1. El CATIE EN LA PRACTICA�El SOHO HOY
¿Qué sabemos? ¿Qué aprendimos?
2. Parte 1:
Destacar algunos conceptos de SOHO y
CATIE y compararlos con nuestras observaciones en la clínica diaria
Parte 2:
Presentar una nueva conceptualización de los antipsicóticos atípicos, más acorde con los nuevos descubrimientos de mecanismos y modos de acción y su aplicabilidad clínica
3. �Parte 1�
Destacar
algunos conceptos
CATIE y SOHO
y compararlos
con nuestra clínica diaria
4. Efectividad Key Points: The concept of treatment effectiveness considers the impact of the medication on controlling the various symptoms of the illness, as well as the safety and tolerability of the medication.1 Despite the established need for a patient to continue on their prescribed treatment, many patients with schizophrenia fail to adhere to their medication. Interruption of antipsychotic treatment in patients with schizophrenia, through treatment discontinuation or inconsistent adherence, is associated with increases in rates of relapse, hospitalization, and treatment costs.2-5
Background: Poor adherence to treatment of chronic diseases is a worldwide problem of striking magnitude. Adherence to long-term therapy for chronic illnesses in developing countries averages 50%.6
References:
1. Swartz MS, Perkins DO, Stroup TS, et al. Assessing clinical and functional outcomes in the clinical antipsychotic trials of intervention effectiveness (CATIE) schizophrenia trial. Schizophr Bull 2003;29(1):33-43.
2. Herz MI, et al. Intermittent vs. maintenance medication in schizophrenia: two-year results. Arch Gen Psychiatry 1991;48:333-339.
3. Svarstad BL, Shireman TI, Sweeney JK. Using drug claims data to assess the relationship of medication adherence with hospitalization and costs. Psychiatr Serv 2001;52:805-811.
4. Ascher-Svanum H, Zhu B, Faries D, et al. A comparison of olanzapine and risperidone on the risk of psychiatric hospitalization in the naturalistic treatment of patients with schizophrenia. Ann Gen Hosp Psychiatry 2004;3(1):11.
5. Gilmer TP, Dolder CR, Lacro JP, et al. Adherence to treatment with antipsychotic medication and health care costs among Medicaid beneficiaries with schizophrenia. Am J Psychiatry 2004;161(4):692-699.
6. Haynes RB. Interventions for helping patients to follow prescriptions for medications. Cochrane Database of Systematic Reviews 2001;1.
7. Lehman AF, Lieberman JA, Dixon LB, et al. APA practice guideline for the treatment of patients with schizophrenia. Am J Psychiatry 2004;161(suppl 2):1-56.Key Points: The concept of treatment effectiveness considers the impact of the medication on controlling the various symptoms of the illness, as well as the safety and tolerability of the medication.1 Despite the established need for a patient to continue on their prescribed treatment, many patients with schizophrenia fail to adhere to their medication. Interruption of antipsychotic treatment in patients with schizophrenia, through treatment discontinuation or inconsistent adherence, is associated with increases in rates of relapse, hospitalization, and treatment costs.2-5
Background: Poor adherence to treatment of chronic diseases is a worldwide problem of striking magnitude. Adherence to long-term therapy for chronic illnesses in developing countries averages 50%.6
References:
1. Swartz MS, Perkins DO, Stroup TS, et al. Assessing clinical and functional outcomes in the clinical antipsychotic trials of intervention effectiveness (CATIE) schizophrenia trial. Schizophr Bull 2003;29(1):33-43.
2. Herz MI, et al. Intermittent vs. maintenance medication in schizophrenia: two-year results. Arch Gen Psychiatry 1991;48:333-339.
3. Svarstad BL, Shireman TI, Sweeney JK. Using drug claims data to assess the relationship of medication adherence with hospitalization and costs. Psychiatr Serv 2001;52:805-811.
4. Ascher-Svanum H, Zhu B, Faries D, et al. A comparison of olanzapine and risperidone on the risk of psychiatric hospitalization in the naturalistic treatment of patients with schizophrenia. Ann Gen Hosp Psychiatry 2004;3(1):11.
5. Gilmer TP, Dolder CR, Lacro JP, et al. Adherence to treatment with antipsychotic medication and health care costs among Medicaid beneficiaries with schizophrenia. Am J Psychiatry 2004;161(4):692-699.
6. Haynes RB. Interventions for helping patients to follow prescriptions for medications. Cochrane Database of Systematic Reviews 2001;1.
7. Lehman AF, Lieberman JA, Dixon LB, et al. APA practice guideline for the treatment of patients with schizophrenia. Am J Psychiatry 2004;161(suppl 2):1-56.
5. ESTUDIOS OBSERVACIONALES Eficacia
Discontinuación por falta de respuesta
6. SOHO:�ESTUDIO OBSEVACIONAL DE ESQUIZOFRENIA A 2 AÑOS.
7. SOHO �EVALUACIÓN A 2 AÑOS. Section 7 Page 282 (started on mono analysis)
By definition, patients that had an overall CGI-S of 1 or 2 at baseline were excluded from the analysis of responders.
Following 24 months of treatment, there was a greater proportion of responders in the olanzapine group compared with the quetiapine, risperidone or haloperidol treatment groups
Comparison adjusted for baseline differences
The likelihood of response to treatment in the olanzapine group was significantly greater compared with quetiapine, risperidone or haloperidol (p<0.001; odds ratio comparisons)
The likelihood of response to treatment in the risperidone group was not significantly greater compared with quetiapine (p=0.071; odds ratio comparison).
There was no significant difference for odds ratio comparisons between the haloperidol and quetiapine groups, however; for the comparison of risperidone with haloperidol the p-value =0.094 – not significant at the p<0.001 level set for ICR study.
Section 7 Page 282 (started on mono analysis)
By definition, patients that had an overall CGI-S of 1 or 2 at baseline were excluded from the analysis of responders.
Following 24 months of treatment, there was a greater proportion of responders in the olanzapine group compared with the quetiapine, risperidone or haloperidol treatment groups
Comparison adjusted for baseline differences
The likelihood of response to treatment in the olanzapine group was significantly greater compared with quetiapine, risperidone or haloperidol (p<0.001; odds ratio comparisons)
The likelihood of response to treatment in the risperidone group was not significantly greater compared with quetiapine (p=0.071; odds ratio comparison).
There was no significant difference for odds ratio comparisons between the haloperidol and quetiapine groups, however; for the comparison of risperidone with haloperidol the p-value =0.094 – not significant at the p<0.001 level set for ICR study.
8. SOHO�TIEMPO PARA CAMBIO DESDE EL TRATAMIENTO INICIAL
10. CATIE Diseño Estudio
11. CATIE I TIEMPO DE DICONTINUACIÓN POR CUALQUIER CAUSA. The Kaplan Meier median is the time by which half of the patients have discontinued
The hazard ratio for olanzapine vs. quetiapine is 0.63: at any given time, patients on olanzapine are 63% less likely to discontinue treatment compared to patients on quetiapine.
The Hazard ratio is from Cox proportional hazards regression, and is the ratio of the probability of discontinuing the phase at any timepoint for one treatment group vs. another.The Kaplan Meier median is the time by which half of the patients have discontinued
The hazard ratio for olanzapine vs. quetiapine is 0.63: at any given time, patients on olanzapine are 63% less likely to discontinue treatment compared to patients on quetiapine.
The Hazard ratio is from Cox proportional hazards regression, and is the ratio of the probability of discontinuing the phase at any timepoint for one treatment group vs. another.
12. CATIE I TIEMPO DE DISCONTINUACIÓN POR FALTA DE EFICACIA. The Kaplan Meier 25th %ile is the time by which 25% of the patients have discontinued. The median can not be estimated due to low event rates.
The hazard ratio for olanzapine vs. quetiapine is 0.41: at any given time, patients on olanzapine are 41% less likely to discontinue treatment for lack of efficacy compared to patients on quetiapine.
The Hazard ratio is from Cox proportional hazards regression, and is the ratio of the probability of discontinuing the phase at any timepoint for one treatment group vs. another.The Kaplan Meier 25th %ile is the time by which 25% of the patients have discontinued. The median can not be estimated due to low event rates.
The hazard ratio for olanzapine vs. quetiapine is 0.41: at any given time, patients on olanzapine are 41% less likely to discontinue treatment for lack of efficacy compared to patients on quetiapine.
The Hazard ratio is from Cox proportional hazards regression, and is the ratio of the probability of discontinuing the phase at any timepoint for one treatment group vs. another.
13. CATIE FASE 2
14. CATIE II TIEMPO DE DISCONTINUACIÓN POR CUALQUIER CAUSA
15. CATIE II (I) TIEMPO DISCONTINUACIÓN POR FALTA DE EFICACIA
16. CATIE II (II) TIEMPO DISCONTINUACIÓN POR CUALQUIER CAUSA �
17. CLINICA DIARIA ¿Tenemos en nuestros pacientes un 74% de discontinuación?
18. CATIE vs CLINICA DIARIA No se incluyeron pacientes de primer episodio
No se combinaron drogas
¿Dosis son suficientes?
¿Típicos evaluadas son válidos?
19. CATIE vs CLINICA DIARIA No se incluyeron pacientes de primer episodio
No se combinaron drogas
¿Dosis son suficientes?
¿Típicos evaluadas son válidos?
20. PRIMER EPISODIO - Si es menor de seis meses: psicosis reactiva breve o trastorno esquizofreniforme DSM IV
- Sintomatología florida Schooler 86, Lieberman 95
- Generalmente hay prodromos de duración variable Lieberman 95
- El grado de respuesta terapéutica es mayor y más rápida. Loebel 92
- Requieren menos dosis antipsicóticos Meltzer 92
- Son más sensibles a reacciones de extrapiramidalismo. Lieberman 95 Keks 96
21. RESPUESTA AL TRATAMIENTO �DEL PRIMER EPISODIO Remisión completa: 73%
Remisión parcial: 16%
Sin remisión: 11%
22. CATIE vs CLINICA DIARIA No se incluyeron pacientes de primer episodio
No se combinaron drogas antipsicóticas
¿Dosis son suficientes?
¿Típicos evaluadas son válidos?
23. CATIE I: MEDICACIONES CONCOMITANTES.
24. CLINICA DIARIA ¿Qué porcentaje de nuestros pacientes esquizofrénicos están solo con monoterapia de antipsicóticos atípicos ?
25. CLINICA DIARIA Asociación de antipsicóticos
Atípico más típico en bajas dosis
Atípico más atípico
Asociación antipsicótico más antirrecurrencial
Asociación antipsicótico más antidepresivos
Asociación antipsicótico más BDZ
26. CATIE vs CLINICA DIARIA No se incluyeron pacientes de primer episodio
No se combinaron drogas
¿Dosis son suficientes?
¿Típicos evaluadas son válidos?
27. SOHO DOSIS SEGÚN GRUPO Section 7 Page 398 (started on mono)
Olanzapine: Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit – pp.409-410 (no depot available)
Quetiapine : Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit – pp. 411-412, Stats – (no depot available)
Risperidone : Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit –pp. 413-415 (oral and depot)
Haloperidol : Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit – pp. 404-405 (oral and depot)
Daily dose of each treatment is shown. Mean is the average dose, mode is the most commonly prescribed dose (or most common value). In situations where there was more than one mode, no mode is reported. Results include oral and depot.
The median dose of olanzapine and haloperidol remained at 10.0 mg/day throughout the 24 months. The median dose of quetiapine increased from 200.0 mg/day at baseline to 300.0 mg/day at 3 months, and 400 at 24 months. The median dose of risperidone also increased during treatment from 3.0 mg/day at baseline to 4.0 mg/day at 3, 6, 12 and 24 months.
Note: The dose summary at each time point is based on patients remaining on the same drug, therefore the patient numbers reduce over time.Section 7 Page 398 (started on mono)
Olanzapine: Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit – pp.409-410 (no depot available)
Quetiapine : Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit – pp. 411-412, Stats – (no depot available)
Risperidone : Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit –pp. 413-415 (oral and depot)
Haloperidol : Table 7.9.2 Dose (mg/day) of antipsychotics prescribed at each visit – pp. 404-405 (oral and depot)
Daily dose of each treatment is shown. Mean is the average dose, mode is the most commonly prescribed dose (or most common value). In situations where there was more than one mode, no mode is reported. Results include oral and depot.
The median dose of olanzapine and haloperidol remained at 10.0 mg/day throughout the 24 months. The median dose of quetiapine increased from 200.0 mg/day at baseline to 300.0 mg/day at 3 months, and 400 at 24 months. The median dose of risperidone also increased during treatment from 3.0 mg/day at baseline to 4.0 mg/day at 3, 6, 12 and 24 months.
Note: The dose summary at each time point is based on patients remaining on the same drug, therefore the patient numbers reduce over time.
28. CATIE II (I) DOSIS EN FASE Intent-to-treat (ITT) patients received at least one dose of study medication.
Dose and efficacy assessments are reported for the ITT patients. Safety assessments are reported for all randomized patients.Intent-to-treat (ITT) patients received at least one dose of study medication.
Dose and efficacy assessments are reported for the ITT patients. Safety assessments are reported for all randomized patients.
29. CATIE II (II) RANDOMIZACION Y TRATAMIENTO Intent-to-treat (ITT) patients received at least one dose of study medication.
Dose and efficacy assessments are reported for the ITT patients. Safety assessments are reported for all randomized patients.Intent-to-treat (ITT) patients received at least one dose of study medication.
Dose and efficacy assessments are reported for the ITT patients. Safety assessments are reported for all randomized patients.
30. CATIE II (III) RANDOMIZACIÓN Y TRATAMIENTO. Intent-to-treat (ITT) patients received at least one dose of study medication.
Dose and efficacy assessments are reported for the ITT patients. Safety assessments are reported for all randomized patients.Intent-to-treat (ITT) patients received at least one dose of study medication.
Dose and efficacy assessments are reported for the ITT patients. Safety assessments are reported for all randomized patients.
31. CLINICA DIARIA ¿Qué dosis son suficientes y habituales en la clínica?
32. CATIE vs CLINICA DIARIA No se incluyeron pacientes de primer episodio
No se combinaron drogas
¿Dosis son suficientes?
¿Típicos evaluadas son válidos?
33. CLINICA DIARIA ¿Perfenazina es igual a haloperidol?
Dosis de haloperidol elejida por profesional en SOHO
Dosis de perfenazina elejida por diseño de protocolo en CATIE
34. Key Points: The concept of treatment effectiveness considers the impact of the medication on controlling the various symptoms of the illness, as well as the safety and tolerability of the medication.1 Despite the established need for a patient to continue on their prescribed treatment, many patients with schizophrenia fail to adhere to their medication. Interruption of antipsychotic treatment in patients with schizophrenia, through treatment discontinuation or inconsistent adherence, is associated with increases in rates of relapse, hospitalization, and treatment costs.2-5
Background: Poor adherence to treatment of chronic diseases is a worldwide problem of striking magnitude. Adherence to long-term therapy for chronic illnesses in developing countries averages 50%.6
References:
1. Swartz MS, Perkins DO, Stroup TS, et al. Assessing clinical and functional outcomes in the clinical antipsychotic trials of intervention effectiveness (CATIE) schizophrenia trial. Schizophr Bull 2003;29(1):33-43.
2. Herz MI, et al. Intermittent vs. maintenance medication in schizophrenia: two-year results. Arch Gen Psychiatry 1991;48:333-339.
3. Svarstad BL, Shireman TI, Sweeney JK. Using drug claims data to assess the relationship of medication adherence with hospitalization and costs. Psychiatr Serv 2001;52:805-811.
4. Ascher-Svanum H, Zhu B, Faries D, et al. A comparison of olanzapine and risperidone on the risk of psychiatric hospitalization in the naturalistic treatment of patients with schizophrenia. Ann Gen Hosp Psychiatry 2004;3(1):11.
5. Gilmer TP, Dolder CR, Lacro JP, et al. Adherence to treatment with antipsychotic medication and health care costs among Medicaid beneficiaries with schizophrenia. Am J Psychiatry 2004;161(4):692-699.
6. Haynes RB. Interventions for helping patients to follow prescriptions for medications. Cochrane Database of Systematic Reviews 2001;1.
7. Lehman AF, Lieberman JA, Dixon LB, et al. APA practice guideline for the treatment of patients with schizophrenia. Am J Psychiatry 2004;161(suppl 2):1-56.Key Points: The concept of treatment effectiveness considers the impact of the medication on controlling the various symptoms of the illness, as well as the safety and tolerability of the medication.1 Despite the established need for a patient to continue on their prescribed treatment, many patients with schizophrenia fail to adhere to their medication. Interruption of antipsychotic treatment in patients with schizophrenia, through treatment discontinuation or inconsistent adherence, is associated with increases in rates of relapse, hospitalization, and treatment costs.2-5
Background: Poor adherence to treatment of chronic diseases is a worldwide problem of striking magnitude. Adherence to long-term therapy for chronic illnesses in developing countries averages 50%.6
References:
1. Swartz MS, Perkins DO, Stroup TS, et al. Assessing clinical and functional outcomes in the clinical antipsychotic trials of intervention effectiveness (CATIE) schizophrenia trial. Schizophr Bull 2003;29(1):33-43.
2. Herz MI, et al. Intermittent vs. maintenance medication in schizophrenia: two-year results. Arch Gen Psychiatry 1991;48:333-339.
3. Svarstad BL, Shireman TI, Sweeney JK. Using drug claims data to assess the relationship of medication adherence with hospitalization and costs. Psychiatr Serv 2001;52:805-811.
4. Ascher-Svanum H, Zhu B, Faries D, et al. A comparison of olanzapine and risperidone on the risk of psychiatric hospitalization in the naturalistic treatment of patients with schizophrenia. Ann Gen Hosp Psychiatry 2004;3(1):11.
5. Gilmer TP, Dolder CR, Lacro JP, et al. Adherence to treatment with antipsychotic medication and health care costs among Medicaid beneficiaries with schizophrenia. Am J Psychiatry 2004;161(4):692-699.
6. Haynes RB. Interventions for helping patients to follow prescriptions for medications. Cochrane Database of Systematic Reviews 2001;1.
7. Lehman AF, Lieberman JA, Dixon LB, et al. APA practice guideline for the treatment of patients with schizophrenia. Am J Psychiatry 2004;161(suppl 2):1-56.
35. ESTUDIOS OBSERVACIONALES Discontinuación por intolerancia
Efectos colaterales
36. ESTUDIOS OBSERVACIONALES y CONTROLADOS
Discontinuación por intolerancia
Efectos colaterales
37. CATIE I TIEMPO DE DISCONTINUACIÓN POR INTOLERANCIA� Kaplan Meier medians and 25th %ile can not be estimated due to low event rates
The hazard ratio for risperidone vs. olanzapine is 0.62: at any given time, patients on risperidone are 62% less likely to discontinue treatment for intolerability compared to patients on olanzapine. This difference is not significant since the overall p-value was not less than 0.05.
The Hazard ratio is from Cox proportional hazards regression, and is the ratio of the probability of discontinuing the phase at any timepoint for one treatment group vs. another.Kaplan Meier medians and 25th %ile can not be estimated due to low event rates
The hazard ratio for risperidone vs. olanzapine is 0.62: at any given time, patients on risperidone are 62% less likely to discontinue treatment for intolerability compared to patients on olanzapine. This difference is not significant since the overall p-value was not less than 0.05.
The Hazard ratio is from Cox proportional hazards regression, and is the ratio of the probability of discontinuing the phase at any timepoint for one treatment group vs. another.
38. RAZONES DE DISCONTINUACIÓN POR INTOLERANCIA:. FYI: the percentages of patients discontinued for intolerability differ slightly between this slide and the previous one because this slide is based on all randomized patients, and the previous slide is limited to ITT patients who took at least one dose of study medication.FYI: the percentages of patients discontinued for intolerability differ slightly between this slide and the previous one because this slide is based on all randomized patients, and the previous slide is limited to ITT patients who took at least one dose of study medication.
39. Discontinuación por intolerancia
Efectos colaterales
40. CATIE EFECTOS ADVERSOS
41. CATIE ESCALA DE MOVIMIENTOS ANORMALES
42. CATIE: SIMPSON-ANGUS (SEP) �
43. CATIE BARNES AKATHISIA RATING SCALE�
44. CRITERIOS de EXCLUSIÓN�¿Es esto un “bias”?� En CATIE se excluyeron para perfenazina pacientes con antecedentes de SEP
No se excluyeron para olanzapina o cloza antecedentes de desorden metabólico
No se excluyeron para risperidona antecedentes de SEP
No se excluyeron para ziprasidona antecedentes de cardiopatía.
45. SOHO�DISKINESIA TARDIA EN PAC. QUE MANTUVIERON TERAPIA INICIAL Section 8 Page 529 of 1166
Cumulative treatment emergent events from T1 to T6
This graph is a measure of TD that was not present at baseline and emerged during treatment within each treatment group.
Treatment emergent TD was greatest in the haloperidol group.
Olanzapine was significantly different to haloperidol and risperidone. Small patient numbers in the quetiapine group make it hard to draw statistical conclusions.
Section 8 Page 529 of 1166
Cumulative treatment emergent events from T1 to T6
This graph is a measure of TD that was not present at baseline and emerged during treatment within each treatment group.
Treatment emergent TD was greatest in the haloperidol group.
Olanzapine was significantly different to haloperidol and risperidone. Small patient numbers in the quetiapine group make it hard to draw statistical conclusions.
46. CLINICA DIARIA�MOVIMIENTOS ANORMALES POR AP:
47. PARKINSONISMO Parkinsonismo Motor
EPS
Distonía
Diskinesia tardía
Parkinsonismo Cognitivo
Pensamiento enlentecido y pobre
Sentimiento de vacío
Dificultades de concentración
48. PARKINSONISMO Parkinsonismo Social
Falta de iniciativa
Disminución de las energías
Pobreza de contactos sociales
Parkinsonismo Emocional
Indiferencia emocional
Anhedonia
Falta de placer en las actividades
49. PROLACTINA (NG/ML) EN ENSAYOS CONTROLADOS CON OLANZAPINA
50. LA PROLACTINA ES MÁS QUE�UNA HORMONA DE MATERNAJE Función sexual y maternal
Función en “coping” (afrontamiento) al stress
Función metabólica (hormona anabólica)
Función sobre SNC (crecimiento neuronal, sinaptogénesis y poda dendrítica)
Función sobre inmunomodulación
51. CLINICA DIARIA�AUMENTO PROLACTINA POR AP:
52. CLINICA DIARIA�OTROS EFECTOS ADVERSOS ENDÓCRINOS POR AP. Disminución de LH y FSH
Osteoporosis
Intolerancia a la glucosa
Síndrome metabólico
53. SOHO: GANANCIA MAYOR A 7 % DEL PESO CORPORAL PREVIO. Section 7 Pages 1188-1192 (started on mono)
Clinically significant weight gain is thought to be a gain >7% of the starting body weight.
the proportion of patients in the olanzapine group gaining >7% of their starting body weight was higher when compared with the other groups.Section 7 Pages 1188-1192 (started on mono)
Clinically significant weight gain is thought to be a gain >7% of the starting body weight.
the proportion of patients in the olanzapine group gaining >7% of their starting body weight was higher when compared with the other groups.
54. CATIE I: PROPORCIÓN DE SUJETOS QUE GANARON MÁS DEL 7 % DEL PESO CORPORAL.
55. CATIE I: CAMBIOS DESDE BASAL HASTA 2 ENTREVISTAS POSTERIORES patients were instructed to fast, nonfasting results were not excluded
Exposure-adjusted means are the estimated mean values that we would see at the average treatment duration across all groups (8.3 months). They are least squares means from an ANCOVA model adjusting for treatment duration.patients were instructed to fast, nonfasting results were not excluded
Exposure-adjusted means are the estimated mean values that we would see at the average treatment duration across all groups (8.3 months). They are least squares means from an ANCOVA model adjusting for treatment duration.
56. CAMBIO EN PESO CON ANTIPSICOTICOS.
57. CAMBIO DE PESO EN LA ERA PREANTIPSICOTICA “The taking of food fluctuates from complete refusal to the greatest voracity. The body weight usually falls at first, often to a considerable degree, even to extreme emaciation, in spite of the most abundant nourishment. Later, on the contrary, we see the weight not infrequently rise quickly in the most extraordinary way, so that patients in short time acquire an uncommonly well-nourished turgid appearance”
58. ¿POR QUÉ LOS PACIENTES GANAN PESO CON ANTIPSICÓTICOS?
59. INTERVENCIONES CONDUCTUALES PARA LA PÉRDIDA DE PESO [Keywords] 530, Maguire, Justice, CME, Optima Q, Optima, 6/18/2001, neuroscience, schizophrenia, psychosis, Zyprexa, Olanzapine, critical, breakthroughs, psychiatric, treatment, redefining, standard, care, Lilly, Echo Swinford, Angela Sisson, choices, results , weight, change ###
[Narration] Behavioral interventions in patients on atypical antipsychotics have been studied as to effectiveness. In a study by Wirshing et al (1), a stepwise approach was taken such that patients were subject to increasingly intensive interventions (self-weighing, food diary, nutrition consult, education, group support, exercise classes) depending on their ability to control their weight. ###
[Narration] The maximum weight gained during therapy and final weight gain after interventions is depicted in this graph for different drugs. Only clozapine showed a sustained increase in weight unresponsive to intervention.###
[Narration] It is important to note that these patients were not enrolled in one large, comparative trial but were rather enrolled in multiple controlled trials at Dr. Wirshing's site. Thus, they should be taken as pilot data but nonetheless suggest that behavioral interventions may be successful in moderating olanzapine-associated weight gain.###
[Narration] Average Duration of Treatment:###
[Narration] Clozapine, 27.2 wks###
[Narration] Olanzapine, 73.1 wks###
[Narration] Risperidone 25.8 wks###
[Narration] Haloperidol, 24.7 wks###
[Narration] Sertindole, 42.5 wks###
[Narration] 1 "Novel Antipsychotics: Comparison of Weight Gain Liabilities" by Wirshing DA et al. J Clin Psych 1999; 60(6):358-3###
[Keywords] 530, Maguire, Justice, CME, Optima Q, Optima, 6/18/2001, neuroscience, schizophrenia, psychosis, Zyprexa, Olanzapine, critical, breakthroughs, psychiatric, treatment, redefining, standard, care, Lilly, Echo Swinford, Angela Sisson, choices, results , weight, change ###
[Narration] Behavioral interventions in patients on atypical antipsychotics have been studied as to effectiveness. In a study by Wirshing et al (1), a stepwise approach was taken such that patients were subject to increasingly intensive interventions (self-weighing, food diary, nutrition consult, education, group support, exercise classes) depending on their ability to control their weight. ###
[Narration] The maximum weight gained during therapy and final weight gain after interventions is depicted in this graph for different drugs. Only clozapine showed a sustained increase in weight unresponsive to intervention.###
[Narration] It is important to note that these patients were not enrolled in one large, comparative trial but were rather enrolled in multiple controlled trials at Dr. Wirshing's site. Thus, they should be taken as pilot data but nonetheless suggest that behavioral interventions may be successful in moderating olanzapine-associated weight gain.###
[Narration] Average Duration of Treatment:###
[Narration] Clozapine, 27.2 wks###
[Narration] Olanzapine, 73.1 wks###
[Narration] Risperidone 25.8 wks###
[Narration] Haloperidol, 24.7 wks###
[Narration] Sertindole, 42.5 wks###
[Narration] 1 "Novel Antipsychotics: Comparison of Weight Gain Liabilities" by Wirshing DA et al. J Clin Psych 1999; 60(6):358-3###
60. ESTRATEGIAS PARA PREVENIR AUMENTO DE PESO
Estrógenos
Metformina (Glucophage ®)
Sibutramina (Ipomex® Aderan ®)
Fluoxetina (Prozac ®)
Amantadina (Symmetrel®)
Quetiapina (Seroquel)
Topiramato (Topamax®)
Orlistat
Antagonistas H2 ; Nizatadine (Axid®) , Ranitidina
(Taural) Cimetidina (Tagamet)
61. CLINICA DIARIA�AUMENTO DE PESO POR AP:
62. CATIE I ELECTOCARDIOGRAMA Y CATARATAS
63. CLINICA DIARIA�RIESGO DE EVENTOS CARDIOLÓGICOS POR AP:
64. EFECTOS ADVERSOS NEUROCOGNITIVOS
Sedación
Confusión
Deterioro de memoria
Enlentecimiento psicomotor
Delirium
Descenso del umbral convulsivo
65. CLINICA DIARIA �RIESGO DE EVENTOS NEUROCOGNITIVO POR AP:
66. CLINICA DIARIA �RIESGO DE SIADH POR AP:
67. RIESGO DE AUMENTO DE DESORDEN INMUNITARIO POR ANTIPSICÓTICOS
68. Parte 2 Presentar una nueva conceptualización de los antipsicóticos atípicos más acorde con los nuevos conocimientos científicos
y desafios clínicos .
69. � Tamayo,J; López-Mato,A; Téllez,J; Calil,HM; Fernández,A
Revista Latinoamericana de Psiquiatría, v.3, n.1, p. 5-36, 2003.
70. AA Y FUNCIÓN RECEPTORIAL This slide is a simplistic way to discuss the differences between the antipsychotics from a mechanistic point of view. It is important to point out the broad receptor binding affinity of olanzapine and how this relates to improvement in a wide range of psychiatric symptoms.This slide is a simplistic way to discuss the differences between the antipsychotics from a mechanistic point of view. It is important to point out the broad receptor binding affinity of olanzapine and how this relates to improvement in a wide range of psychiatric symptoms.
72. FARMACODINÁMIA DE AA
73. ATIPICIDAD: �PROPUESTAS EXISTENTES
74. ATIPICIDAD: PROPUESTAS
82. PORQUÉ ES AMPLIO ESPECTRO?� Mecanismo de acción más allá de la interacción DA con perfil de afinidad por otros receptores:
D1 (clozapina y olanzapina),
5-HT1A (clozapina y ziprasidona),
5-HT2C (sertindol, clozapina, olanzapina y ziprasidona),
5HT6 (clozapina, olanzapina y sertindol),
5HT7 (clozapina y risperidona),
?2 (risperidona),
H1 (clozapina, olanzapina, risperidona y quetiapina)
M4 (clozapina y olanzapina).
84. SPECTRUM II Acción terapéutica sobre algún otro trastorno psiquiátrico como trastorno bipolar, trastornos depresivos, tratornos de personalidad, drogodependencia, trastorno obsesivo-compulsivo, enfermedad de Parkinson, demencias…
85. SPECTRUM III Efectividad en resocialización (calidad de vida, funcionamiento global)
Eficacia a largo plazo
Eficacia en pacientes refractarios
Seguridad con mínimos efectos extrapiramidales, hormonales y otros
89. AA EFICACIA EN: ESQUIZOFRENIA
TRASTORNO BIPOLAR
TRASTORNO UNIPOLAR REFRACTARIO
TRASTORNOS DE PERSONALIDAD
TRASTORNO DE CONDUCTA
DEMENCIAS
TRASTORNOS DE ALIMENTACIÓN
TRASTORNOS DE ANSIEDAD (TAG,PTSD)
??????????
90. ¿POR QUÉ SEGUIR LLAMANDOLOS ANTIPSICÓTICOS?
¿POR QUÉ SEGUIR LLAMANDOLOS ATÍPICOS?
91. ¿QUÉ ANTIPSICÓTICO ELEGIRÍA UN PSIQUIÁTRA PARA ÉL Y SUS FAMILIARES?
92. LA MISMA MOLÉCULA NO ASEGURA EL MISMO MEDICAMENTO!!! Se analizaron distintas olanzapinas, algunas de ellas provienen de farmacias que las prepararon como recetas magistrales – no parece muy magistral lo que les salio-. Y otras fueron tomadas del mercado por el breve periodo en que fueron comercializadas, como el caso de la olanzapina de Luar en Cordoba y la de Dosa. El ketolactam, la amida y el ketotiolactam son productos de degradacion de la olanzapina y el N-oxido es una impureza de sintesis. En rojo se destacan los valores mas fuera de especificaciones. Hay casos pateticos como el de la olanzapina que fabricaba la Farmacia Vasallo, no solamente tenia el 8% la la olanzapina que deberia tener, sino que ademas tenia 10 veces mas impurezas que el maximo admisible.Se analizaron distintas olanzapinas, algunas de ellas provienen de farmacias que las prepararon como recetas magistrales – no parece muy magistral lo que les salio-. Y otras fueron tomadas del mercado por el breve periodo en que fueron comercializadas, como el caso de la olanzapina de Luar en Cordoba y la de Dosa. El ketolactam, la amida y el ketotiolactam son productos de degradacion de la olanzapina y el N-oxido es una impureza de sintesis. En rojo se destacan los valores mas fuera de especificaciones. Hay casos pateticos como el de la olanzapina que fabricaba la Farmacia Vasallo, no solamente tenia el 8% la la olanzapina que deberia tener, sino que ademas tenia 10 veces mas impurezas que el maximo admisible.
93. DEGRADACIÓN DE UNA OLANZAPINA GENÉRICA EN UN ENSAYO DE ESTABILIDAD ACELERADA La velocidad de degradacion de la olanzapina de Biocrom – actualmente en el mercado – demuestra que solo 45 dias a 33°C y 76% de humedad son suficientes para alcanzar el limite superior de impurezas admisible. La curva de degradacion muestra un perfil exponencial con un R casi perfecto.La velocidad de degradacion de la olanzapina de Biocrom – actualmente en el mercado – demuestra que solo 45 dias a 33°C y 76% de humedad son suficientes para alcanzar el limite superior de impurezas admisible. La curva de degradacion muestra un perfil exponencial con un R casi perfecto.
94. DIFERENTES FORMAS CRISTALINAS DE OLANZAPINA SE DISUELVEN DIFERENTEMENTE La olanzapina tiene varias formas de cristalizacion. Algunas son estables como la forma polimorfica 2 que presenta Zyprexa (y Midax) y otras forma son metaestables como la forma polimorfica 1 y 3. En Chile se vende Olivin que es una olanzapina que es una mezcla de polimorfos 1 y 3. Como claramente se ve la velocidad de disolucion, y por lo tanto los perfiles de absorcion son marcadamente diferentes de los de Zyprexa.La olanzapina tiene varias formas de cristalizacion. Algunas son estables como la forma polimorfica 2 que presenta Zyprexa (y Midax) y otras forma son metaestables como la forma polimorfica 1 y 3. En Chile se vende Olivin que es una olanzapina que es una mezcla de polimorfos 1 y 3. Como claramente se ve la velocidad de disolucion, y por lo tanto los perfiles de absorcion son marcadamente diferentes de los de Zyprexa.
95. SI CREE QUE �ELIGE LO MEJOR �ELIJA LO SEGURO �
96. LA CLINICA ES SOBERANA..�Y MUCHO MÁS DIVERTIDA MUCHAS GRACIAS POR ATENDER...
