BALTIMORE — The lack of diagnostic criteria has hamstrung neurologists in their attempt to diagnose involuntary emotional expression disorder, Dr. Sharon Handel said at a meeting on Alzheimer's disease and related disorders sponsored by Johns Hopkins University.
Even when they make the diagnosis with certainty, neurologists have little to offer by way of Food and Drug Administration-approved therapy, said Dr. Handel, of the department of psychiatry at Johns Hopkins University, Baltimore.
Part of the problem with identifying this condition has been the numerous names under which it is known, she noted. Involuntary emotional expression disorder (IEED) is also known as pseudobulbar affect and pathologic laughing or crying.
It's been estimated that more than 1 million people in the United States have IEED. The disorder has been associated with cerebrovascular accident, Alzheimer's disease, multiple sclerosis, amyotrophic lateral sclerosis, and traumatic brain injury.
The hallmark of IEED is episodes of crying or laughing that are unrelated to or out of proportion with the eliciting stimulus. There is a disconnection between emotional experience and expression.
Emotional outbursts in IEED are involuntary, episodic, and incongruent with baseline mood. The outbursts are intense, but are followed by a return to baseline.
Disorders of affect—which IEED appears to be—involve impairment of the moment-to-moment regulation of emotion. “There's a disconnection of the neural networks in this condition from the experienced emotion to the display of emotion,” said Dr. Handel.
The neural networks of emotion involve the frontal lobes, the limbic system, the brainstem, the cerebellum, and white-matter tracts. In particular, the prefrontal cortex integrates complex sensory and limbic information that determines the emotional valence of a stimulus and modulates motor and autonomic responses involved in emotional expression. It's not clear where the neural interruption occurs in IEED.
For now, the current diagnostic criteria include:
▸ Episodes of involuntary crying, laughing, or related displays.
▸ An origin in brain injury or disease.
▸ A change in the patient's emotional behavior from that prior to the disease or injury.
▸ Incongruent or exaggerated mood.
▸ A response that is excessive or unrelated to the stimulus.
▸ Significant distress or impairment.
The differential diagnosis should include epilepsy; facial dystonia or dyskinesias; vocal tics; axis I disorders (such as major depression or bipolar disorder); axis II disorders (such as borderline personality disorder); and substance abuse.
“These patients often have major depression, and while specific treatment is often the same, I think it's important to differentiate the two conditions,” said Dr. Handel.
The differential diagnosis should also include affective lability, essential crying, and witzelsucht (a tendency to inappropriate jokes). With affective lability, the subjective and objective dimensions of affect are not dissociated. Essential crying is a hereditary and lifelong tendency to cry easily. Witzelsucht is an addiction to trivial joking, which can take the form of both an inappropriate giddy affect and irritability or aggressiveness.
In terms of clinical course, IEED frequently remits spontaneously within 6 months. Others may have remission with treatment within 3 months. Resolution of IEED can be independent of the resolution of depression. However, in some cases the disorder is chronic and persistent without treatment.
Treatment of IEED is still evolving. At present, there is no FDA-approved treatment for IEED. “What are typically used—at least up to this point—are SSRIs. They tend to work quite quickly,” said Dr. Handel.
In fact, response can be seen in just a few days in some patients.
Dextromethorphan, in combination with quinidine, is being studied to treat patients with IEED. Dextromethorphan is a nonopioid antitussive, but it also has a number of other neuropharmacologic properties. It is a potent sigma1 agonist (inhibiting the release of the excitatory neurotransmitter, glutamate) and is also an N-methyl-D-aspartic acid glutamate receptor antagonist.
Dextromethorphan undergoes significant first-pass metabolism by the cytochrome P450 isoenzyme CYP2D6. Quinidine is a potent inhibitor of this isoenzyme, thereby increasing and sustaining dextromethorphan levels.