Skip to main content
Full access
Clinical Research Reports
Published Online: 1 April 2011

Catatonia in Psychotic Patients: Clinical Features and Treatment Response

Publication: The Journal of Neuropsychiatry and Clinical Neurosciences

Abstract

The authors report clinical features and treatment response in 25 patients with catatonia admitted to an inpatient psychiatric unit specializing in psychotic disorders. Electroconvulsive therapy, benzodiazepines, and clozapine had beneficial effects on catatonic features, whereas typical antipsychotics resulted in clinical worsening.
Catatonia is a severe clinical syndrome, first described by Karl Kahlbaum in 1874; it is characterized by a cluster of signs and symptoms, including mutism, stupor/immobility, staring, posturing, negativism, withdrawal, rigidity, and autonomic abnormalities.13 Recent literature suggests a 10%–15% prevalence of catatonia among acute psychiatric inpatients.4,5 Whereas classic cases of catatonia are easily recognized, subtler signs and symptoms of catatonia are more prevalent, and their recognition is more challenging for clinicians.6,7 Catatonic presentations are often overlooked in the context of psychotic and/or mood episodes, but the treatment of catatonia can be very different from that for psychotic and mood disorders.5,7,8 Since most patients present with catatonia and a mixture of psychotic/mood symptoms it is critical to treat each entity without adversely affecting the other. In this report, we examined the clinical characteristics and treatment response of patients with catatonia admitted to a psychiatric inpatient unit specializing in psychotic disorders including mood disorders with psychotic features.

METHOD

We conducted a retrospective chart review of 25 patients admitted to McLean Hospital's Schizophrenia and Bipolar Disorder Inpatient Unit from July 2004 to July 2009 and diagnosed with catatonia on the basis of SCID criteria by the treating psychiatrists. We examined demographic features, psychiatric symptoms, and catatonic features in this cohort. The investigators knew these patients during their clinical stay, and one clinician carried out a retrospective rating of the most severe catatonic signs and symptoms during the admission, using the Bush-Francis Catatonia Rating Scale (BFCRS).2 We examined details of the clinical course and patterns of response to various treatments. We reviewed response to medications throughout the patients' hospitalization by correlating medication administration records with clinical documentation.

RESULTS

Demographics

The group's median age was 26 years (range=18–60) and included 15 men and 10 women patients; 9 patients were previously diagnosed with bipolar disorder, 8 with psychosis (not otherwise specified), 1 with a depressive episode and anxiety disorder, and 4 with schizophrenia; 2 patients had no previous psychiatric history. Ten patients had episodes of catatonia reported in previous inpatient admissions. Six patients had a significant substance abuse history, but only one was abusing opiates and methamphetamines before this admission; 5 patients had a family history of bipolar disorder noted in the chart; 5 of schizophrenia; 6 of depression; and 4 of substance abuse; 13 patients had no documented psychiatric family history.

Clinical Characteristics

All patients had formal medical evaluations by an internist to rule out underlying medical conditions that might have contributed to their psychiatric symptoms. The medical work-ups were consistently unremarkable. Ten patients were also evaluated by a neurologist, who found no neurologic abnormalities contributing to catatonia. Fifteen patients had brain MRIs; eight patients had head CT scans; and eight had EEGs, all with no remarkable findings.
All patient records were evaluated by the same clinician and rated for presence and severity of catatonic symptoms by use of the BFCRS.2 The frequency of catatonic symptoms, in order of declining frequency, were as follows: immobility/stupor, 24/25; mutism, 23/25; staring, 22/25; posturing/catalepsy, 17/25; withdrawal, 16/25; stereotypy and ambitendency, 12/25; mannerism, waxy flexibility, and negativism, 10/25; rigidity and grimacing, 9/25; verbigeration and automatic obedience, 7/25; gegenhalten, 6/25; perseveration, 5/25; autonomic instability, 4/25; echophenomena and excitement, 3/25; impulsivity, combativeness, and mitgehen, 2/25; and grasp reflex, 0/25.
Eighteen patients with higher BFCRS scores (scores: 12–34) were rated as high in severity for withdrawal (including minimal intake of food), immobility, stupor, staring and posturing, resulting in inability to care for themselves. Seven patients with lower scores (scores: 6–11) presented with immobility, mutism, and staring. Although their catatonic symptoms were not rated as severe according to the symptom scale, these symptoms significantly impaired the patients' ability to care for themselves. Among the three patients with the highest BFCRS scores (34, 30, and 29), two vacillated from excitation marked by combativeness to stupor characterized by negativism and withdrawal, with little intake of food and water. The third progressed to severe immobility, muscular rigidity, catalepsy, mutism, and autonomic instability, and was transferred to a general hospital for emergency medical care and to rule out possible neuroleptic malignant syndrome.

Treatment Response

We reviewed medication administration records and correlated the clinical response to medications. Although the effects of particular treatments were often dramatic and obvious, we could not definitively attribute a clinical response to a particular treatment, since most of the patients were simultaneously on multiple treatments. Nonetheless, we examined the timing of initiation, dosage change, and discontinuation of various treatments, and categorized the treatment response patterns into the following categories: definitely beneficial, likely beneficial, neutral, likely detrimental, and definitely detrimental (Table 1).
TABLE 1. Pattern of Treatment Response
A total of 12 patients received ECT, with 10 receiving bilateral electrode placement. ECT led to dramatic improvement in most cases, with rapid response seen within 1–5 treatments. The response pattern showed that 10 (83%) had definite beneficial effects and 2 (17%) had likely beneficial effects, resulting in effective treatment of catatonic symptoms with a mean of 10 treatments. Six patients treated with ECT were noted to have cognitive/memory impairment during treatment, but these resolved by the time of discharge.
All 25 patients were treated with benzodiazepines. High-dose lorazepam (up to 16 mg/day) was rated as definitely beneficial for 28% of patients. The mean response time for resolving catatonia in these patients was 9 days; 68% had a “likely beneficial” response to lorazepam, whereas one did not show any response. The majority of patients required maintenance on lorazepam throughout their hospital course, including through their ECT course. While most patients had a robust response to lorazepam, some could not tolerate the higher doses, or the effects were not sustained, requiring addition of ECT or clozapine; 70% of patients were on lorazepam at time of discharge.
Seven patients were treated with clozapine, and it was rated as definitely beneficial for six of the patients and likely beneficial for one. In all cases, clozapine was initiated following unsuccessful trials of lorazepam and other atypical antipsychotic medications. While clozapine was effective, it required slow titration and close monitoring, and the response time was slower, with a mean 7-week duration for resolution of symptoms.
Although clozapine was routinely beneficial, this characteristic was not shared by other antipsychotic medications. Olanzapine and quetiapine showed mixed results, and risperidone and aripiprazole tended to have more detrimental effects. Patients treated with typical antipsychotics routinely showed detrimental effects. The adverse effects noted with these antipsychotics included worsening of catatonic symptoms, increasing confusion, agitation, and restlessness. This pattern of detrimental effects with typical antipsychotics is similar to the treatment response patterns we have reported in patients with delirious mania.9 Twelve of the patients were also treated with mood stabilizers (lithium, valproate, lamotrigine), and all were likely beneficial during the treatment of these patients.
Patients with catatonia often presented with intense fears, perseverations, and delusional preoccupations. In 60% of our patients, we found that the treatment of catatonia was accompanied by resolution of psychotic symptoms as well, whereas 40% of these patients still had psychotic symptoms after resolution of catatonia, according to clinical notes.

DISCUSSION

Recognition and proper treatment of catatonia is crucial, especially in patients with psychotic disorders, since effective treatments for catatonia differ from treatment regimens for psychosis. Catatonic symptoms can often be misunderstood as bizarre psychotic behavior and hence not recognized and treated. Historically, catatonia has been classified as a subtype of schizophrenia, but there is convincing evidence that catatonia is a syndrome that is not limited to patients with schizophrenia.10,11 In our sample, only 4 of the 25 subjects carried a diagnosis of schizophrenia. Moreover, improper treatment with antipsychotics can lead to clinical worsening and transition to lethal catatonia/neuroleptic malignant syndrome. In an effort to distinguish catatonic from psychotic presentations and to delineate treatment responses specific to the former, we examined symptoms and treatment response in patients with catatonia in an inpatient unit specializing in psychotic disorders.
We have delineated the most prevalent symptoms that should raise suspicions for a catatonic syndrome. We also report patterns of response to different treatment modalities. Benzodiazepines at high doses and ECT have routinely beneficial effects in treating catatonia, as has been described in the literature by others.5,8 For patients with malignant catatonia, investigations have shown that daily, bilateral ECT during the first week is most effective.4,8 We also note that no significant difference in short-term outcome was observed between ECT, sham ECT, and nonconvulsive stimulation in catatonia associated with chronic schizophrenia.12,13
In our study, we found that effective treatment of catatonia resulted in resolution of psychosis in over half of the patients. This interesting observation is in line with a previous study reporting that 32% of patients had resolution of psychotic symptoms once catatonia was effectively treated.14 This effect may be explained by the collateral impact of treatments directed at catatonia on psychotic symptoms, or by a worsening in psychotic symptoms by catatonia, which improve secondarily as catatonia is treated.
There is less clarity on the role played by antipsychotic medications in patients with catatonia.14 This is an important issue in treating patients presenting with both psychosis and catatonia. We found that clozapine stood out uniquely as an antipsychotic agent that was uniformly beneficial. However, this characteristic was not shared by other typical or atypical antipsychotic medications. We note that detrimental effects were more prevalent with antipsychotics that have more “typical” D2-antagonism. This should guide clinicians to have a lower threshold in using clozapine in psychotic patients with catatonia and in avoiding typical antipsychotic medications.

Acknowledgments

Dr. DO was supported by an NIH Mentored, Patient-Oriented Research Career Development Award (1K23MH079982-01A1). Dr. GTK was supported by a NARSAD Young Investigator Award. Dr. RK was supported by the Maria Lorenz Pope Fellowship from Harvard Medical School, a NARSAD Young Investigator Award, and the American Psychiatric Association/AstraZeneca Young Minds in Psychiatry International Award.

References

1.
Kahlbaum KL: Die katatonie oder das Spannungsirresein. Berlin, Verlag Aug Hirschwald, 1874
2.
Bush G, Fink M, Petrides G, et al.: Catatonia I: rating scale and standardized examination. Acta Psychiatr Scand 1996; 93:129–136
3.
Daniels J: Catatonia: clinical aspects and neurobiological correlates. J Neuropsychiatry Clin Neurosci 2009; 21:371–380
4.
Fink M, Taylor MA: The catatonia syndrome: forgotten but not gone. Arch Gen Psychiatry 2009; 66:1173–1177
5.
Rosebush P, Mazurek M: Catatonia and its treatment. Schizophr Bull 2010; 36:239–242
6.
Taylor M: Catatonia: a review of a behavioral neurologic syndrome. Neuropsychiatry Neuropsychol Behav Neurol 1990; 3:48–72
7.
Taylor MA, Fink M: Catatonia in psychiatric classification: a home of its own. Am J Psychiatry 2003; 160:1233–1241
8.
Taylor MA, Fink M: Catatonia: A Clinician's Guide to Diagnosis and Treatment. Cambridge University Press, 2003
9.
Karmacharya R, England M, Öngür D: Delirious mania: clinical features and treatment response. J Affect Disord 2008; 109:312–316
10.
Fink M, Shorter E, Taylor MA: Catatonia is not schizophrenia: Kraepelin's error and the need to recognize catatonia as an independent syndrome in medical nomenclature. Schizophr Bull 2010; 36:314–320
11.
Heckers S, Tandon R, Bustillo J: Catatonia in the DSM: shall we move or not? Schizophr Bull 2010; 36:205–207
12.
Miller DH, Clancy J, Cumming E: A comparison between unidirectional current nonconvulsive electrical stimulation given with Reiter's machine, standard alternating current electro-shock (Cerletti method), and pentothal in chronic schizophrenia. Am J Psychiatry 1953; 109:617–620
13.
Ungvari GS, Caroff SN, Gerevich J: The catatonia conundrum: evidence of psychomotor phenomena as a symptom dimension in psychotic disorders. Schizophr Bull 2010; 36:231–238
14.
Bush G, Fink M, Petrides G, et al.: Catatonia II: treatment with lorazepam and electroconvulsive therapy. Acta Psychiatr Scand 1996; 93:137–143

Information & Authors

Information

Published In

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: 223 - 226
PubMed: 21677256

History

Received: 16 March 2010
Revision received: 13 July 2010
Accepted: 26 July 2010
Published online: 1 April 2011
Published in print: Spring 2011

Authors

Details

Mary L. England, B.S.N., R.N.
From Harvard Medical School, Schizophrenia and Bipolar Disorder Program, McLean Hospital, 115 Mill St., Belmont, MA 02478.
Dost Öngür, M.D., Ph.D.
From Harvard Medical School, Schizophrenia and Bipolar Disorder Program, McLean Hospital, 115 Mill St., Belmont, MA 02478.
Glenn T. Konopaske, M.D.
From Harvard Medical School, Schizophrenia and Bipolar Disorder Program, McLean Hospital, 115 Mill St., Belmont, MA 02478.
Rakesh Karmacharya, M.D., Ph.D.
From Harvard Medical School, Schizophrenia and Bipolar Disorder Program, McLean Hospital, 115 Mill St., Belmont, MA 02478.

Notes

Send correspondence to Rakesh Karmacharya, M.D., Ph.D., Harvard Medical School, Schizophrenia and Bipolar Disorder Program, McLean Hospital, 115 Mill St., Belmont, MA 02478. e-mail: [email protected] (e-mail).

Metrics & Citations

Metrics

Citations

Export Citations

If you have the appropriate software installed, you can download article citation data to the citation manager of your choice. Simply select your manager software from the list below and click Download.

For more information or tips please see 'Downloading to a citation manager' in the Help menu.

Format
Citation style
Style
Copy to clipboard

View Options

View options

PDF/EPUB

View PDF/EPUB

Get Access

Login options

Already a subscriber? Access your subscription through your login credentials or your institution for full access to this article.

Personal login Institutional Login Open Athens login
Purchase Options

Purchase this article to access the full text.

PPV Articles - Journal of Neuropsychiatry and Clinical Neurosciences

PPV Articles - Journal of Neuropsychiatry and Clinical Neurosciences

Not a subscriber?

Subscribe Now / Learn More

PsychiatryOnline subscription options offer access to the DSM-5-TR® library, books, journals, CME, and patient resources. This all-in-one virtual library provides psychiatrists and mental health professionals with key resources for diagnosis, treatment, research, and professional development.

Need more help? PsychiatryOnline Customer Service may be reached by emailing [email protected] or by calling 800-368-5777 (in the U.S.) or 703-907-7322 (outside the U.S.).

Media

Figures

Other

Tables

Share

Share

Share article link

Share