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Published Online: 1 April 2012

Dissociative Identity Disorder May Be Relieved by the Combined Treatments of Mirtazapine and Risperidone: Case Report of an Adolescent

Publication: The Journal of Neuropsychiatry and Clinical Neurosciences
To the Editor: Dissociative identity disorder (DID) is characterized by the existence of two or more personalities that recurrently take control of behavior. Here, we present an adolescent patient with DID, who had improvement of symptoms after the combined treatment of mirtazapine and risperidone.
“Miss G” is a 16-year-old adolescent girl with past emotional trauma associated with physical abuse in childhood and recent frustrations in her school and love-life. She visited my clinic, and her mother mentioned that she had said that, for the past 6 months, there were four personalities inside her mind, each with its own relatively enduring pattern of perceiving, relating to, and thinking about the environment and self. These personalities would provoke her odd behaviors, such as school-refusal; self-harm, such as cutting wrists at superficial depth; verbal aggression; physical aggression; talking to herself; dressing different when her personality changed; initial insomnia; anger outbursts; and mood swings. These odd behaviors have caused impairments in social and academic functioning. No history of substance abuse or medical illness was mentioned. Mild depression (Hamilton Rating Scale for Depression: 13) was also revealed. The scores of the Adolescent Dissociative Experience Scale (A-DES) were 167, with most items rated more than 5 points (at least moderately-severe).
With the impression of DID, aggression risk, and deliberate self-harming behavior, we prescribed mirtazapine 30 mg and risperidone 2 mg. After the first week of treatment, her personality switch decreased, and less aggression or self-harm was noted (A-DES scores: 127). Mild sedation and somnolence side effects were mentioned, but without extrapyramidal side effects. Her mother assisted her in receiving the biological treatment and monitored whether she took these medications because of the possibility of poor medication adherence. She mentioned that her original personality could control her mind and behavior longer after the mirtazapine and risperidone treatment. The other three personalities became diminished after medication treatment. The A-DES scores also decreased from 167 to 45, with significant improvement after 1 month of treatment. The symptoms changed mostly in the dimensions of behavioral control, thought control, body self-awareness, personality-switch frequency and duration, and better ability to recall what she did while another personality manipulated her mind and behavior. Her symptoms maintained stationary (A-DES: 41) under mirtazapine and risperidone combined treatment for the next 6 months until the present, with mild body-weight gain, around 1 kg in these 7 months.
Emotional trauma is usually associated with mesocortical and mesolimbic dopaminergic system dysfunction, which may alter midbrain defense response, a reaction associated with DID.1 Besides dopamine, the serotoninergic system, such as serotonin-transporter gene polymorphism, might also be associated with childhood emotional trauma or physical abuse.2 Serotonin-transporter short alleles also contribute to emotional sensitivity to stressors in the victims of childhood physical maltreatments.3 The combined treatment might cover the dopamine and serotonin mechanisms and provide the therapeutic effects in this patient.

References

1.
Corrigan FM, Fisher JJ, Nutt DJ: Autonomic dysregulation and the Window of Tolerance model of the effects of complex emotional trauma. J Psychopharmacol 2011; 25:17–25
2.
Lochner C, Seedat S, Hemmings SM, et al.: Investigating the possible effects of trauma experiences and 5-HTT on the dissociative experiences of patients with OCD using path analysis and multiple regression. Neuropsychobiology 2007; 56:6–13
3.
Stein MB, Schork NJ, Gelernter J: Gene-by-environment (serotonin transporter and childhood maltreatment) interaction for anxiety sensitivity, an intermediate phenotype for anxiety disorders. Neuropsychopharmacology 2008; 33:312–319

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Go to The Journal of Neuropsychiatry and Clinical Neurosciences
Go to The Journal of Neuropsychiatry and Clinical Neurosciences
The Journal of Neuropsychiatry and Clinical Neurosciences
Pages: E34
PubMed: 22772693

History

Published online: 1 April 2012
Published in print: Spring 2012

Authors

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Chen-Han Lai, M.D.
Dept. of Psychiatry Buddhist Tzu-Chi General Hospital, Taipei Branch Taipei, Taiwan Institute of Brain Science National Yang Ming University Taipei City, Taiwan

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