proven benefits in numerous randomized controlled trials (RCTs) in treating PD include SSRIs, SNRIs, TCAs, and BDZs, and are recommended as first-line therapy (APA, 2010, 2013; Marchesi, 2008). Because of their favorable safety and side-effect profile, SSRIs and SNRIs are considered the best initial choice for PD (APA, 2010, 2013). Because of their larger evidence base, SSRIs are more likely to be chosen as first-line treatment (Marchesi, 2008).

Although TCAs have demonstrated effectiveness in PD, the side effects and greater toxicities associated with overdose limit their usefulness and are associated with higher dropout rates. The most studied TCA is imipramine and has demonstrated effectiveness in PD. In addition, clomip-ramine has considerable empirical support for use in PD (APA, 2010, 2013; Marchesi, 2008). Most common side effects of TCAs include anticholinergic effects, increased sweating, sleep disturbances, orthostatic hypotension and dizziness, fatigue and weakness, cognitive disturbances, weight gain, and sexual dysfunction. TCAs have been associated with significant or fatal arrhythmias and must be used with caution with the elderly population; they are contraindicated for patients with prostatic hypertrophy or narrow-angle glaucoma (APA, 2010, 2013). BDZs are appropriate for monotherapy only in the absence of co-occurring mood disorders. For dosing information for the use of antidepressants and benzodiazepines with panic disorder, refer to current drug guidelines. However, they may be used in combination with antidepressants for rapid symptom control (APA, 2010, 2013). Alprazolam has demonstrated efficacy in treatment of PD. Because of its short half-life this medication requires 3 to 4 times daily dosing and presents compliance problems for many patients and with missed doses can result in more rapid and profound withdrawal symptoms (APA, 2010, 2013). There is also a sustained-release form of alprazolam that may alleviate some of these dosing problems. Monoamine oxidase inhibitors (MAOIs), although an effective treatment for PD, because of their safety profile, are generally reserved for patients who fail first-line treatment (APA, 2010, 2013). MAOIs have serious drug-drug interactions resulting in serotonin syndrome causing hypertensive crisis that can be fatal. Symptoms include confusion, agitation, hyperthermia, as well as autonomic and neuro-muscular symptoms. Serotonin syndrome can occur when MAOIs are used with other antidepressants (particularly SSRIs); linezolid; analgesics (meperidine, fentanly, tramadol); over-the-counter (OTC) dextromethorphan; and other medications such as busiprone, as well as antimigraine medications. A recent meta-analysis (Mitte, 2005) comparing the efficacies of TCA, SSRI, and BDZ therapies demonstrated a similar effect in improving anxiety in both symptoms and frequency of panic attacks, as well as agoraphobia. In this same meta-analysis, SSRIs and TCAs were superior to BDZs in alleviating depression (Marchesi, 2008).

SSRIs available in the United States include fluoxetine, sertraline, paroxetine, fluvoxamine, citalopram, and escitalopram. Evidence does not exist for differential efficacy between agents in this class. Other agents used in the management of PDs include anticonvulsants, antipsy-chotics, antihypertensives, and buspirone. Limited data exist for the use of anticonvulsants in PD (APA, 2010, 2013). Only one RCT provided partial support to the fact that gabapentin is safe and efficacious for PD. Therefore, gabapentin should not be considered as first-line treatment for PD (APA, 2010, 2013). There is no evidence that first-generation antipsychotics (typical) are effective in PD and the risk of neurological side effects outweighs any potential usefulness (APA, 2010, 2013). There is limited positive evidence for the use of the second-generation antipsychotics (atypical) olanzepine and adjunctive risperidone. However, evidence is limited for efficacy and concern about second-generation side effects limits their ability to be broadly recommended. The antihypertensive beta-adrenergic blocking agents (e.g., propranolol, ateno-lol) are ineffective in PD but may help reduce somatic sensations in selected patients (APA, 2010, 2013). Buspirone as monotherapy is not effective for PD and there are no published data except case reports for its use as an augmentation strategy.

Additional concerns include the fact that, initially, SSRIs can be panicogenic. As such they need to be initiated at low doses and slowly tapered up. It is recommended that the initial low dose be maintained for 3 to 7 days and gradually increased in weekly increments. Both SSRIs and SNRIs are associated with discontinuation syndromes including dizziness, headache, and nausea, and require tapering over at least 7 to 10 days. Elderly patients with PD have higher rates of co-occurring mood disorders and recommendations for treatment are use of an antidepressant as first-line therapy. SNRIs are preferred in this population (Resch, 1999).