1. Slide No. 1 • Footer • rFVIIa: usos clínicos para manejo del sangrado crítico. Servicio de Terapia Intensiva - Hospital de Clínicas
Montevideo – Uruguay.
2. Slide No. 2 • Footer • rFVIIa en el manejo del sangrado crítico Introducción
Mecanismo de acción
Uso en hemofilia congénita
Uso en hemofilia adquirida
Déficit congénito de FVII
Trombastenia de Glanzmann y trombocitopatías
Nuevas indicaciones (Uso compasivo)
3. Slide No. 3 • Footer • INTRODUCCION 1981 la Dra. Ulla Hedner purifica pequeñas cantidades de FVIIa.
1983 se publica el primer trabajo en el J Clin Invest.
1988 primer paciente hemofílico tratado en forma efectiva en una cirugía ortopédica mayor.
1996 aprobación para su uso en Europa.
2000 aprobación para su en Japón.
2003 aprobación para su uso en Europa para la Tromboastenia de Glanzmann.
4. Slide No. 4 • Footer • NovoSeven® – Factor recombinante VIIa (rFVIIa)
5. Slide No. 5 • Footer • Comparación de FVIIa recombinante con el FVII plasmático.
6. Slide No. 6 • Footer • Mecanismos de acción NovoSeven® tiene dos mecanismos de acción
• Sustitución del FVIIa congénitamente ausente en la iniciación de la hemostasia.
• Derivación (by-pass) de defectos en el proceso normal de coagulación en ciertos pacientes con coagulopatía.
7. Slide No. 7 • Footer • El sistema hemostático �Las tres fases
Hemostasia primaria: vasoconstricción y tapón plaquetario
Hemostasia secundaria: coágulo de fibrina
Fibrinólisis: lisis del coágulo
8. Slide No. 8 • Footer • FVIIa en la iniciación de la coagulación
9. Slide No. 9 • Footer • Hemostasia primaria – Formación del trombo plaquetario
10. Slide No. 10 • Footer • Fisiopatología de la hemofilia A
11. Slide No. 11 • Footer •
12. Slide No. 12 • Footer •
13. Slide No. 13 • Footer •
14. Slide No. 14 • Footer • rFVIIa en la hemofilia A con inhibidores
15. Slide No. 15 • Footer • El FVIIa se une a las Plaquetas La baja afinidad de la unión del rFVIIa a las plaquetas activadas explica el requerimiento de altas dosis.
El hallazgo de que el rFVIIa no se une al resto de las plaquetas explica porqué no se observa una coagulación sistémica luego de la utilización del rFVIIa.
FVIIa Binding to Platelets
To assess the interaction of FVIIa with platelets, the binding of FVIIa to platelets was examined using indirect immunofluorescence and flow cytometry. The results are shown on this slide. The units of measure in flow cytometry are relative fluorescence. The fluorescence levels from several different experiments were normalized so that binding from several people could be compared. FVIIa did not bind to the unactivated platelets (shown in red), nor did it bind to activated platelets in the absence of calcium (shown in orange). However, in the presence of calcium, FVIIa bound weakly to activated platelets with a half-maximal binding at 100 nM (in contrast to binding to tissue factor [TF], which is half maximal at less than 0.01 nM).
Monroe DM et al. Br J Haematol 1997;99:542–547.La baja afinidad de la unión del rFVIIa a las plaquetas activadas explica el requerimiento de altas dosis.
El hallazgo de que el rFVIIa no se une al resto de las plaquetas explica porqué no se observa una coagulación sistémica luego de la utilización del rFVIIa.
FVIIa Binding to Platelets
To assess the interaction of FVIIa with platelets, the binding of FVIIa to platelets was examined using indirect immunofluorescence and flow cytometry. The results are shown on this slide. The units of measure in flow cytometry are relative fluorescence. The fluorescence levels from several different experiments were normalized so that binding from several people could be compared. FVIIa did not bind to the unactivated platelets (shown in red), nor did it bind to activated platelets in the absence of calcium (shown in orange). However, in the presence of calcium, FVIIa bound weakly to activated platelets with a half-maximal binding at 100 nM (in contrast to binding to tissue factor [TF], which is half maximal at less than 0.01 nM).
Monroe DM et al. Br J Haematol 1997;99:542–547.
16. Slide No. 16 • Footer • • Convierte el fibrinógeno en monómeros de fibrina
• Activa más plaquetas y otros factores, amplificando así adicionalmente el sistema.
• Activa el inhibidor de la fibrinólisis activado por trombina (TAFI)
• Activa el factor XIII, que ayuda a estabilizar el coágulo de fibrina. Hemostasia secundaria – La explosión de trombina
17. Slide No. 17 • Footer • Fibrinólisis – Rutas de la fibrinólisis
18. Slide No. 18 • Footer • Fibrinólisis – Equilibrio hemostático
19. Slide No. 19 • Footer • Indicaciones autorizadas Hemofilia congénita con inhibidores para los factores de coagulación VIII o IX >5 BU o que se espera que tengan una respuesta anamnésica alta con los factores VIII o IX.
Hemofilia adquirida.
Deficiencia congénita del factor VII.
Trombastenia de Glanzmann con anticuerpos contra glucoproteína GP IIb-IIIa y/ó HLA, y con respuestas pasadas o presentes a la transfusión de plaquetas.
20. Slide No. 20 • Footer • Hemofilia Congénita Hemofilia A: déficit de factor VIII
Hemofilia B: déficit de factor IX
1800 pacientes registrados en el país
Con inhibidor aproximadamente 45 pacientes
Hemofilia
Leve: 5 a 25%
Moderada: 1 a 4%
Severa: <1%
21. Slide No. 21 • Footer • Hemofilia Congénita Inhibidores:
Prevalencia:
Hemofilia A ~30% (10% a 50%)
Hemofilia B 3% a 5%
Unidades de medición:
Unidades Bethesda = UB
1 BU = cantidad de inhibidor que neutraliza el 50% de la actividad del factor luego de 2 h a 37°C.
Bajo título: < 5UB
Alto título: > 5UB
The prevalence of inhibitors for persons with severe FVIII deficiency has been estimated to be approximately 30% with a reported range of 10% to 50%. In individuals with severe FIX deficiency, inhibitors are mush less common with a prevalence of approximately 3% to 5%. The presence of an inhibitor is measured in the Bethesda assay and is reported in Bethesda units (BU). One BU is the amount of inhibitor that will result in a loss of 50% of factor activity when the patient’s plasma is incubated with normal plasma for 2 hours at 37? C.
The prevalence of inhibitors for persons with severe FVIII deficiency has been estimated to be approximately 30% with a reported range of 10% to 50%. In individuals with severe FIX deficiency, inhibitors are mush less common with a prevalence of approximately 3% to 5%. The presence of an inhibitor is measured in the Bethesda assay and is reported in Bethesda units (BU). One BU is the amount of inhibitor that will result in a loss of 50% of factor activity when the patient’s plasma is incubated with normal plasma for 2 hours at 37? C.
22. Slide No. 22 • Footer • Hemofilia Congénita Dosis efectiva:
90 - 120 mcg/kg cada 2-3 horas hasta lograr hemostasia
Dosis > 200 mcg/kg puede disminuir la necesidad de dosis repetidas.
Kenet et al han utilizado mega dosis de 300 mcg/kg, siendo estas dosis efectivas y seguras.
23. Slide No. 23 • Footer • Hemofilia adquirida Descripción
Autoanticuerpos contra el factor VIII
Se presentan clinicamente con sangrados espontáneos.
Generalmente en pacientes añosos
Antecedentes de enfermedades autoinmunes, cáncer, embarazo, exposición a drogas.
Incidencia de 1 por millon, por año
Laboratorio: KPTT prolongado (que no corrige con plasma normal). Niveles del FVIII 1-2%
24. Slide No. 24 • Footer • Hemofilia adquirida Mortalidad del 13 al 22%
Objetivos del tratamiento
Control del sangrado: rFVIIa – FEIBA – PCCs – FVIIIporcino
Eliminar el anticuerpo
Se utilizan agentes inmunosupresores (ciclofosfamida, ciclosporina ó corticoterapia)solos ó en combinación con plasmaféresis
25. Slide No. 25 • Footer • Hemofilia adquirida�Experiencia con rFVIIa Tratamiento de salvataje: >90% de eficacia
Primera línea terapéutica: 100% de eficacia
NovoSeven en hemofilia adquirida
> eficacia que FVIIIp, PCC, PCCa,
> seguridad
26. Slide No. 26 • Footer • Déficit de FVII Alteración hereditaria del sangrado
Presenta hemorragias severas cuando los niveles plasmáticos son <2%. Sangrado en articulaciones, menstruaciones importantes, epistaxis, sangrado después de una cirugía.
Incidencia 2/1000000.
Tratamiento: rFVIIa, FVII derivado de plasma, plasma fresco, y PCCs.
Dosis recomendada de rFVIIa: 20-30 µg/kg de peso.
Eficacia > al 90%.
Su uso fue aprobado en Europa por la EMEA en enero de 2004.
27. Slide No. 27 • Footer • Alteraciones plaquetarias Alteraciones de la cantidad de las plaquetas
Transplante de Stem Cell
Fiebre hemorrágica – Dengue
Alteraciones en la función plaquetaria
Trombastenia de Glanzmann
Síndrome de Bernard Soulier
Enfermedad de pool de depósito
28. Slide No. 28 • Footer • Trombastenia de Glanzmann Alteración congénita del sangrado
Defecto en receptores específicos de la membrana plaquetaria (GP IIb/IIIa).
Incidencia 1/1000000
Las plaquetas pierden la habilidad de agregarse y formar un tapón hemostático.
Más frecuente en la mujer. Edad < 20 años.
Se caracteriza por epistaxis, sangrado de encías, hematomas, mentruaciones abundantes, anemia.
Requerimiento transfusional en el 77% de los casos
29. Slide No. 29 • Footer • Trombastenia de Glanzmann 3 Tipos
Tipo I: GP IIb/IIIa ausente (<5%)
Tipo II: GP IIb/IIIa (5-20%)
Variantes (modificaciones cualitativas de la GP IIb/IIIa)
Tratamiento convencional: transfusión de plaquetas, agentes antifibrinolíticos, desmopresina
Dosis de rFVIIa:
80-120 mcg/kg cada 2 horas hasta lograr hemostasia.
30. Slide No. 30 • Footer • Déficit de FXI Alteración hereditaria del sangrado
Es un desórden genético frecuente entre la población judía Ashkenazi.
Se diferencia de la hemofilia A y B por no presentar sangrado en articulaciones y músculos. No son frecuentes los sangrados espontáneos. Tienen riesgo de sangrado después de una cirugía
Tratamiento convencional: plasma fresco, concentrados plasmáticos de FXI y desmopresina
Existen 4 publicaciones que informan un uso exitoso con NovoSeven en profilaxis quirúrgica y manejo del sangrado
31. Slide No. 31 • Footer • Enfermedad de Von Willebrand – Tipo 3 Alteración hereditaria del sangrado
Caracterizada por ausencia parcial o total del factor de von Willebrand
El Factor vW transporta al FVIII en el torrente sanguíneo y media la adhesión plaquetaria en el sitio de la lesión.
Ocurre cuando una persona tiene 2 genes defectuosos
6% del total de enfermedad de vW.
Tratamiento convencional:
Concentrados de FVIII/vW
Concentrados de FVIII más transfusiones de plaquetas
Seis pacientes fueron tratados con rFVIIa con una efectividad del 95%
32. Slide No. 32 • Footer • rFVIIa para reversión de la anticoagulación En ratas tratadas con Warfarina, el rFVIIa corrigió el tiempo de protrombina.
En voluntarios sanos, tratados con acenocumarol, la prolongación del RIN (>2) se revirtió con una dosis de rFVIIa con dosis de entre 5 a 320 mcg/kg
Dosis < 120 mcg/kg pueden normalizar el RIN por el lapso de 24 horas.
rFVIIa resultó eficaz a una dosis de 90 mcg/kg para revertir la acción de fondaparinux con una normalización en la generación de trombina por más de 6 horas luego de la administración.
La incidencia de trombosis resultó de un 1-2%
33. Slide No. 33 • Footer • Otras indicaciones (uso compasivo) Sangrado quirúrgico
Trauma
Hemorragia intracerebral
Hemorragia posparto
Hepatectomía
Cirugía cardíaca
Injuria cerebral
34. Slide No. 34 • Footer • Indicaciones quirúrgicas • Hepatectomía parcial,
• Transplante ortotópico de hígado,
• Cirugía cardíaca (de adulto e infantil),
• Cirugía de la columna vertebral, y
• Cirugía reconstructora de la pelvis.
35. Slide No. 35 • Footer • Otras situaciones hemorrágicas Ejemplos de otras situaciones hemorrágicas críticas son
• Hemorragia postransplante de médula ósea.
• Infecciones víricas hemorrágicas (por ejemplo, dengue).
• Hemorragia aguda por varices esofágicas aguda.
• Hemorragia intracerebral.
• Lesión por traumatismo cerebral.
• Hemorragia posparto.
• Quemaduras.
36. Slide No. 36 • Footer • Trauma La hemorragia severa es la principal causa de muerte en pacientes traumatizados.
El 65% de las muertes ocurre después de la admisión en hospitalaria.
El traumatismo severo se correlaciona con coagulopatía pos-traumática, acidosis, hipotermia y síndrome de transfusiones múltiples.
37. Slide No. 37 • Footer • La injuria traumática es la principal causa de muerte entre los 5–44 años
La transfusión masiva de GR es una variable de riesgo independiente de morbilidad y mortalidad.
El sangrado es la segunda causa de mortalidad en la injuria del SNC
La prevención del sangrado, previene la exanguinación, reduce la incidencia de shock y previene la muerte en los pacientes traumatizados. Trauma is highly prevalent in the young, and bleeding episodes associated with traumatic injury are an important cause of mortality.
Preventing, or significantly reducing, bleeding following trauma will lead to a reduction in the number of RBC units transfused. This, in turn, will reduce:
The incidence of haemodynamic shock
The number of transfusion-related complications, such as MOF and ARDS
The length of stay in ICU
The time spent on mechanical ventilation
Trauma is highly prevalent in the young, and bleeding episodes associated with traumatic injury are an important cause of mortality.
Preventing, or significantly reducing, bleeding following trauma will lead to a reduction in the number of RBC units transfused. This, in turn, will reduce:
The incidence of haemodynamic shock
The number of transfusion-related complications, such as MOF and ARDS
The length of stay in ICU
The time spent on mechanical ventilation
38. Slide No. 38 • Footer • Trauma�Boffard et al. J Trauma (2005).�
39. Slide No. 39 • Footer • Upon receiving 6 units of RBC within a 4-hour period, eligible patients within each trauma population were equally randomised to receive either placebo or NovoSeven®.
Patients receiving a further 2 units of RBC (a total of 8 units of RBC) then received their assigned study medication upon transfusion of the 8th unit of RBC:
Three IV injections of NovoSeven® (200, 100 and 100 µg/kg), or
Three placebo injections
The second and third doses were administered after 1 and 3 hours.
During the first 48 hours after administration the following were monitored: transfusion and infusion requirements; adverse events; surgical procedures.
During the 30-day follow-up, mortality, time on ventilator, hospitalization data, and serious adverse events including pre-defined critical complications (MOF and acute respiratory distress syndrome [ARDS]) were recorded.Upon receiving 6 units of RBC within a 4-hour period, eligible patients within each trauma population were equally randomised to receive either placebo or NovoSeven®.
Patients receiving a further 2 units of RBC (a total of 8 units of RBC) then received their assigned study medication upon transfusion of the 8th unit of RBC:
Three IV injections of NovoSeven® (200, 100 and 100 µg/kg), or
Three placebo injections
The second and third doses were administered after 1 and 3 hours.
During the first 48 hours after administration the following were monitored: transfusion and infusion requirements; adverse events; surgical procedures.
During the 30-day follow-up, mortality, time on ventilator, hospitalization data, and serious adverse events including pre-defined critical complications (MOF and acute respiratory distress syndrome [ARDS]) were recorded.
40. Slide No. 40 • Footer • Boffard et al. J Trauma (2005).� Variable de análisis primaria:
Número de unidades de GR transfundidas dentro de las 48hs de administrado el rFVIIa.
Resultados de la terapia:
Número de transfusiones de otros hemoderivados, mortalidad, días en respirador y días en UTI.
Evaluación de la seguridad
41. Slide No. 41 • Footer • As would be expected, most of the blunt trauma was due to motor vehicle accidents and falls.
As would be expected, most of the blunt trauma was due to motor vehicle accidents and falls.
42. Slide No. 42 • Footer • Penetrating trauma was mostly due to gunshot wounds and stab wounds and was predominantly in males.
Penetrating trauma was mostly due to gunshot wounds and stab wounds and was predominantly in males.
43. Slide No. 43 • Footer • Treatment with NovoSeven® produced a significant reduction in RBC requirements over 48 hours in patients surviving >48 hours (p=0.019).
However, a statistically significant haemostatic effect for NovoSeven® treatment was observed at 12 hours (p=0.008) and at 24 hours (p=0.018) following the initial treatment dose.
This effect was supported by observations of significant reductions in the transfusion rate in patients treated with NovoSeven® relative to placebo (0.26 units/hour versus 0.37 units/hour, p=0.036).Treatment with NovoSeven® produced a significant reduction in RBC requirements over 48 hours in patients surviving >48 hours (p=0.019).
However, a statistically significant haemostatic effect for NovoSeven® treatment was observed at 12 hours (p=0.008) and at 24 hours (p=0.018) following the initial treatment dose.
This effect was supported by observations of significant reductions in the transfusion rate in patients treated with NovoSeven® relative to placebo (0.26 units/hour versus 0.37 units/hour, p=0.036).
44. Slide No. 44 • Footer • Administration of NovoSeven® significantly reduced the need for massive transfusions by 56% (95% CI: [9%; 79%]; p=0.03) in the first 48 hours after administration in the blunt trauma group.
The need for massive transfusion in penetrating trauma patients was reduced by 63% (95% CI: [-12%; 88%]; p= 0.08).
The importance of reducing massive transfusions has recently been demonstrated. A retrospective study has shown that mortality is significantly correlated with the amount of RBC transfused:1
In 5645 acute trauma patients:
479/5645 (8%) patients received RBCs
In patients receiving 11 to 20 units RBCs mortality was 30%
In patients receiving >20 units RBCs, mortality rose significantly to >50%
This effect was independent of severity of injury
1Como JJ et al. Transfusion 2004;44:809-13.
Administration of NovoSeven® significantly reduced the need for massive transfusions by 56% (95% CI: [9%; 79%]; p=0.03) in the first 48 hours after administration in the blunt trauma group.
The need for massive transfusion in penetrating trauma patients was reduced by 63% (95% CI: [-12%; 88%]; p= 0.08).
The importance of reducing massive transfusions has recently been demonstrated. A retrospective study has shown that mortality is significantly correlated with the amount of RBC transfused:1
In 5645 acute trauma patients:
479/5645 (8%) patients received RBCs
In patients receiving 11 to 20 units RBCs mortality was 30%
In patients receiving >20 units RBCs, mortality rose significantly to >50%
This effect was independent of severity of injury
1Como JJ et al. Transfusion 2004;44:809-13.
45. Slide No. 45 • Footer • Further support for the haemostatic effect of NovoSeven® came from significant reductions in both FFP (p=0.036) and platelets (p=0.023) relative to placebo in blunt trauma patients who survived 48 hours or more.
The requirement for cryoprecipitate in patients treated with NovoSeven® showed a trend towards reduction relative to placebo (p=0.053).
Further support for the haemostatic effect of NovoSeven® came from significant reductions in both FFP (p=0.036) and platelets (p=0.023) relative to placebo in blunt trauma patients who survived 48 hours or more.
The requirement for cryoprecipitate in patients treated with NovoSeven® showed a trend towards reduction relative to placebo (p=0.053).
46. Slide No. 46 • Footer • The results from this randomised, double-blind, placebo controlled, parallel group study demonstrate a significant advance in the treatment of critically bleeding, severely ill trauma patients.
NovoSeven® significantly reduced the need for transfusion in patients with blunt trauma injuries after they have already received eight units of red blood cells.
There was also a significant reduction in the need for massive transfusions.
The results from this randomised, double-blind, placebo controlled, parallel group study demonstrate a significant advance in the treatment of critically bleeding, severely ill trauma patients.
NovoSeven® significantly reduced the need for transfusion in patients with blunt trauma injuries after they have already received eight units of red blood cells.
There was also a significant reduction in the need for massive transfusions.
47. Slide No. 47 • Footer • Hemorragia intracerebral (HIC) Factores de riesgo:
Hipertensión arterial
Terapia anticoagulante oral
Otras causas:
Sangrado de tumor cerebral
Abuso de drogas
Alteraciones del sangrado
En el 2001, 150.000 sufrieron HIC en el mundo desarrollado
48. Slide No. 48 • Footer • HIC�Mayer et al. N Engl J Med. (2005).�
49. Slide No. 49 • Footer •
50. Slide No. 50 • Footer • Patients were enrolled from August 2002 through March 2004 at 73 hospitals in 20 countries. Patients were enrolled from August 2002 through March 2004 at 73 hospitals in 20 countries.
51. Slide No. 51 • Footer • Subjects in whom spontaneous ICH was confirmed by CT scanning within 3 hours of symptom onset were eligible for enrollment and were treated within 1 hour of the baseline scan.Subjects in whom spontaneous ICH was confirmed by CT scanning within 3 hours of symptom onset were eligible for enrollment and were treated within 1 hour of the baseline scan.
52. Slide No. 52 • Footer • Of the 400 randomized patients, 1 subsequently withdrew consent, leaving 399 patients for analysis. Baseline characteristics were similar across groups and representative of what is known from the literature.
There were 96, 108, 92, and 103 patients in the placebo, 40 ?g/kg, 80 ?g/kg, and 160 ?g/kg treatment arms, respectively. The mean age was 66 years; 61% were male, and most of the patients were white. The mean ICH volume at baseline (24 mL; range, 0.4 to 153 mL) was similar in the 4 groups.
70% of the patients were treated within a 3-hour time period.
The timing of treatment was similar in the 4 treatment groups.Of the 400 randomized patients, 1 subsequently withdrew consent, leaving 399 patients for analysis. Baseline characteristics were similar across groups and representative of what is known from the literature.
There were 96, 108, 92, and 103 patients in the placebo, 40 ?g/kg, 80 ?g/kg, and 160 ?g/kg treatment arms, respectively. The mean age was 66 years; 61% were male, and most of the patients were white. The mean ICH volume at baseline (24 mL; range, 0.4 to 153 mL) was similar in the 4 groups.
70% of the patients were treated within a 3-hour time period.
The timing of treatment was similar in the 4 treatment groups.
53. Slide No. 53 • Footer • Total Intracranial Blood Volume (ICH + IVH Volume) [not shown]
The treatment effect was similar (P for trend = 0.0156 [ICTR value]; P for trend = 0.02 [NEJM value]) for hemorrhages with extension into the ventricles. The combined rFVIIa groups showed significant reduction in ICH + intraventricular hemorrhage (IVH) volume compared to placebo (P = 0.006 [NEJM value]).Total Intracranial Blood Volume (ICH + IVH Volume) [not shown]
The treatment effect was similar (P for trend = 0.0156 [ICTR value]; P for trend = 0.02 [NEJM value]) for hemorrhages with extension into the ventricles. The combined rFVIIa groups showed significant reduction in ICH + intraventricular hemorrhage (IVH) volume compared to placebo (P = 0.006 [NEJM value]).
54. Slide No. 54 • Footer • The trial showed a statistically significant reduction (38% relative reduction) in mortality for the combined rFVIIa groups compared to placebo (P = 0.025, chi-square test [ICTR value]; P = 0.02 [NEJM value]).
The use of the combination of death and severe disability as a single category made it unlikely that decisions to withdraw life support influenced the results.The trial showed a statistically significant reduction (38% relative reduction) in mortality for the combined rFVIIa groups compared to placebo (P = 0.025, chi-square test [ICTR value]; P = 0.02 [NEJM value]).
The use of the combination of death and severe disability as a single category made it unlikely that decisions to withdraw life support influenced the results.
55. Slide No. 55 • Footer • Scores of 0 to 1 on the mRS, 7 to 8 on the E-GOS, 95 to 100 on the Barthel Index, and 0 to 1 on the NIHSS indicated a favorable outcome.
Percentages may not total 100 because of rounding off.
Twenty patients (5%) were alive but lacked complete outcome data and thus had some or all scores at day 15 carried forward.Scores of 0 to 1 on the mRS, 7 to 8 on the E-GOS, 95 to 100 on the Barthel Index, and 0 to 1 on the NIHSS indicated a favorable outcome.
Percentages may not total 100 because of rounding off.
Twenty patients (5%) were alive but lacked complete outcome data and thus had some or all scores at day 15 carried forward.
56. Slide No. 56 • Footer • In total, 23 patients experienced 26 serious thromboembolic events.
There appeared to be more thromboembolic SAEs in the actively treated groups (7%) compared to placebo (2%); however, the difference was not statistically significant (P = 0.12, Fisher’s exact test). In total, 23 patients experienced 26 serious thromboembolic events.
There appeared to be more thromboembolic SAEs in the actively treated groups (7%) compared to placebo (2%); however, the difference was not statistically significant (P = 0.12, Fisher’s exact test).
57. Slide No. 57 • Footer • The use of rFVIIa offers hope for a future treatment of acute ICH—an area where there is currently very little opportunity to actively intervene. Available medical options have been shown to have limited success. The role of surgical treatment of ICH remains controversial.1 It is possible that the use of an agent such as rFVIIa may enhance the safety of early surgical evacuation of haematomas.1,2
rFVIIa appears not only to limit haematoma growth and reduce mortality but also to improve functional outcomes. Thus, more patients receiving the treatment survive and are functionally more independent than patients receiving placebo.3
Until further safety and efficacy data are available, rFVIIa should be used with caution in patients with ICH who have risk factors for thromboembolic disease. More research is required to identify such patients and to determine the optimal therapeutic window. More data are also needed regarding the potential use of rFVIIa for management of patients with ICH related to anticoagulant therapy.3
Morgenstern LB et al. Neurology. 2001;56:1294-1299.
Brown DL et al. N Engl J Med. 2005;352:828-830.
Mayer SA et a. N Engl J Med. 2005;352:777-785.The use of rFVIIa offers hope for a future treatment of acute ICH—an area where there is currently very little opportunity to actively intervene. Available medical options have been shown to have limited success. The role of surgical treatment of ICH remains controversial.1 It is possible that the use of an agent such as rFVIIa may enhance the safety of early surgical evacuation of haematomas.1,2
rFVIIa appears not only to limit haematoma growth and reduce mortality but also to improve functional outcomes. Thus, more patients receiving the treatment survive and are functionally more independent than patients receiving placebo.3
Until further safety and efficacy data are available, rFVIIa should be used with caution in patients with ICH who have risk factors for thromboembolic disease. More research is required to identify such patients and to determine the optimal therapeutic window. More data are also needed regarding the potential use of rFVIIa for management of patients with ICH related to anticoagulant therapy.3
Morgenstern LB et al. Neurology. 2001;56:1294-1299.
Brown DL et al. N Engl J Med. 2005;352:828-830.
Mayer SA et a. N Engl J Med. 2005;352:777-785.
58. Slide No. 58 • Footer • Hemorragia Posparto
59. Slide No. 59 • Footer • Hemorragia Posparto En 11 mujeres se obtuvo una respuesta parcial o satisfactoria con el uso de rFVIIa.
En 1 paciente no se obtuvo respuesta.
En 4 pacientes que fueron sometidas a embolización arterial, hubo una disminución significativa del sangrado pero no se detuvo en forma completa.
El uso de rFVIIa puede ser beneficioso en el tratamiento de la hemorragia posparto con riesgo de vida
60. Slide No. 60 • Footer • Cirugía Cardiaca
61. Slide No. 61 • Footer • El uso de rFVIIa redujo en forma significativa el uso de transfusiones, Diprose et al, Br J Anaesth, Sept 2005.
El uso de rFVIIa como terapia de rescate es efectivo en lograr la hemostasia, prevenir la reexploración quirúrgica y en la reducción de los requerimientos transfusionales. Halkos et al, Ann Thorac Surg 2005; 79: 1303-6.
El uso tardío de rFVIIa resultó seguro pero no incremento la eficacia respecto de la terapéutica hemostática convencional. Von Heymann et al, Crit Care Med, 2005; 33:2241-46. Cirugía Cardiaca
62. Slide No. 62 • Footer • Hemorragia variceal esofágica aguda
63. Slide No. 63 • Footer • Hemorragia variceal esofágica aguda El rFVIIa corrige el tiempo de protrombina en los pacientes cirróticos.
No se observaron diferencias significativas respecto al tratamiento standard en la población general.
El rFVIIa disminuye en forma significativa el número de fallas y el control de sangrado a las 24 horas en el subgrupo Child B y C con varices esofágicas.
No hubo diferencias respecto a placebo en la mortalidad a 5 o 42 días.
No hubo diferencias significativas en la incidencia de efectos adversos inclusive eventos tromboembólicos respecto a placebo.
64. Slide No. 64 • Footer • Cirugía Prostática
65. Slide No. 65 • Footer • Estudio doble ciego, randomizado controlado contra placebo.
Pacientes sometidos a prostactetomía retropúbica.
Dosis 20 y 40 mcg/kg versus placebo.
Perdida sanguínea promedio:
20 mcg/kg: 1235 mL
40 mcg/kg: 1089 mL p=0.001
Placebo: 2688 mL
Ningún paciente del grupo de 40 mcg/kg (16 pacientes) requirieron transfusiones. Siendo la diferencia significativa de ambos grupos respecto a placebo.
No se observaron efectos adversos (el riesgo estándar de trombosis venosa es del 2-4% en esta cirugía) Cirugía Prostática
