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Pharmacy Practice (Granada)
versão On-line ISSN 1886-3655versão impressa ISSN 1885-642X
Pharmacy Pract (Granada) vol.5 no.1 Redondela Jan./Mar. 2007
Original Research |
Positive and Negative Syndrome Scale as a long-term outcome measurement tool in patients receiving clozapine ODT- A Pilot Study
Gollapudi SHANKAR, Carmen NATE.
ABSTRACT Objective: This pilot, twelve-week, open-label study examined the effect of clozapine orally disintegrating tablet or ODT in patients with schizophrenia and schizoaffective disorder utilizing Positive and Negative Syndrome Scale (PANSS) as a long-term outcome measurement tool. Key words: Antipsychotic Agents. Quality of Life. Treatment Outcome. United States. | RESUMEN Objetivo: Este estudio piloto de 12 semanas examinó el efecto de comprimidos oralmente dispersables (OD) de clozapina en pacientes con esquizofrenia o desordenes esquizo-afectivos utilizando la escala Positive and Negative Syndrome Scale (PANSS) como herramienta de medida de resultados. Palabras clave: Antipsicóticos. Calidad de vida. Resultados del tratamiento. Estados Unidos. |
Gollapudi SHANKAR. PharmD. Assistant Professor of Pharmacy Practice-Psychiatry. College of Pharmacy, Western University of Health Sciences, Pomona, CA (USA).
Carmen NATE. MD. Clinical Assistant Professor of Psychiatry. College of Pharmacy, Western University of Health Sciences and Medical Director, Olive Vista , Pomona, CA (USA).
INTRODUCTION
Approximately 20% of the two million Americans who suffer from schizophrenia are considered refractory because they receive modest benefit from conventional antipsychotic medications. Clozapine is the only atypical antipsychotic drug indicated for treatment-refractory schizophrenia based on its established superior efficacy. It is the only atypical antipsychotic that is approved for the reduction of suicidal behaviour.1 Patients who are refractory to treatment are typically more disabled as compared to other patients with schizophrenia and have a history of poor adherence which may contribute to relapse, adequate treatment can be challenging. Orally disintegrating tablets (ODT) of clozapine, offers a better way to increase adherence and improve control of psychotic symptoms.2
The Positive and Negative Syndrome Scale (PANSS) is an established psychiatric rating system that is an operationalized, drug-sensitive instrument that offers balanced representation of positive and negative symptoms and estimates their relationship to one another and to global (or general) psychopathology. The reliability and stability of the PANSS was tested previously in a large study.3 Previous studies have shown that clozapine treatment significantly improve PANSS scores in patients with schizophrenia or schizoaffective disorder after 12 and 14 weeks of treatment.4,5
In this study, PANSS is conducted on patients receiving clozapine ODT in a free-standing mental health facility to determine long term patient outcomes in cognition as related to creativity and quality of life.
The main purpose of the prospective study is to use the Positive and Negative Syndrome Scale (PANSS) as a tool to evaluate changes in positive, negative and cognitive symptoms in patients with schizophrenia or schizoaffective disorder who are receiving clozapine orally disintegrating tablet or ODT (FazaClo®).
METHODS
Subjects
Inclusion Criteria: Study subjects were selected by reviewing clients' medical charts in Olive Vista, a long-term care psychiatric facility, in Pomona, California. Clients were included in the study if they were on either on clozapine ODT or clozapine, and also have the following inclusion criteria: (1) diagnosis of schizophrenia or schizoaffective disorder diagnosed based on DSM-IV by the facility's psychiatrist; (2) have been placed on clozapine ODT by the facility's psychiatrist or had been on the study medication before coming to this facility due to refractory to previous antipsychotic medication treatments. Subjects from 18 65 years of age were included. Subjects currently using other typical or atypical antipsychotic medications are not excluded.
Exclusion Criteria: Clients allergic to clozapine ODT or clozapine, or intolerant to the study medications due to severe adverse drug reactions were excluded.
The study received IRB approval; and informed consents were obtained from each of the study subjects. All subjects were on dosages of clozapine ODT that were titrated by the facility psychiatrist to achieve maximum clinical benefits not based on PANSS scores. Other than encouraging the subjects in their creative expressions of music, art, drama, games, poetry, humor, ensure their need for medication compliance and their sense of spiritual value no treatment intervention was necessary to carry out the study except the allowance of dosage reduction of study medications in the event of adverse drug reaction.
Design and Assessment
Positive and Negative Syndrome Scale (PANSS) composes of 3 components: Positive (P), Negative (N) and cognitive or General Psychopathology (G).
Positive syndrome is composed of symptoms such as delusions, hallucinations and disorganized thinking. Negative syndrome is characterized by deficits in cognitive, affective, and social functions, including blunting of affect and passive withdrawal. General Psychopathology is composed of many deficits in cognition such as disorientation, poor attention, lack of insight and active social avoidance.
Positive and Negative subscales each contain 7 items (P1 P7, N1 N7); General Psychopathology subscale contains 16 items with the major emphasis on cognition (G 1 - G16) (Table 1).
Each item is scored from 1-7 based on the presence and severity of symptoms: (1 = absent, 2 = minimal, 3 = mild, 4 = moderate, 5 = moderate severe, 6 = severe, 7 = extreme).
Each item on the PANSS is accompanied by a complete definition as well as thorough anchoring criteria for all 7 rating points. Based on the above scoring method, the least scores for the Positive and Negative subscales are 7 points each, and 16 points for the cognitive category; for a combined total of minimum 30 points. Most points for each category are 49, 49 and 112 for Positive, Negative, and cognition, respectively; for a combined total of maximum 210 points.
Subjects were interviewed by the facility's psychiatrist and Psychiatric pharmacist at baseline and every 4 weeks thereafter (baseline, week-4, week-8 and week-12). The interviewer asked questions pertaining to PANSS and also encouraged subjects to discuss their history, circumstances surrounding their hospitalization, their current life situation and their symptoms. The objective of this process is to establish rapport and allow subjects to express areas of concern. During each clinical interview, subject's affective, motor, behavioral and cognitive functions were observed. Their ability to participate by empowering them through their creative expressions and their integrative and interactive functions were also directly observed by the interviewers.
The duration of each clinical interview was 15-20 minutes. Their overall functioning in their creative, integrative and interactive expressions as an exclusive group in each separate sessions was 20 to 30 minutes The PANSS ratings are based on all information derived from the clinical interview, direct observation of the subjects and reports of primary care staff.
Each rating was assigned by first referring to the item definition to determine presence of a symptom. The severity of an item is then determined by deciding which anchoring point best described the subject's functioning, whether or not all components of the description are observed. The highest applicable rating was always assigned even if the subject meets criteria for the lower rating as well. White blood cell (WBC) count with differential and absolute neutrophil count (ANC) are monitored weekly to avoid hematologic adverse reactions, such as agranulocytosis. Paired sample t-tests were used to compare the total score improvement as well as score improvement in each of the three subscales (positive, negative and general psychopathology) at baseline and the end of 12-weeks of treatment. Results are statistical significant if P<0.05.
RESULTS
Final sample consisted of nineteen males and one female at the beginning of the study. However only nineteen clients finished the 12-week study (March 27th, 2006 to June 19th, 2006); one male client was transferred to another psychiatric facility before the week-4 assessment period. Final assessment thus only included data for 19 subjects who finished the study. Mean age of 39.5 years; range from 20 54 years of age.
Clozapine ODT dosing ranged 300 mg 900 mg daily throughout the study period. 35% of subjects were on clozapine ODT as monotherapy. Other concurrent antipsychotic medications include ziprasidone, quetiapine, risperidone, olanzapine, aripiprazole, haloperidol, and chlorpromazine. None of the subject experienced agranulocytosis during the 6-week study period. One subject developed seizure during week-8 resulted in the dose reduction of study medication from 900 mg to 600 mg daily.
Improvement in mean PANSS scores was observed in all three categories across the 12-week study period (Table 3). Paired sample t-tests showed statistically significant differences in all three scales and the total score between baseline and at week-6 (Table 3).Compared to baseline, at week-12, the average reduction in Positive scale was 4.000 ± 2.828 points, 4.947 ± 3.341 points in Negative scale, and 7.842 ± 5.833 points in General psychopathology scale (Table 4). Two subjects were discharged at week-12, and one subject was planning to be discharged shortly after reaching acceptable, stable clinical improvement.
DISCUSSION
The results of the initial part of a longer study showed a statistical significant improvement in all three areas of PANSS at the end of 12-week when compared to baseline. On average, scores in all three areas (positive, negative and cognitive) progressively improved over the 12-week study period. A greater improvement in negative scale compared to the positive scale was observed during the 6-week study period (-4.947 vs. -4.000). Negative syndrome is characterized by deficits in cognitive, affective, and social functions, including blunting of affect and passive withdrawal. This observation concurs with the current understanding of the clinical benefit of clozapine and other atypical antipsychotics, that in addition to improving positive and negative symptoms of schizophrenia (ex: delusion, hallucination, paranoia, etc.), these medications are effective in improving cognitive symptoms including their creative expressions and overall quality of life as their compliance are ensured.
The greater improvement in negative symptoms, including cognitive functions, observed in this study is in accordance with results of some previous studies. A study done on subjects with schizophrenia or schizoaffective disorder by Volavka et al5 in 2002 comparing clozapine, olanzapine, risperidone and haloperidol showed that clozapine was the most effective treatment for negative symptoms. Lindemayer et al4 (1994) showed improvement in all three categories of PANSS in 12-weeks treatment period in treatment-refractory schizophrenics with significant negative symptoms while on clozapine.
The study did not exclude subjects who were on other antipsychotic medications (in addition to clozapine ODT); the effect of other concurrent antipsychotic medications could have compounded the results of the study. However, it is a common, clinical practice for patients with schizophrenia or schizoaffective disorder to be on more than one antipsychotic. Clozapine usually is added as a last option to control psychotic symptoms or negative symptoms. This was an open-label study such that the clinical interviewers/investigators were not blinded to the dosage of study medications the subjects were using. It would be very difficult to blind the interviewers/investigators since one of them was the facility psychiatrist.
Clinical relevance and importance of current study: Unlike previous studies, clozapine ODT is used in here. Clozapine is typically used for refractory schizophrenia or schizoaffective disorder after other atypical antipsychotics, so its clinical effect on positive and negative symptoms, including cognition, is emphasized in the study. Primary measure of efficacy is the improvement in total PANSS score after twelve weeks of clozapine ODT treatment, including total score, as well as positive, negative and cognition (or general psychopathology) subscales in the study.
CONCLUSIONS
The present study used PANSS as an outcome measuring tool to evaluate the effect of clozapine ODT in patients with schizophrenia and schizoaffective disorder. The results of the 12-week preliminary study period showed statistically significant improvement in total score as well as in positive, negative and general psychopathology scales. The statistically significant improvement in PANSS further validates the clinical benefit of clozapine in treating refractory schizophrenia. Clozapine is typically reserved as treatment resistant schizophrenia due its potential risk of inducing agranulocytosis, so patients usually are given clozapine after they have only responded minimally to other antipsychotics. The promising results of the study confer hope to those refractory-schizophrenic patients and their families, in that, clozapine can help to improve positive and negative symptoms, and more importantly, cognition (creativity and expression). With improved cognition, patients can function more normally and more independently in society.
ACKNOWLEDGEMENT
The authors would like to thank the following people for their support of this project:
Alamo Pharmaceutical and Ms. Cheryl Eakin for their grant for this study.
Ryan Quist, Ph.D. for his statistical expertise.
References |
1. Lexi-Comp. UpToDate®: "Clozapine: Drug information. [ Links ]".
2. Alamo Pharmaceuticals. FazaClo® General Information. http://www.fazaclo.com/GeneralInfo.asp. (Accessed 03/02/2006). [ Links ]
3. Kay SR, Fiszbein A, Opler LA. The Positive and Negative Syndrome Scale (PANSS) for schizophrenia. Schizophrenia Bulletin 1987; 2:261-76. [ Links ]
4. Lindenmayer J, Grochowski S, Mabugat L. Clozapine effects on Positive and Negative Symptoms: A six-month trial in treatment-refractory schizophrenics. J Clin Psychopharmacol 1994; 14:201-4. [ Links ]
5. Volavka J, Czobor P, Sheitman B, Lindenmayer J, Citrome L, McEvoy JP, Cooper TB, Chakos M, Lieberman JA. Clozapine, olanzapine, risperidone, and haloperidol in the treatment of patients with chronic schizophrenia and schizoaffective disorder. Am J Psychiatry 2002; 159:255-62. [ Links ]