Tout sur l AVC en 3 heures

1. Tout sur l�AVC en 3 heures �

2. Epid�miologie

3. I. �pid�miologie 1. incidence

4. Incidence D�finition : nombre de nouveaux AVC par an dans une population d�finie

5. Incidence Mondiale : 16 millions de 1er AVC en 2005 (Strong et al, 2007) Pays industrialis�s : 2400 AVC / an / million d�habitants (Hankey et Warlow, 1999) 80 % isch�miques / 20 % h�morragiques 75% 1er AVC / 25% r�cidives 500 AIT / an / million d�habitants (Hankey et Warlow, 1999)

6. Incidence Influence de l��ge :

7. Incidence Variations g�ographiques :

8. Incidence Evolution dans le temps : Diminution par cat�gorie d��ge Augmentation globale Augmentation des cardio-emboliques (Lemesle et al, 1989) D�passe maintenant celle de l�infarctus du myocarde Incidence relative des �v�nements c�r�braux / coronaires : 1.19 (95% CI 1.06-1.33) pour tout �v�nement 1.40 (1.23-1.59) pour �v�nements non mortels 1.21 (1.04-1.41) si exclusion des AIT et angors instables. (Rothwell et al, 2005)

9. Incidence Projections : Augmentation dans les pays industrialis�s Augmentation de l�esp�rance de vie Baisse de la mortalit� coronaire Baisse de mortalit� par AVC Augmentation dans les pays � faibles revenus Augmentation de l�esp�rance de vie SIDA Modification des facteurs de risque (tabac, surpoids, HTA, diab�te, cholest�rol et inactivit� physique) (Strong et al, 2007)

10. I. �pid�miologie 2. pr�valence

11. Pr�valence D�finition : nombre de sujets dans une population d�finie qui ont un jour dans leur vie eu un AVC ou un AIT Pays industrialis�s : 12000 personnes / million d�habitants (Hankey et Warlow, 1999)

12. Pr�valence

13. I. �pid�miologie 3. facteurs de risque

14. Facteurs de risque non modifiables Age Sexe masculin Migraine Ethnie Pr�disposition g�n�tique

15. Hypertension art�rielle Risque relatif = 5 40% pour 5-10 mmHg de PA Pas de seuil. (Mac Mahon et al, 1990)

16. Hypertension art�rielle Facteur de risque de r�cidive (Rodgers et al, 1996)

17. Hypercholest�rol�mie Cholest�rol et isch�mie. cholest�rol total et LCL plus �lev�s. Cholest�rol et h�morragie c�r�brale. �tudes cas t�moins : cholest�rol total plus bas.

18. Autres facteurs modifiables

19. I. �pid�miologie 4. mortalit�

20. Mortalit� D�finition : tout d�c�s survenant end�ans le mois suivant l�AVC

21. Mortalit� Mondiale : 5.7 millions de d�c�s par AVC en 2005 (Strong et al, 2007) Pays industrialis�s : 480 d�c�s par AVC / an / million d�habitants (Hankey et Warlow, 1999) 3� cause de d�c�s (2� chez la femme)

22. Mortalit� Variations selon l��ge :

23. Mortalit� Variations g�ographiques :

24. Mortalit� Variations dans le temps :

25. Nombre de d�c�s attendus par AVC (millions) (Strong et al, 2007) Mortalit�

26. I. �pid�miologie 5. r�cidives

27. R�cidives Globale : 5% par an (Hankey et Warlow, 1999) Extr�me h�t�rog�n�it� : Patients � faible risque de r�cidive (Hankey et Warlow, 1999) Sujets jeunes (Leys et al, 2002) Dissections (Leys et al, 1995; Touze et al, 2002) Patients � haut risque de r�cidive (Hankey et Warlow, 1999) St�noses carotides > 70% (NASCET 1991; ECST 1991) Fibrillation auriculaire (EAFT 1993)

28. II. Sous types d�AVC

30. Pourquoi la connaissance des sous types d�AVC est elle importante ? pathologies diff�rentes pronostics diff�rents (mortalit� et r�cidive) pr�vention diff�rente

31. III. Cas particulier : AIT

32. Accident isch�mique transitoire Signification : Marqueur de risque �lev� d�accident isch�mique constitu� � court et moyen terme. 50% des infarctus constitu�s survenant apr�s un AIT surviennent dans la semaine qui suit (Weimar et al, 2003) m�mes causes et facteurs de risques que les infarctus c�r�braux

33. Accident isch�mique transitoire D�finition classique : Perte brutale de fonction c�r�brale ou oculaire d�installation brutale, d�origine isch�mique, dont les sympt�mes durent < 24 h et r�gressent sans s�quelle.

34. Accident isch�mique transitoire D�finition classique : Difficult�s : D�finition bas�e sur id�e que l�isch�mie ne laisse pas de s�quelle anatomique. Limite de 24h arbitraire (pas de support anatomique La plupart des AIT durent moins d�une heure. Etude NINDS (groupe placebo): si d�ficit persistant � 1h, probabilit� d�AIT = 2% (Marler et al, 2000) 50% des AIT ont anomalies de diffusion (Engelter et al, 1999) D�finition non op�rationnelle depuis thrombolyse < 3h.

35. Accident isch�mique transitoire Nouvelle d�finition : D�ficit neurologique bref d� � une isch�mie c�r�brale focale ou r�tinienne, ne laissant pas de signe d�infarctus c�r�bral r�cent en imagerie, et r�gressant habituellement en moins d�une heure (Albers et al 2002)

36. Accident isch�mique transitoire Marqueur de risque �lev� apr�s un AIT: Age Pression art�rielle Sympt�mes c�r�braux Diab�te D�lai apr�s l�AIT

37. Accident isch�mique transitoire Marqueur de risque �lev� apr�s un AIT (ABCD2): Age Blood pressure Cerebral Duration Diabetes mellitus

38. Prise en charge en phase aigu�

39. L�AVC est une urgence �tat des connaissances L�AVC est une urgence m�dicale et occasionnellement une urgence chirurgicale La majorit� des patients pr�sentant un infarctus c�r�bral n�arrivent pas assez rapidement � l�h�pital Le d�lai entre le d�but de l�AVC et l�admission � l�h�pital est ; R�duit si le centre 15 est contact� imm�diatement Augment� si le m�decin g�n�raliste est appel� en premier The aims of public education initiatives are to enable and encourage the general population to recognise immediately the symptoms of stroke, to realise that urgent medical attention is needed, and to use the emergency transportation services and immediately go to an adequately equipped hospital. Primary contact with general practitioners may cause delays and prevent early start of adequate therapy (Evenson et al. 2000). Educational efforts should be directed to patients at risk for stroke, their families, caregivers or co-workers and to large employers (Wein et al 2000). Teaching the public about symptoms and signs of stroke is one of the highest priorities of public medical education. Inaccurate initial diagnosis by professional groups represents a major problem. Ambulance dispatchers may have false positive assessment rate of up to 50%, and even in trained paramedics, this rate is about 25% (Kothari et al. 1997). However, this result can be improved by adequate training (Kothari et al. 1997). Physicians also need to be trained in the recognition of symptoms and signs of acute stroke and the necessity of immediate transportation to an adequately equipped unit. The medical personnel should be trained in recognising the acute presentations of ischaemic stroke and should be able to cope with the early complications after stroke. Training should include the ability to conduct a medical examination that focuses on the Niveau of consciousness, presence of focal weakness, presence of seizure activity and recognition of aphasia and other major cognitive disturbances. The concept of �Time is Brain� should be understood by all involved in the �Stroke Chain of Survival�. No waste of time should be allowed when the patient has arrived to hospital and written standards for in-hospital delays should be available in hospitals receiving patients with acute stroke. Although such pathways have not been shown to be effective by themselves (Kwan and Sandercock 2003) they can be considered effective in preventing in-hospital delays. One example is that set by the National Institute of Neurological Disorders and Stroke in 1997 (National Institute of Neurological Disorders and Stroke 1997). The aims of public education initiatives are to enable and encourage the general population to recognise immediately the symptoms of stroke, to realise that urgent medical attention is needed, and to use the emergency transportation services and immediately go to an adequately equipped hospital. Primary contact with general practitioners may cause delays and prevent early start of adequate therapy (Evenson et al. 2000). Educational efforts should be directed to patients at risk for stroke, their families, caregivers or co-workers and to large employers (Wein et al 2000). Teaching the public about symptoms and signs of stroke is one of the highest priorities of public medical education. Inaccurate initial diagnosis by professional groups represents a major problem. Ambulance dispatchers may have false positive assessment rate of up to 50%, and even in trained paramedics, this rate is about 25% (Kothari et al. 1997). However, this result can be improved by adequate training (Kothari et al. 1997). Physicians also need to be trained in the recognition of symptoms and signs of acute stroke and the necessity of immediate transportation to an adequately equipped unit. The medical personnel should be trained in recognising the acute presentations of ischaemic stroke and should be able to cope with the early complications after stroke. Training should include the ability to conduct a medical examination that focuses on the Niveau of consciousness, presence of focal weakness, presence of seizure activity and recognition of aphasia and other major cognitive disturbances. The concept of �Time is Brain� should be understood by all involved in the �Stroke Chain of Survival�. No waste of time should be allowed when the patient has arrived to hospital and written standards for in-hospital delays should be available in hospitals receiving patients with acute stroke. Although such pathways have not been shown to be effective by themselves (Kwan and Sandercock 2003) they can be considered effective in preventing in-hospital delays. One example is that set by the National Institute of Neurological Disorders and Stroke in 1997 (National Institute of Neurological Disorders and Stroke 1997).

40. Unit� neurovasculaire L�unit� neurovasculaire (UNV) est une zone g�ographiquement d�finie d�un h�pital qui prend en charge les patients admis pour un AVC est compos�e d�une �quipe sp�cialis�e, assurant une approche coordonn�e et multidisciplinaire du traitement et de la prise en charge du malade est constitu�e de m�decins, d�infirmi�res, de kin�sith�rapeutes, d�ergoth�rapeutes, d�orthophonistes et d�assistantes sociales1 20032003

41. Unit� neurovasculaire Les traitement en UNV, en comparaison aux traitements en unit� de soins conventionnelle1 ; r�duisent la mortalit� (r�duction du risque absolu de 3%) r�duisent la d�pendance (5%) r�duisent la n�cessit� d�institutionnalisation (2%) Tous les patients, quels que soient leur sexe, leur �ge, le type d�infarctus c�r�bral et sa s�v�rit�, semblent b�n�ficier des traitements prodigu�s en UNV1 24.01.0824.01.08

42. Traitement G�n�ral Contenu Monitoring Prise en charge pulmonaire et respiratoire Solutions hydriques intraveineuses Pression Art�rielle M�tabolisme glucidique Temp�rature corporelle 24.01.0824.01.08

43. Traitement Sp�cifique Contenu Traitement thrombolytique Traitement anti-thrombotique pr�coce Traitement de l�hypertension intracr�nienne Pr�vention et traitement des complications 23.01.08 PAR23.01.08 PAR

44. Traitement Thrombolytique(rtPA IV) �tat des connaissances (NINDS1, ECASS I2 + II3, ATLANTIS4) Le rtPA intraveineux (0.9mg/kg, max 90mg) donn� dans les 3 heures apr�s le d�but de l�infarctus c�r�bral, am�liore significativement le pronostic des patients 23.01.08 PAR: Thrombolytic therapy with rtPA (0.9 mg/kg body weight, maximum dose 90mg) given within 3 hours after stroke onset, significantly improves outcome in patients with acute ischaemic stroke {The National Institute of Neurological Disorders and Stroke rt-PA Stroke Study Group, 1995 #678}: the NNT to achieve a favourable clinical outcome after 3 months is 7. By contrast, the ECASS and ECASS II studies did not show statistically significant superiority of rtPA for the primary endpoints when treatment was given within 6 hours {Hacke, 1998 #84;Hacke, 1995 #83}. Trials with rtPA, involving a total of 2,889 patients, have shown a significant reduction in the number of patients with death or dependency (OR 0.83; 95%CI 0.73-0.94) {Wardlaw, 2003 #910}. A pooled analysis of individual data of rtPA trials showed that, even within a 3-hour window, earlier treatment results in a better outcome (0-90 min: OR 2.11; 95%CI 1.33 to 3.55; 90-180 min: OR 1.69; 95%CI 1.09 to 2.62) {Hacke, 2004 #510}. This analysis suggested a benefit up to 4.5 hours. Ongoing trials (ECASS III, IST-3) are further investigating the benefits of rtPA beyond 3 hours. 23.01.08 PAR: Thrombolytic therapy with rtPA (0.9 mg/kg body weight, maximum dose 90mg) given within 3 hours after stroke onset, significantly improves outcome in patients with acute ischaemic stroke {The National Institute of Neurological Disorders and Stroke rt-PA Stroke Study Group, 1995 #678}: the NNT to achieve a favourable clinical outcome after 3 months is 7. By contrast, the ECASS and ECASS II studies did not show statistically significant superiority of rtPA for the primary endpoints when treatment was given within 6 hours {Hacke, 1998 #84;Hacke, 1995 #83}. Trials with rtPA, involving a total of 2,889 patients, have shown a significant reduction in the number of patients with death or dependency (OR 0.83; 95%CI 0.73-0.94) {Wardlaw, 2003 #910}. A pooled analysis of individual data of rtPA trials showed that, even within a 3-hour window, earlier treatment results in a better outcome (0-90 min: OR 2.11; 95%CI 1.33 to 3.55; 90-180 min: OR 1.69; 95%CI 1.09 to 2.62) {Hacke, 2004 #510}. This analysis suggested a benefit up to 4.5 hours. Ongoing trials (ECASS III, IST-3) are further investigating the benefits of rtPA beyond 3 hours.

45. Traitement Thrombolytique(rtPA IV)

46. Traitement Thrombolytique(rtPA IV) Donn�es sp�cifiques Une analyse combin�e, des 6 �tudes sur le rtPA IV, confirme que la thrombolyse IV pourrait �tre efficace jusque 4.5 heures1 La prudence est de mise lorsque le rtPA IV est envisag� chez les patients avec un infarctus c�r�bral s�v�re (NIHSS>25), ou si le CT met en �vidence des signes pr�coces et �tendus d�isch�mie Le traitement thrombolytique doit �tre administr� par un neurologue exp�riment�, apr�s que l�imagerie c�r�brale ait �t� lue par des m�decins exp�riment�s dans la lecture de ce type d�examen2 23.01.08 PAR23.01.08 PAR

47. Traitement Thrombolytique(rtPA IV) Donn�es sp�cifiques Facteurs associ�s avec une majoration du risque h�morragique1 hyperglyc�mie ant�c�dent de diab�te s�v�rit� initiale (NIHSS) �ge avanc� long d�lai dans l�administration du traitement utilisation pr�alable d�aspirine ant�c�dent d�insuffisance cardiaque congestive violations de protocole (selon les crit�res de NINDS) Aucun de ces facteurs ne contrebalance l�effet b�n�fique global du rtPA 23.01.08 PAR: Post hoc analyses have identified the following potential factors associated with increased risk of intracerebral bleeding complications after rtPA use {Lansberg, 2007 #485}: elevated serum glucose; history of diabetes; baseline symptom severity; advanced age; increased time to treatment; previous aspirin use; history of congestive heart failure; low plasminogen activator inhibitor; NINDS protocol violations. However, none of these factors reversed the overall benefit of rtPA.23.01.08 PAR: Post hoc analyses have identified the following potential factors associated with increased risk of intracerebral bleeding complications after rtPA use {Lansberg, 2007 #485}: elevated serum glucose; history of diabetes; baseline symptom severity; advanced age; increased time to treatment; previous aspirin use; history of congestive heart failure; low plasminogen activator inhibitor; NINDS protocol violations. However, none of these factors reversed the overall benefit of rtPA.

48. Traitement Sp�cifique Recommandations (1) Il est recommand� d�administrer, dans les 3 heures qui suivent le d�but d�un infarctus c�r�bral, du rtPA IV (0.9mg/kg de poids corporel, dose maximale de 90mg), en donnant 10% de la dose totale en bolus suivie d�une perfusion de 60 minutes (Cat�gorie I, Niveau A) L�administration du rtPA IV, au-del� des 3 heures, pourrait �galement �tre b�n�fique pour les infarctus c�r�braux (Cat�gorie I, Niveau B), mais son utilisation n�est pas recommand�e en pratique routini�re. L�utilisation de techniques d�imagerie multimodale pourrait �tre utile � la s�lection de certains candidats � une thrombolyse (Cat�gorie III, Niveau C) 23.01.08 PAR23.01.08 PAR

49. Traitement Sp�cifique Recommandations (2) Il est recommand� de diminuer les pressions art�rielles sup�rieures ou �gales � 185/110 mmHg, avant la thrombolyse (Cat�gorie IV, BPC) Le rtPA IV peut �tre utilis� chez les patients pr�sentant une crise d��pilepsie au d�but de l�infarctus c�r�bral, si le d�ficit neurologique est attribuable � l�isch�mie c�r�brale aigu� (Cat�gorie IV, BPC) Le rtPA IV peut �tre �galement utilis� chez certains patients de plus de 80 ans, malgr� le fait que cette indication soit en-dehors de l�indication r�glementaire (Cat�gorie III, Niveau C) 23.01.08 PAR23.01.08 PAR

50. EMEA : AMM conditionnelle (2002) Condition 1: prouver que les r�sultats en pratique de soins sont superposables � ceux des patients du groupe rtPA des essais : registre SITS-MOST Condition 2: faire un nouvel essai au del� de 3heures : ECASS 3

51. SITS-MOST

52. SITS-MOST

53. SITS-MOST

54. SITS-MOST

55. SITS-MOST

56. SITS-MOST

57. ECASS 3

59. NNT to prevent 1 mRS 2-6 < 90 minutes : 2 90 � 180 minutes : 7 180-270 minutes : 14

60. Traitement Antiplaquettaire �tat des connaissances L�aspirine a �t� �valu�e dans l�infarctus c�r�bral aigu (<48 h) dans de larges �tudes randomis�es et contr�l�es1,2 Elle entra�ne une r�duction significative de la mortalit� et de la perte d�autonomie (NNT 70) ainsi que du nombre de r�cidive d�infarctus c�r�bral (NNT 140) Une �tude de phase III avec l�abciximab, un inhibiteur de la glycoprot�ine IIb-IIIA, a �t� pr�matur�ment stopp�e suite � l�augmentation du taux d�h�morragies3 26.01.08: The results of two large randomized, non-blinded, intervention studies indicate that aspirin is safe and effective when started within 48 hours after stroke {International-Stroke-Trial-Collaborative-Group, 1997 #908;CAST-Collaborative-Group, 1997 #907}. In absolute terms, 13 more patients were alive and independent at the end of follow-up for every 1000 patients treated. Furthermore, treatment increased the odds of making a complete recovery from the stroke (OR 1.06; 95%CI 1.01-1.11): 10 more patients made a complete recovery for every 1000 patients treated. Antiplatelet therapy was associated with a small but definite excess of two symptomatic intracranial haemorrhages for every 1000 patients treated, but this was more than offset by a reduction of seven recurrent ischaemic strokes and about one pulmonary embolism for every 1000 patients treated. In a double-blind phase II, the GPIIb-IIIa inhibitor abciximab produced a non-significant shift in favourable outcomes, as measured by modified Rankin scores (mRS) at 3 months, compared with placebo (OR 1.20; 95%CI 0.84-1.70) {AbESST investigators, 2005 #888}. A phase III study evaluating the safety and efficacy of abciximab has been halted because of an increased rate of bleeding with abciximab {Adams, 2007 #887}. 26.01.08: The results of two large randomized, non-blinded, intervention studies indicate that aspirin is safe and effective when started within 48 hours after stroke {International-Stroke-Trial-Collaborative-Group, 1997 #908;CAST-Collaborative-Group, 1997 #907}. In absolute terms, 13 more patients were alive and independent at the end of follow-up for every 1000 patients treated. Furthermore, treatment increased the odds of making a complete recovery from the stroke (OR 1.06; 95%CI 1.01-1.11): 10 more patients made a complete recovery for every 1000 patients treated. Antiplatelet therapy was associated with a small but definite excess of two symptomatic intracranial haemorrhages for every 1000 patients treated, but this was more than offset by a reduction of seven recurrent ischaemic strokes and about one pulmonary embolism for every 1000 patients treated. In a double-blind phase II, the GPIIb-IIIa inhibitor abciximab produced a non-significant shift in favourable outcomes, as measured by modified Rankin scores (mRS) at 3 months, compared with placebo (OR 1.20; 95%CI 0.84-1.70) {AbESST investigators, 2005 #888}. A phase III study evaluating the safety and efficacy of abciximab has been halted because of an increased rate of bleeding with abciximab {Adams, 2007 #887}.

61. Anticoagulation H�parine non fractionn�e Absence de r�elle �tude ayant �valu� l�h�parine IV L��tude IST n�a pas d�montr� de r�el b�n�fice des patients trait�s par h�parine SC, suite � une majoration des HIC1 H�parines de bas poids mol�culaires (HBPM) Absence de b�n�fice sur le pronostic (nadroparine, certoparine, tinzaparine, dalteparine) H�parino�des (orgaran) Pas d�effet dans l��tude TOAST2 26.01.08: Subcutaneous unfractionated heparin (UFH) at low or moderate doses {International-Stroke-Trial-Collaborative-Group, 1997 #908}, nadroparin {Kay, 1995 #215;Wong, 2007 #477}; certoparin {Diener, 2001 #53}, tinzaparin {Bath, 2001 #15}, dalteparin {Berge, 2000 #21} and intravenous danaparoid {The Publications Committee for the Trial of ORG 10172 in Acute Stroke Treatment (TOAST) Investigators, 1998 #216} have failed to show an overall benefit of anticoagulation when initiated within 24 to 48 hours from stroke onset. Improvements in outcome or reductions in stroke recurrence rates were mostly counterbalanced by an increased number of haemorrhagic complications. In a meta-analysis of 22 trials, anticoagulant therapy was associated with about nine fewer recurrent ischaemic strokes per 1000 patients treated (OR 0.76; 95%CI 0.65-0.88), and with about nine more symptomatic intracranial haemorrhages per 1000 (OR 2.52; 95%CI 1.92-3.30) {Gubitz, 2004 #918}. However, the quality of the trials varied considerably. The anticoagulants tested were standard UFH, low molecular weight heparins, heparinoids, oral anticoagulants, and thrombin inhibitors.26.01.08: Subcutaneous unfractionated heparin (UFH) at low or moderate doses {International-Stroke-Trial-Collaborative-Group, 1997 #908}, nadroparin {Kay, 1995 #215;Wong, 2007 #477}; certoparin {Diener, 2001 #53}, tinzaparin {Bath, 2001 #15}, dalteparin {Berge, 2000 #21} and intravenous danaparoid {The Publications Committee for the Trial of ORG 10172 in Acute Stroke Treatment (TOAST) Investigators, 1998 #216} have failed to show an overall benefit of anticoagulation when initiated within 24 to 48 hours from stroke onset. Improvements in outcome or reductions in stroke recurrence rates were mostly counterbalanced by an increased number of haemorrhagic complications. In a meta-analysis of 22 trials, anticoagulant therapy was associated with about nine fewer recurrent ischaemic strokes per 1000 patients treated (OR 0.76; 95%CI 0.65-0.88), and with about nine more symptomatic intracranial haemorrhages per 1000 (OR 2.52; 95%CI 1.92-3.30) {Gubitz, 2004 #918}. However, the quality of the trials varied considerably. The anticoagulants tested were standard UFH, low molecular weight heparins, heparinoids, oral anticoagulants, and thrombin inhibitors.

62. Traitement Sp�cifique Recommendations (4/5) L�aspirine (160 � 325 mg) doit �tre prescrite dans les 48 heures apr�s un infarctus c�r�bral (Cat�gorie I, Niveau A) Si une thrombolyse est envisag�e ou r�alis�e, il est recommand� d�attendre 24 heures avant de commencer un traitement par aspirine ou un autre traitement anti-thrombotique (Cat�gorie IV, BPC) L�utilisation d�autres agents anti-plaquettaires (seuls ou en association) n�est pas recommand�e � la phase aigu� de l�infarctus c�r�bral (Cat�gorie III, Niveau C) L�utilisation d�inhibiteurs de la glycoprot�ine IIb-IIIa n�est pas recommand�e (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

63. Traitement Sp�cifique Recommendations (5/5) L�administration pr�coce d�h�parine non fractionn�e (HNF), d�h�parine de bas poids mol�culaire (HBPM) ou d�h�parino�des n�est pas recommand�e pour le traitement des patients avec un infarctus c�r�bral aigu (Cat�gorie I, Niveau A) Actuellement, il n�existe aucune recommandation pour traiter les patients, victimes d�un infarctus c�r�bral, avec des agents neuroprotecteurs (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

64. Hypertension Intracr�nienne Prise en charge de base �l�vation de la t�te de 30� par rapport au corps Contr�le de la douleur et s�dation si n�cessaire Osmoth�rapie (glyc�rol, mannitol, solutions salines hypertoniques) Assistance respiratoire Barbituriques, hyperventilation, ou ��THAM-buffer�� Traiter la fi�vre L�hypothermie pourrait r�duire la mortalit�1 26.01.08: Medical therapy in patients with large space-occupying infarctions and brain oedema is based mostly on observational data. Basic management includes head positioning at an elevation of up to 30�, avoidance of noxious stimuli, pain relief, appropriate oxygenation and normalizing body temperature. If intracranial pressure (ICP) monitoring is available, cerebral perfusion pressure should be kept above 70�mmHg {Unterberg, 1997 #234}. Intravenous glycerol (4 x 250 ml of 10% glycerol over 30�60 minutes) or mannitol (25�50 g every 3�6 hours) is first line medical treatment if clinical or radiological signs of space-occupying oedema occur {Righetti, 2002 #146;Bereczki, 2001 #23}. Intravenous hypertonic saline solutions are probably similarly effective {Schwarz, 2002 #154}. Hypotonic and glucose-containing solutions should be avoided as replacement fluids. Dexamethasone and corticosteroids are not useful {Qizilbash, 2002 #143}. Thiopental given as a bolus can quickly and significantly reduce ICP, and can be used to treat acute crises. Barbiturate treatment requires ICP and electroencephalography (EEG) monitoring and careful haemodynamic monitoring, as a significant blood pressure drop may occur. Mild hypothermia (i.e. brain temperature between 32-33�C) reduces mortality in patients with severe MCA infarcts, but may cause severe side effects including recurrent ICP crisis during re-warming {Schwab, 1998 #152;Steiner, 2001 #163}. In a small RCT, mild hypothermia (35�C) in addition to decompressive surgery produced a trend towards a better clinical outcome than decompressive surgery alone (P=0.08) {Els, 2006 #250}. 26.01.08: Medical therapy in patients with large space-occupying infarctions and brain oedema is based mostly on observational data. Basic management includes head positioning at an elevation of up to 30�, avoidance of noxious stimuli, pain relief, appropriate oxygenation and normalizing body temperature. If intracranial pressure (ICP) monitoring is available, cerebral perfusion pressure should be kept above 70�mmHg {Unterberg, 1997 #234}. Intravenous glycerol (4 x 250 ml of 10% glycerol over 30�60 minutes) or mannitol (25�50 g every 3�6 hours) is first line medical treatment if clinical or radiological signs of space-occupying oedema occur {Righetti, 2002 #146;Bereczki, 2001 #23}. Intravenous hypertonic saline solutions are probably similarly effective {Schwarz, 2002 #154}. Hypotonic and glucose-containing solutions should be avoided as replacement fluids. Dexamethasone and corticosteroids are not useful {Qizilbash, 2002 #143}. Thiopental given as a bolus can quickly and significantly reduce ICP, and can be used to treat acute crises. Barbiturate treatment requires ICP and electroencephalography (EEG) monitoring and careful haemodynamic monitoring, as a significant blood pressure drop may occur. Mild hypothermia (i.e. brain temperature between 32-33�C) reduces mortality in patients with severe MCA infarcts, but may cause severe side effects including recurrent ICP crisis during re-warming {Schwab, 1998 #152;Steiner, 2001 #163}. In a small RCT, mild hypothermia (35�C) in addition to decompressive surgery produced a trend towards a better clinical outcome than decompressive surgery alone (P=0.08) {Els, 2006 #250}.

65. Hypertension Intracr�nienne Infarctus h�misph�riques malins Analyse combin�e de 3 �tudes europ�ennes randomis�es et contr�l�es sur la craniectomie d�compressive (N=93)1,2 : R�duction significative de la mortalit� � 30 jours Augmentation significative du nombre de patients avec un mRS <4 ou un mRS <3 dans le groupe trait� � un an Pas d�augmentation du nombre de survivants avec un mRS=5 L�intervention chirurgicale doit �tre r�alis�e dans les 48 heures1,2 Le c�t� de l�infarctus n�influence pas le pronostic1,2 Un �ge > 50 ans est un facteur de mauvais pronostic3 26.01.08: Malignant MCA infarction: A pooled analysis of 93 patients included in three European RCTs (DECIMAL, DESTINY, HAMLET) showed that, compared with the control group, at 1 year more patients in the decompressive surgery group had a mRS <4 or mRS <3, and more survived (NNTs 2, 4 and 2, respectively) {Vahedi, 2007 #240;Juttler, 2007 #961}. There was no increase in the proportion of patients who survived surgery in a vegetative stage (mRS 5). Inclusion criteria for this combined analysis were age 18-60 years, NIHSSS >15, decrease in Niveau of consciousness to a score of 1 or greater on item 1a of the NIHSS, infarct signs on CT of 50 % or more of the MCA territory or >145 cm� on DWI, and inclusion <45 hours after onset (surgery <48 hours). Follow-up of survival and functional status beyond 1 year is currently ongoing in the DECIMAL and DESTINY studies {Juttler, 2007 #961}. A systematic review of 12 observational retrospective studies found age above 50 years to be a predictor of poor outcome. The timing of surgery, side of infarction, clinical signs of herniation before surgery, and involvement of other vascular territories did not significantly affect outcome {Gupta, 2004 #266}.26.01.08: Malignant MCA infarction: A pooled analysis of 93 patients included in three European RCTs (DECIMAL, DESTINY, HAMLET) showed that, compared with the control group, at 1 year more patients in the decompressive surgery group had a mRS <4 or mRS <3, and more survived (NNTs 2, 4 and 2, respectively) {Vahedi, 2007 #240;Juttler, 2007 #961}. There was no increase in the proportion of patients who survived surgery in a vegetative stage (mRS 5). Inclusion criteria for this combined analysis were age 18-60 years, NIHSSS >15, decrease in Niveau of consciousness to a score of 1 or greater on item 1a of the NIHSS, infarct signs on CT of 50 % or more of the MCA territory or >145 cm� on DWI, and inclusion <45 hours after onset (surgery <48 hours). Follow-up of survival and functional status beyond 1 year is currently ongoing in the DECIMAL and DESTINY studies {Juttler, 2007 #961}. A systematic review of 12 observational retrospective studies found age above 50 years to be a predictor of poor outcome. The timing of surgery, side of infarction, clinical signs of herniation before surgery, and involvement of other vascular territories did not significantly affect outcome {Gupta, 2004 #266}.

66. Hypertension Intracr�nienne RRA (ARR) et OR des pronostic d�favorables � 12 mois : analyse combin�e des 3 �tudes sur la craniectomie d�compressive1 26.01.08:26.01.08:

67. Hypertension Intracr�nienne Recommendations (1/2) Une d�compression chirurgicale, dans les 48 heures qui suivent le d�but des sympt�mes est recommand�e, chez les patients de moins de 60 ans et qui pr�sentent un infarctus c�r�bral malin et �volutif, de l�ACM (Cat�gorie I, Niveau A) Il est recommand� de recourir � une osmoth�rapie pour traiter une hypertension intracr�nienne, avant une intervention neurochirurgicale lorsque cette derni�re est envisag�e (Cat�gorie III, Niveau C) 23.01.08 PAR23.01.08 PAR

68. Hypertension Intracr�nienne Recommendations (2/2) Aucune recommandation ne peut �tre formul�e concernant les traitements antipyr�tiques pour les patients avec un infarctus associ� � un effet de masse (Cat�gorie IV, BPC) Il est recommand� d�envisager une ventriculostomie ou une d�compression chirurgicale en cas d�infarctus c�r�belleux volumineux comprimant le tronc c�r�bral (Cat�gorie III, Niveau C) 23.01.08 PAR23.01.08 PAR

70. Essais randomis�es





75. Pr�vention primaire

76. Pr�vention Primaire 25.01.0825.01.08

77. Hypertension art�rielle (HTA) �tat des connaissances L�HTA (>120/80mmHg) est le facteur de risque d�AVC le plus important et le plus facilement modifiable Une diminution de l�HTA entra�ne une r�duction significative de l�incidence des AVC1 Aucune classe d�anti-hypertenseurs ne semble clairement sup�rieure LIFE: le lorsatan est sup�rieur � l�at�nolol2 ALLHAT: la chlorthalidone est plus efficace que l�amlodipine et le lisinopril3 26.01.0826.01.08

78. �tat des connaissances Le diab�te est un facteur de risque ind�pendant d�AVC Am�liorer le contr�le glyc�mique pourrait ne pas r�duire l�incidence des AVC1 La PA des diab�tiques doit �tre <130/80mmHg2 Les statines, chez les diab�tiques, r�duisent le risque d��v�nements vasculaires majeurs, dont celui d�AVC3 Les hyperglyc�mies � la phase aigu� des AVC sont associ�es � un plus haut taux de mortalit� et � un mauvais pronostic fonctionnel Diab�te 26.01.0826.01.08

79. �tat des connaissances Les statines r�duisent l�incidence des AVC de 2.7 � 3.4%.1 Il n�existe par contre pas d�effet pr�ventif significatif contre les AVC mortels1 La��Heart Protection Study�� a mis en �vidence un taux de myopathie de 1 pour 10.000 patients par an2 Aucune donn�e ne soutient l�utilisation des statines pour les patients avec un LDL-cholest�rol <150 mg/dl (3.9 mmol/l) Hypercholest�rol�mie 26.01.0826.01.08

80. �tat des connaissances Le tabagisme est un facteur de risque ind�pendant d�infarctus c�r�bral chez l�homme et chez la femme Le risque est multipli� d�un facteur 2 � 3 en par rapport aux non fumeurs1 Le tabagisme passif pourrait �tre associ� � une majoration du risque d�AVC2 La r�duction du risque est de 50% deux ans apr�s l�arr�t du tabac3 Tabagisme 26.01.0826.01.08

81. �tat des connaissances Une consommation excessive d�alcool (>60g/jour) est associ� � une augmentation du risque d�infarctus c�r�bral (RR 1.69) et d�HIC (RR 2.18)1 L��l�vation de la PA pourrait en �tre l�explication3 Une consommation l�g�re d�alcool (<12g/jour) est associ�e � une r�duction du risque d�infarctus c�r�bral (RR 0.80) et d�HIC1 Le vin rouge est associ� � un risque plus faible que les autres alcools2 Alcool 26.01.0826.01.08

82. �tat des connaissances La pratique r�guli�re d�exercices (au moins 3x30min/semaine) est associ�e � une diminution du risque d�AVC Les sujets actifs physiquement ont un risque individuel d�AVC ou de mortalit� plus bas que les sujets s�dentaires (RR 0.73)1 Ceci s�explique, partiellement, par des effets b�n�fiques sur le poids, la PA, le taux de cholest�rol et la tol�rance glucidique2 Activit� Physique 26.01.0826.01.08

83. Poids, R�gimes, Nutrition �tat des connaissances Un index de masse corporelle �lev� (BMI =25) majore le risque d�AVC chez l�homme et la femme1 L�adiposit� abdominale est un facteur de risque d�AVC chez l�homme mais pas chez la femme2 Une �tude randomis�e r�alis�e chez des femmes n�a pas pu d�montr� d�impact positif des r�gimes di�t�tiques sur la r�duction de l�incidence des AVC3 Les suppl�ments de tocoph�rol et de b�ta-carot�ne ne r�duisent pas le risque d�AVC. La vitamine E � haute dose (=400 IU/d) pourrait m�me majorer la mortalit� 26.01.0826.01.08

84. �tat des connaissances L�incidence des AVC augmente rapidement chez la femme, apr�s la m�nopause Le traitement hormonal de substitution des femmes m�nopaus�es est associ� � une augmentation du risque d�AVC de 44%1 Traitement Hormonalde Substitution 26.01.0826.01.08

85. �tat des connaissances Chez les sujets � faible risque vasculaire, une petite dose d�aspirine r�duit le nombre d��v�nements coronariens, mais pas le nombre d�AVC1 Chez les femmes de plus de 45 ans, l�aspirine r�duit le risque d�infarctus c�r�bral (OR 0.76; 95%IC 0.63-0.93)2 L�aspirine r�duit le risque d�infarctus du myocarde chez les patients avec une ath�romatose Carotide asymptomatique3 Traitement anti-thrombotique 26.01.08: Six large randomized trials have evaluated the benefits of aspirin for the primary prevention of cardiovascular (CV) events in men and women (47,293 on aspirin, 45,580 controls) with a mean age of 64.4 years {Peto, 1988 #137;Steering Committee of the Physicians' Health Study Research Group, 1989 #162;ETDRS Investigators, 1992 #62;Hansson, 1998 #89;de Gaetano, 2001 #51;Iso, 1999 #845}. Aspirin reduced coronary events and CV events, but not stroke, CV mortality, or all-cause mortality {Bartolucci, 2006 #844}. In women, aspirin reduced stroke (OR 0.83; 95%CI 0.70-0.97) and ischaemic stroke (OR 0.76; 95%CI 0.63-0.93) {Berger, 2006 #843}. In a separate study in 39,876 healthy women aged 45 years or more, aspirin reduced stroke (RR 0.83; 95%CI 0.69-0.99) and ischaemic stroke (RR 0.76; 95%CI 0.63-0.93), and caused a non-significant increase in haemorrhagic stroke, over 10 years; it did not reduce the risk of fatal or nonfatal myocardial infarction, or cardiovascular death {Ridker, 2005 #842}. No data are currently available on the use of other antiplatelet agents in primary prevention in low-risk subjects.26.01.08: Six large randomized trials have evaluated the benefits of aspirin for the primary prevention of cardiovascular (CV) events in men and women (47,293 on aspirin, 45,580 controls) with a mean age of 64.4 years {Peto, 1988 #137;Steering Committee of the Physicians' Health Study Research Group, 1989 #162;ETDRS Investigators, 1992 #62;Hansson, 1998 #89;de Gaetano, 2001 #51;Iso, 1999 #845}. Aspirin reduced coronary events and CV events, but not stroke, CV mortality, or all-cause mortality {Bartolucci, 2006 #844}. In women, aspirin reduced stroke (OR 0.83; 95%CI 0.70-0.97) and ischaemic stroke (OR 0.76; 95%CI 0.63-0.93) {Berger, 2006 #843}. In a separate study in 39,876 healthy women aged 45 years or more, aspirin reduced stroke (RR 0.83; 95%CI 0.69-0.99) and ischaemic stroke (RR 0.76; 95%CI 0.63-0.93), and caused a non-significant increase in haemorrhagic stroke, over 10 years; it did not reduce the risk of fatal or nonfatal myocardial infarction, or cardiovascular death {Ridker, 2005 #842}. No data are currently available on the use of other antiplatelet agents in primary prevention in low-risk subjects.

86. �tat des connaissances La FA entra�ne un risque moyen d�AVC de 5% par an L�aspirine r�duit le risque (RR 0.78) d�infarctus c�r�bral chez les patients avec une FA non valvulaire1 La warfarine (avec un INR entre 2.0 et 3.0) est plus efficace que l�aspirine pour r�duire le risque d�infarctus c�r�bral (RR 0.36; 95%IC 0.26-0.51)1 La combinaison de l�aspirine et du clopidogrel est moins efficace que la warfarine et pr�sente le m�me risque h�morragique2 Fibrillation Auriculaire 26.01.08: AF is a strong independent risk factor for stroke. A meta-analysis of randomized trials with at least 3 months� follow-up showed that antiplatelet agents reduced stroke (RR 0.78; 95%CI 0.65-0.94) in patients with non-valvular AF {Hart, 2007 #841}. Warfarin (target INR 2.0-3.0) is more effective than aspirin at reducing stroke (RR 0.36; 95%CI 0.26-0.51) {Hart, 2007 #841}. As the risk of stroke in people with AF varies considerably, risk stratification should be used to determine whether patients should be given oral anticoagulation, aspirin or nothing {Fuster, 2001 #72}. Oral anticoagulation is more effective in patients with AF who have one or more risk factors, such as previous systemic embolism, age over 75 years, high blood pressure or poor left ventricular function {Fuster, 2001 #72}. In the meta-analysis described above, absolute increases in major extracranial haemorrhage were less than the absolute reductions in stroke {Hart, 2007 #841}. The WASPO {Rash, 2007 #840} and BAFTA {Mant, 2007 #930} trials showed that warfarin was safe and effective in older individuals. The ACTIVE W study found that the combination of aspirin and clopidogrel was less effective than warfarin and had a similar bleeding rate {Connolly, 2006 #839}.26.01.08: AF is a strong independent risk factor for stroke. A meta-analysis of randomized trials with at least 3 months� follow-up showed that antiplatelet agents reduced stroke (RR 0.78; 95%CI 0.65-0.94) in patients with non-valvular AF {Hart, 2007 #841}. Warfarin (target INR 2.0-3.0) is more effective than aspirin at reducing stroke (RR 0.36; 95%CI 0.26-0.51) {Hart, 2007 #841}. As the risk of stroke in people with AF varies considerably, risk stratification should be used to determine whether patients should be given oral anticoagulation, aspirin or nothing {Fuster, 2001 #72}. Oral anticoagulation is more effective in patients with AF who have one or more risk factors, such as previous systemic embolism, age over 75 years, high blood pressure or poor left ventricular function {Fuster, 2001 #72}. In the meta-analysis described above, absolute increases in major extracranial haemorrhage were less than the absolute reductions in stroke {Hart, 2007 #841}. The WASPO {Rash, 2007 #840} and BAFTA {Mant, 2007 #930} trials showed that warfarin was safe and effective in older individuals. The ACTIVE W study found that the combination of aspirin and clopidogrel was less effective than warfarin and had a similar bleeding rate {Connolly, 2006 #839}.

87. �tat des connaissances Une anticoagulation avec un INR inf�rieur � 2.0 n�est pas efficace Le risque de complications h�morragiques augmente avec un INR > 3.5 Les patients de < 65ans avec une ��FA isol�e�� (sans autre facteur de risque) pr�sente un risque faible d�AVC, alors que les patients > 65ans sont � haut risque d�AVC cardio-embolique L�anticoagulation peut �tre s�re et efficace chez certains patients �g�s1, 2 Fibrillation Auriculaire 26.01.0826.01.08

88. Traitement anti-thrombotique Recommandations (1/4) Une faible dose d�aspirine est recommand�e chez les femmes de 45 ans, ou plus, qui ne pr�sentent pas un risque individuel accru d�HIC et qui ont une bonne tol�rance gastro-intestinale; cependant cet effet est tr�s discret (Cat�gorie I, Niveau A) Il est recommand� d�envisager un traitement avec une faible dose d�aspirine, chez les hommes en pr�vention primaire d�infarctus du myocarde; toutefois, le risque d�infarctus c�r�bral n�est pas r�duit (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

89. Traitement anti-thrombotique Recommandations (2/4) Les autres anti-plaquettaires que l�aspirine, ne sont pas recommand�s pour la pr�vention primaire des infarctus c�r�braux (Cat�gorie IV, BPC) L�aspirine peut �tre recommand�e pour les patients pr�sentant une FA non valvulaire, qui ont moins de 65 ans et qui ne pr�sentent aucun facteur de risque vasculaire (Cat�gorie I, Niveau A) En l�absence de contre-indication, l�aspirine ou un traitement anticoagulant oral (ACO) (avec un INR de 2.0-3.0) sont recommand�es pour les patients pr�sentant une FA non valvulaire, qui ont entre 65 et 75 ans et qui ne pr�sentent aucun facteur de risque vasculaire (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

90. Traitement anti-thrombotique Recommandations (3/4) En l�absence de contre-indication, un traitement ACO (avec un INR de 2.0-3.0) est recommand� pour les patients pr�sentant une FA non valvulaire, qui ont plus de 75 ans, ou qui ont moins de 75 ans mais qui pr�sentent des facteurs de risque vasculaire, comme une HTA, une dysfonction ventriculaire gauche, ou un diab�te (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

91. Traitement anti-thrombotique Recommandations (4/4) Il est recommand� de traiter les patients, avec une FA et qui pr�sentent une contre-indication au traitement ACO, par de l�aspirine (Cat�gorie I, Niveau A) Il est recommand� de traiter les patients, avec une FA et une valve cardiaque proth�tique m�canique, par un traitement ACO au long cours, en ciblant un INR variable selon le type de proth�se, mais jamais inf�rieur � 2.0-3.0 (Cat�gorie II, Niveau B) Une faible dose d�aspirine est recommand�e pour les patients porteurs d�une st�nose asymptomatique > 50% de la carotide interne, afin de r�duire le risque d��v�nements vasculaires (Cat�gorie II, Niveau B) 23.01.08 PAR23.01.08 PAR

92. �tat des connaissances1,2 L�int�r�t de l�endart�rectomie Carotide (EAC) reste d�battu en cas de st�nose asymptomatique de l�ACI La r�duction du risque relatif (RRR) pour les st�noses >60%NASCET est de 38-53% La r�duction du risque absolu (RRA) est de 5.9-12.6% Le nombre de patients � traiter (NNT) pour �viter un AVC par an est 63-166 Le risque chirurgical global ne peut pas exc�der 3% St�nose Asymptomatique del�Art�re Carotide Interne (ACI) 26.01.08: Medical management is the most appropriate option for most asymptomatic subjects; only centres with a perioperative complication rate of 3% or less should contemplate surgery. Patients with a high risk of stroke (men with stenosis of more than 80% and a life expectancy of more than 5 years) may derive some benefit from surgery in appropriate centres 26.01.08: Medical management is the most appropriate option for most asymptomatic subjects; only centres with a perioperative complication rate of 3% or less should contemplate surgery. Patients with a high risk of stroke (men with stenosis of more than 80% and a life expectancy of more than 5 years) may derive some benefit from surgery in appropriate centres

93. Donn�es sp�cifiques Aucune �tude prospective n�a �valu� le b�n�fice d�un traitement antiagr�gant chez les patients avec une st�nose asymptomatique de l�ACI1 Le risque d�infarctus c�r�bral ipsilat�ral augmente avec le degr� de st�nose2 Les patients avec une occlusion de l�ACI controlat�rale ne retirent aucun b�n�fice de l�EAC3 Les b�n�fices de l�EAC sont plus faibles chez les femmes que chez les hommes3 L�aspirine r�duit le risque d�infarctus c�r�bral pendant et apr�s une EAC4 St�nose asymptomatique del�Art�re Carotide Interne 26.01.08: Carotid endarterectomy (CEA) is effective in younger patients, and possibly also in older individuals, but does not appear to benefit women {Chambers, 2005 #901}. Patients with occlusion of the internal carotid artery contralateral to the operated carotid artery do not benefit from CEA {Baker, 2000 #12;Straus, 2002 #165}. The risk of ipsilateral stroke increases with the degree of stenosis {The European Carotid Surgery Trialists Collaborative Group, 1995 #63;Baker, 2000 #12}; CEA appears to be effective irrespective of the degree of ipsilateral stenosis over the range of 60-99% {Chambers, 2005 #901}. CEA is not beneficial for asymptomatic patients who have a life expectancy of less than 5 years. Aspirin should not be stopped in patients undergoing carotid surgery {Mayo Asymptomatic Carotid Endarterectomy Study Group, 1992 #953}. Patients should be followed-up by the referring physician after surgery. There are no data from randomized trials about the benefits and risks of carotid angioplasty, compared with CEA, in asymptomatic patients {Derdeyn, 2007 #830}.26.01.08: Carotid endarterectomy (CEA) is effective in younger patients, and possibly also in older individuals, but does not appear to benefit women {Chambers, 2005 #901}. Patients with occlusion of the internal carotid artery contralateral to the operated carotid artery do not benefit from CEA {Baker, 2000 #12;Straus, 2002 #165}. The risk of ipsilateral stroke increases with the degree of stenosis {The European Carotid Surgery Trialists Collaborative Group, 1995 #63;Baker, 2000 #12}; CEA appears to be effective irrespective of the degree of ipsilateral stenosis over the range of 60-99% {Chambers, 2005 #901}. CEA is not beneficial for asymptomatic patients who have a life expectancy of less than 5 years. Aspirin should not be stopped in patients undergoing carotid surgery {Mayo Asymptomatic Carotid Endarterectomy Study Group, 1992 #953}. Patients should be followed-up by the referring physician after surgery. There are no data from randomized trials about the benefits and risks of carotid angioplasty, compared with CEA, in asymptomatic patients {Derdeyn, 2007 #830}.

94. Chirurgie Carotideet Angioplastie Recommandations La chirurgie Carotide n�est pas recommand�e pour les sujets asymptomatiques avec une st�nose Carotide significative (NASCET 60-99%), � l�exception de ceux qui sont � haut risque d�AVC (Cat�gorie I, Niveau C) L�angioplastie Carotide, avec ou sans stenting, n�est pas recommand�e pour les sujets avec une st�nose Carotide asymptomatique (Cat�gorie IV, BPC) Les patients doivent �tre sous aspirine avant et apr�s une AEC (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

95. Pr�vention secondaire

96. Pr�vention Secondaire Contenu Prise en charge des facteurs de risque vasculaire Traitement anti-thrombotique Chirurgie et angioplastie 23.01.08 PAR23.01.08 PAR

97. Contr�le de la Pression Art�rielle �tat des connaissances Les anti-hypertenseurs r�duisent le risque de r�cidive d�AVC apr�s un AVC ou un AIT (RR 0.76; 95%IC 0.63-0.92)1 Les valeurs cibles doivent �tre adapt�es individuellement La r�duction du risque de r�cidive d�AVC est ind�pendante des valeurs initiales de la PA et du type d�AVC2 26.01.08: High blood pressure A meta-analysis of seven randomized controlled trials showed that antihypertensive drugs reduced stroke recurrence after stroke or TIA (RR 0.76; 95%CI 0.63-0.92) {Rashid, 2003 #897}. This analysis included the PATS (indapamide, a diuretic), HOPE (ramipril) and PROGRESS (perindopril, with or without indapamide) studies {Group, 1995 #828;Yusuf, 2000 #201;Bosch, 2002 #827;PROGRESS collaborative group, 2001 #141}. The reduction in stroke occurs regardless of BP and type of stroke {PROGRESS collaborative group, 2001 #141}. BP should be lowered and monitored indefinitely after stroke or TIA. The absolute target BP Niveau and reduction are uncertain and should be individualized, but benefit has been associated with an average reduction of about 10/5 mm Hg, and normal BP levels have been defined as <120/80 mm Hg {Chobanian, 2003 #883}. However, blood pressure should not be lowered intensively in patients with suspected haemodynamic stroke. The angiotensin receptor antagonist eprosartan may be more effective than the calcium channel blocker nitrendipine 26.01.08: High blood pressure A meta-analysis of seven randomized controlled trials showed that antihypertensive drugs reduced stroke recurrence after stroke or TIA (RR 0.76; 95%CI 0.63-0.92) {Rashid, 2003 #897}. This analysis included the PATS (indapamide, a diuretic), HOPE (ramipril) and PROGRESS (perindopril, with or without indapamide) studies {Group, 1995 #828;Yusuf, 2000 #201;Bosch, 2002 #827;PROGRESS collaborative group, 2001 #141}. The reduction in stroke occurs regardless of BP and type of stroke {PROGRESS collaborative group, 2001 #141}. BP should be lowered and monitored indefinitely after stroke or TIA. The absolute target BP Niveau and reduction are uncertain and should be individualized, but benefit has been associated with an average reduction of about 10/5 mm Hg, and normal BP levels have been defined as <120/80 mm Hg {Chobanian, 2003 #883}. However, blood pressure should not be lowered intensively in patients with suspected haemodynamic stroke. The angiotensin receptor antagonist eprosartan may be more effective than the calcium channel blocker nitrendipine

98. �tat des connaissances En cas de diab�te de type 2 et d�ant�c�dent d�AVC, la pioglitazone r�duit le nombre d�AVC fatals et non fatals (HR 0.53; 95%IC 0.34-0.85; P=0.0085)1 En outre, avec ce m�me traitement, on note une tendance en faveur d�une r�duction de la mortalit� ainsi que des autres �v�nements vasculaires majeurs (HR 0.78; 95%IC 0.60-1.02; P=0.067)1 Diab�te 26.01.2008: The prospective, double-blind PROactive trial randomized 5,238 patients with type 2 diabetes and a history of macrovascular disease to pioglitazone or placebo. In patients with previous stroke (n=486 in the pioglitazone group, n=498 in the placebo group), there was a trend towards benefit with pioglitazone for the combined end point of death and major vascular events (HR 0.78; 95%CI 0.60-1.02; P=0.067). In a secondary analysis, pioglitazone reduced fatal or nonfatal stroke (HR 0.53; 95%CI 0.34-0.85; P=0.0085) and cardiovascular death, nonfatal myocardial infarction, or nonfatal stroke (HR 0.72; 95%CI 0.52-1.00; P=0.0467) {Wilcox, 2007 #957}.26.01.2008: The prospective, double-blind PROactive trial randomized 5,238 patients with type 2 diabetes and a history of macrovascular disease to pioglitazone or placebo. In patients with previous stroke (n=486 in the pioglitazone group, n=498 in the placebo group), there was a trend towards benefit with pioglitazone for the combined end point of death and major vascular events (HR 0.78; 95%CI 0.60-1.02; P=0.067). In a secondary analysis, pioglitazone reduced fatal or nonfatal stroke (HR 0.53; 95%CI 0.34-0.85; P=0.0085) and cardiovascular death, nonfatal myocardial infarction, or nonfatal stroke (HR 0.72; 95%CI 0.52-1.00; P=0.0467) {Wilcox, 2007 #957}.

99. �tat des connaissances L�atorvastatine (80mg) r�duit le risque de r�cidive d�AVC de 16%1 La simvastatine (40mg) r�duit le risque d��v�nements vasculaires, en cas d�ant�c�dent d�AVC, ainsi que le risque d�AVC en cas d�ant�c�dent d�autre pathologie vasculaire (RR 0.76)2 La RRA entra�n�e par les statines est basse (NNT 112-143 par ann�e)1 Le retrait des statines au stade aigu d�un infarctus c�r�bral pourrait �tre dangereux3 Hypercholest�rol�mie 26.01.08: In the SPARCL trial, statin therapy with atorvastatin reduced stroke recurrence (HR 0.84; 95%CI 0.71-0.99) {Amarenco, 2006 #824}, while in the Heart Protection Study simvastatin reduced vascular events in patients with prior stroke, and reduced stroke in patients with other vascular disease (RR 0.76) {Heart Protection Study Collaborative Group, 2002 #96}. Neither trial assessed efficacy by stroke subtype, and SPARCL did not include patients with presumed cardioembolic stroke {Heart Protection Study Collaborative Group, 2002 #96;Amarenco, 2006 #824}. The risk of haemorrhagic stroke was slightly increased in both trials {Heart Protection Study Collaborative Group, 2002 #96;Amarenco, 2006 #824}. The absolute risk reduction achieved with statin therapy is low (NNT 112-143 for 1 year). Statin withdrawal at the acute stage of stroke may be associated with an increased risk of death or dependency {Blanco, 2007 #932}.26.01.08: In the SPARCL trial, statin therapy with atorvastatin reduced stroke recurrence (HR 0.84; 95%CI 0.71-0.99) {Amarenco, 2006 #824}, while in the Heart Protection Study simvastatin reduced vascular events in patients with prior stroke, and reduced stroke in patients with other vascular disease (RR 0.76) {Heart Protection Study Collaborative Group, 2002 #96}. Neither trial assessed efficacy by stroke subtype, and SPARCL did not include patients with presumed cardioembolic stroke {Heart Protection Study Collaborative Group, 2002 #96;Amarenco, 2006 #824}. The risk of haemorrhagic stroke was slightly increased in both trials {Heart Protection Study Collaborative Group, 2002 #96;Amarenco, 2006 #824}. The absolute risk reduction achieved with statin therapy is low (NNT 112-143 for 1 year). Statin withdrawal at the acute stage of stroke may be associated with an increased risk of death or dependency {Blanco, 2007 #932}.

100. �tat des connaissances Le b�ta-carot�ne majore le risque (RR 1.10) de mortalit� cardiovasculaire (CV)1 Les anti-oxydants pourraient augmenter la mortalit�2 L�acide folique et les vitamines B12 et B6, administr�es pour diminuer l�homocyst�in�mie, pourraient ne pas r�duire le risque de r�cidive d�AVC et pourrait m�me majorer le nombre d��v�nements vasculaires3 Vitamines 26.01.08: Beta carotene increased the risk (RR 1.10; 95%CI 1.03-1.17) of cardiovascular death in a meta-analysis of primary and secondary prevention trials {Vivekananthan, 2003 #822}. Vitamin E supplementation does not prevent vascular events {Eidelman, 2004 #821}. Antioxidant supplements may increase mortality {Bjelakovic, 2007 #819}. Vitamins which lower homocysteine (folate, B12, B6) do not reduce stroke recurrence and may increase vascular events {Wald, 2002 #818;Toole, 2004 #817;Bonaa, 2006 #816;Bazzano, 2006 #815}. 26.01.08: Beta carotene increased the risk (RR 1.10; 95%CI 1.03-1.17) of cardiovascular death in a meta-analysis of primary and secondary prevention trials {Vivekananthan, 2003 #822}. Vitamin E supplementation does not prevent vascular events {Eidelman, 2004 #821}. Antioxidant supplements may increase mortality {Bjelakovic, 2007 #819}. Vitamins which lower homocysteine (folate, B12, B6) do not reduce stroke recurrence and may increase vascular events {Wald, 2002 #818;Toole, 2004 #817;Bonaa, 2006 #816;Bazzano, 2006 #815}.

101. �tat des connaissances Les traitements � base d��strog�nes ne sont pas efficaces en pr�vention secondaire apr�s un AIT ou un AVC et pourraient augmenter la s�v�rit� de l�AVC en cas de r�cidive1 Traitement Hormonal de Substitution 26.01.08: Hormone replacement therapy does not protect against vascular events and may increase stroke severity {Viscoli, 2001 #188}.26.01.08: Hormone replacement therapy does not protect against vascular events and may increase stroke severity {Viscoli, 2001 #188}.

102. Prise en chargedes Facteurs de Risque Recommandations (1/3) La PA doit �tre contr�l�e r�guli�rement. La r�duction de la PA est recommand�e apr�s la phase aigu�, y compris pour les patients avec une pression art�rielle normale (Cat�gorie I, Niveau A) Les glyc�mies doivent �tre contr�l�es r�guli�rement. Le diab�te doit �tre traiter en adaptant les mesures hygi�no-di�t�tiques et pour certains patients en introduisant un traitement pharmacologique (Cat�gorie IV, BPC) Parmi les patients avec un diab�te de type 2 non insulino-requ�rant, un traitement par pioglitazone est recommand� (Cat�gorie III, Niveau B) 23.01.08 PAR23.01.08 PAR

103. Recommandations (2/3) Les traitements par statines sont recommand�s (Cat�gorie I, Niveau A) Il est recommand� d�encourager l�arr�t du tabac (Cat�gorie III, Niveau C) Il est recommand� d�encourager d��viter toute consommation abusive d�alcool (Cat�gorie IV, BPC) Il est recommand� de pratiquer une activit� physique r�guli�re (Cat�gorie IV, BPC) Il est recommand� de favoriser les r�gimes pauvres en sel et en graisses satur�es, et de favoriser les r�gimes riches en fruits, l�gumes et fibres (Cat�gorie IV, BPC) Prise en chargedes Facteurs de Risque 23.01.08 PAR23.01.08 PAR

104. Recommandations (3/3) Il est recommand� de faire perdre du poids aux sujets avec un BMI �lev� (Cat�gorie IV, Niveau C) Les suppl�ments en vitamines anti-oxydantes ne sont pas recommand�s (Cat�gorie I, Niveau A) Le traitement hormonal de substitution n�est pas recommand� en pr�vention secondaire d�AVC (Cat�gorie I, Niveau A) Il est recommand� de traiter les troubles respiratoires li�s au sommeil, tels que le syndrome obstructif d�apn�es du sommeil, avec une ventilation en pression positive continue (Cat�gorie III, Niveau BPC) Prise en chargedes Facteurs de Risque 23.01.08 PAR23.01.08 PAR

105. Traitement anti-thrombotique �tat des connaissances : Aspirine Permet une RRR d�AVC de 13% apr�s un AVC ou un AIT1 La plupart des essais cliniques ont �valu� des doses entre 50-150mg L�incidence des effets secondaires gastro-intestinaux est dose d�pendant Il n�existe aucune diff�rence d�efficacit� entre les doses faibles (< 160mg), moyennes (160 � 325mg) ou �lev�es (500 - 1500mg) 26.01.08 Antiplatelet therapy reduces vascular events, including non-fatal myocardial infarction, nonfatal stroke and vascular death in patients with previous stroke or TIA (RR 0.78; 95%CI 0.76-0.80) {Antithrombotic Trialists' Collaboration, 2002 #9}. Aspirin Aspirin reduces recurrence independent of dose (50 to 1300 mg/d) {Algra, 1996 #7;The Dutch TIA Trial Study Group, 1991 #171;Farrell, 1991 #68;Campbell, 2007 #808}, although high doses (>150mg/day) increase adverse events. In patients with symptomatic intracranial atherosclerosis, aspirin is as effective as oral anticoagulation and has fewer complications {Chimowitz, 2005 #807}.26.01.08 Antiplatelet therapy reduces vascular events, including non-fatal myocardial infarction, nonfatal stroke and vascular death in patients with previous stroke or TIA (RR 0.78; 95%CI 0.76-0.80) {Antithrombotic Trialists' Collaboration, 2002 #9}. Aspirin Aspirin reduces recurrence independent of dose (50 to 1300 mg/d) {Algra, 1996 #7;The Dutch TIA Trial Study Group, 1991 #171;Farrell, 1991 #68;Campbell, 2007 #808}, although high doses (>150mg/day) increase adverse events. In patients with symptomatic intracranial atherosclerosis, aspirin is as effective as oral anticoagulation and has fewer complications {Chimowitz, 2005 #807}.

106. Traitement anti-thrombotique �tat des connaissances : association dipyridamole plus aspirine La RRR de la mortalit� CV, d�AVC ou d�infarctus du myocarde avec cette association est significativement plus importante qu�avec l�aspirine seule (RR 0.82; 95%IC 0.71-0.91)1,2 La RRA est de 1.0% par an (NNT 100)2 L�incidence des c�phal�es induites par le dipyridamole peut �tre diminu�e en augmentant progressivement la dose3 Dipyridamole alone reduces stroke recurrence with similar efficacy to aspirin {Diener, 1996 #54}. The combination of aspirin (38-300 mg/d) and dipyridamole (200 mg extended release twice daily) reduces the risk of vascular death, stroke or MI, compared with aspirin alone (RR 0.82; 95%CI 0.74-0.91) {Diener, 1996 #54;Halkes, 2006 #810}. Dipyridamole may cause headache; the incidence of this may be reduced by increasing the dose gradually {Chang, 2006 #933;Diener, 2007 #945}.Dipyridamole alone reduces stroke recurrence with similar efficacy to aspirin {Diener, 1996 #54}. The combination of aspirin (38-300 mg/d) and dipyridamole (200 mg extended release twice daily) reduces the risk of vascular death, stroke or MI, compared with aspirin alone (RR 0.82; 95%CI 0.74-0.91) {Diener, 1996 #54;Halkes, 2006 #810}. Dipyridamole may cause headache; the incidence of this may be reduced by increasing the dose gradually {Chang, 2006 #933;Diener, 2007 #945}.

107. Traitement anti-thrombotique Dipyridamole plus aspirine versus aspirine seule : m�ta-analyse1 Diminution du nombre d��v�nements vasculaires (mortalit� CV, AVC, infarctus du myocarde) avec l�association dipyridamole plus aspirine 26.01.0826.01.08

108. Traitement anti-thrombotique �tat des connaissances : clopidogrel Le clopidogrel est discr�tement mais significativement plus efficace qu�une dose moyenne d�aspirine (RRR 8.7%, RAA 0,5%) pour pr�venir des �v�nements vasculaires chez des patients ayant d�j� fait un AVC, un infarctus du myocarde ou ayant une art�riopathie oblit�rante des membres inf�rieurs)1 26.01.08: Clopidogrel is slightly more effective than aspirin in preventing vascular events (RR 0.91; 95%CI 0.84-0.97) {CAPRIE Steering Committee, 1996 #35}. It may be more effective in high-risk patients (i.e. those with previous stroke, peripheral artery disease, symptomatic coronary disease, or diabetes) {Bhatt, 2006 #836}. 26.01.08: Clopidogrel is slightly more effective than aspirin in preventing vascular events (RR 0.91; 95%CI 0.84-0.97) {CAPRIE Steering Committee, 1996 #35}. It may be more effective in high-risk patients (i.e. those with previous stroke, peripheral artery disease, symptomatic coronary disease, or diabetes) {Bhatt, 2006 #836}.

109. Traitement anti-thrombotique �tat des connaissances : clopidogrel plus aspirine En comparaison au clopidogrel seul, l�association du clopidogrel et de l�aspirine ne diminue pas le risque d�infarctus c�r�bral, d�infarctus du myocarde, de mortalit� CV, ou de r�-hospitalisation1 En comparaison � l�aspirine seule, la combinaison ne diminue pas le risque d�infarctus du myocarde, d�AVC ou de mortalit� CV2 En outre, le risque d�h�morragies majeures, parfois fatales, est major�1,2 26.01.08: Compared with clopidogrel alone, the combination of aspirin and clopidogrel did not reduce the risk of ischaemic stroke, myocardial infarction, vascular death, or re-hospitalisation {Diener, 2004 #809}; however, life-threatening or major bleeding were increased with the combination. Similarly, in the CHARISMA study, the combination of aspirin and clopidogrel did not reduce the risk of myocardial infarction, stroke, or death from cardiovascular causes, compared with aspirin alone {Bhatt, 2006 #836}. In patients who have had an acute coronary event within 12 months, or coronary stenting, the combination of clopidogrel and aspirin reduces the risk of new vascular events {Yusuf, 2001 #902}.26.01.08: Compared with clopidogrel alone, the combination of aspirin and clopidogrel did not reduce the risk of ischaemic stroke, myocardial infarction, vascular death, or re-hospitalisation {Diener, 2004 #809}; however, life-threatening or major bleeding were increased with the combination. Similarly, in the CHARISMA study, the combination of aspirin and clopidogrel did not reduce the risk of myocardial infarction, stroke, or death from cardiovascular causes, compared with aspirin alone {Bhatt, 2006 #836}. In patients who have had an acute coronary event within 12 months, or coronary stenting, the combination of clopidogrel and aspirin reduces the risk of new vascular events {Yusuf, 2001 #902}.

110. Traitement anti-thrombotique Recommandations (1/4) Il est recommand� de mettre les patients sous traitement anti-thrombotique (Cat�gorie I, Niveau A) Il est recommand� de mettre les patients, n�ayant pas d�indication pour un traitement anticoagulant, sous traitement anti-plaquettaire (Cat�gorie I, Niveau A) Lorsque c�est possible, l�association d�aspirine et de dipyridamole, ou bien le clopidogrel seul, doivent �tre utilis�s. Comme alternative, l�aspirine seule, ou le triflusal seul, peuvent �tre utilis�s (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

111. Traitement anti-thrombotique Recommandations (2/4) L�association d�aspirine et de clopidogrel n�est pas recommand�e chez les patients avec un infarctus c�r�bral r�cent, � l�exception des patients ayant une indication sp�cifique (tel que de l�angor, un infarctus du myocarde sans onde Q, ou un stenting r�cent); l�association doit alors �tre donn�e durant 9 mois apr�s l��v�nement (Cat�gorie I, Niveau A) Il est recommand� d��valuer � nouveau l��tiologie et les facteurs de risque d�un infarctus c�r�bral des patients qui r�cidivent un infarctus c�r�bral sous traitement anti-plaquettaire (Cat�gorie IV, BPC) 23.01.08 PAR23.01.08 PAR

112. Anticoagulation �tat des connaissances L�anticoagulation orale (ACO) (INR cible de 2.0 � 3.0) r�duit le risque de r�cidive d�AVC en cas de FA1 L�ACO est �galement indiqu�e pour les autres causes emboliques, comme les valves cardiaques m�caniques, les valvulopathies rhumatismales, les an�vrismes ventriculaires et les cardiomyopathies Il n�y a pas d�indication � une ACO pour les patients avec un infarctus c�r�bral d�origine non cardio-embolique2 26.01.08: Oral anticoagulation after non-cardiac ischaemic strokes is not superior to aspirin, but causes more bleeding {Mohr, 2001 #128;The Stroke Prevention in Reversible Ischemia Trial (SPIRIT) Study Group, 1997 #177;Algra, 2007 #903}, Oral anticoagulation (INR 2.0�3.0) reduces the risk of recurrent stroke in patients with non-valvular AF (whether of permanent, chronic or paroxysmal type) {EAFT (European Atrial Fibrillation Trial) Study Group, 1993 #835} and most other cardiac sources of emboli. Anticoagulation should be taken long term, or for at least 3 months after MI {Visser, 1984 #954}. 26.01.08: Oral anticoagulation after non-cardiac ischaemic strokes is not superior to aspirin, but causes more bleeding {Mohr, 2001 #128;The Stroke Prevention in Reversible Ischemia Trial (SPIRIT) Study Group, 1997 #177;Algra, 2007 #903}, Oral anticoagulation (INR 2.0�3.0) reduces the risk of recurrent stroke in patients with non-valvular AF (whether of permanent, chronic or paroxysmal type) {EAFT (European Atrial Fibrillation Trial) Study Group, 1993 #835} and most other cardiac sources of emboli. Anticoagulation should be taken long term, or for at least 3 months after MI {Visser, 1984 #954}.

113. Anticoagulation Donn�es sp�cifiques Chez les patients avec une FA et une maladie coronarienne stable, l�aspirine ne doit pas �tre ajout�e � l�ACO1 Quelques �tudes r�trospectives sugg�rent que l�ACO pourrait �tre b�n�fique dans l�ath�romatose aortique2, dans les an�vrismes fusiformes du tronc basilaire3, ou dans les dissections art�rielles4 Il est par contre moins �vident que l�ACO soit b�n�fique pour les patients avec un foramen ovale perm�able (FOP)5 26.01.08: In patients with AF and stable coronary disease, aspirin should not be added to oral anticoagulation {Flaker, 2006 #955}. Anticoagulation may be beneficial in patients with aortic atheroma {Dressler, 1998 #58}, fusiform aneurysms of the basilar artery {Echiverri, 1989 #61} or cervical dissection {Engelter, 2007 #935}. It is unclear if patients with patent foramen ovale benefit from oral anticoagulation. Patients without proven deep vein thrombosis (DVT) or atrial septal aneurysm should be given aspirin. The roles of anticoagulation and closure of the patent foramen ovale in patients with proven DVT or atrial septal aneurysm remain to be elucidated {Mas, 2001 #124}.26.01.08: In patients with AF and stable coronary disease, aspirin should not be added to oral anticoagulation {Flaker, 2006 #955}. Anticoagulation may be beneficial in patients with aortic atheroma {Dressler, 1998 #58}, fusiform aneurysms of the basilar artery {Echiverri, 1989 #61} or cervical dissection {Engelter, 2007 #935}. It is unclear if patients with patent foramen ovale benefit from oral anticoagulation. Patients without proven deep vein thrombosis (DVT) or atrial septal aneurysm should be given aspirin. The roles of anticoagulation and closure of the patent foramen ovale in patients with proven DVT or atrial septal aneurysm remain to be elucidated {Mas, 2001 #124}.

114. Traitement anti-thrombotique Recommandations (3/4) Il est recommand� de ne pas recourir � une ACO en cas d�infarctus c�r�bral dont l�origine n�est pas cardio-embolique, exception faite de certaines situations sp�cifiques, comme l�ath�romatose aortique, les an�vrismes fusiformes du tronc basilaire, les dissections d�une art�re cervicale, ou les FOP associ�s � la pr�sence av�r�e de thromboses veineuses profondes (TVP) ou d�un ASIA (Cat�gorie IV, BPC) Il est recommand� d�utiliser une association d�aspirine � faible dose avec du dipyridamole lorsque le traitement ACO est contre-indiqu� (Cat�gorie IV, BPC) 23.01.08 PAR23.01.08 PAR

115. Traitement anti-thrombotique Recommandations (4/4) Un traitement ACO (INR 2.0-3.0) est recommand� apr�s un infarctus c�r�bral associ� � une FA (Cat�gorie I, Niveau A). Le traitement ACO n�est pas recommand� pour les patients avec une co-morbidit� importante, comme ceux qui pr�sentent des chutes � r�p�tition, une mauvaise compliance, une �pilepsie mal contr�l�e, ou des h�morragies gastro-intestinales (Cat�gorie III, Niveau C). Un �ge avanc�, en soi, n�est pas une contre-indication � une ACO (Cat�gorie I, Niveau A) Il est recommand� de traiter les patients avec un infarctus c�r�bral d�origine cardio-embolique, mais non li� � une FA, avec des ACO (INR 2.0-3.0) si le risque de r�cidive est �lev� (Cat�gorie III, Niveau C) 23.01.08 PAR23.01.08 PAR

116. Endart�rectomie Carotide �tat des connaissances1,2 L�EAC r�duit le risque de 48% de r�cidive d�AVC avec r�percussion fonctionnelle ou de d�c�s chez les patients avec une st�nose ipsilat�rale de l�ACI de 70-99%NASCET Si le taux de complications p�ri op�ratoires d�passe 6%, l�int�r�t de l�EAC diminue, si ce taux approche les 10%, le b�n�fice dispara�t compl�tement Il existe aussi une diminution du risque chez les hommes porteurs d�une st�nose ipsilat�rale de l�ACI de 50 - 69%, lorsque le taux de complications p�ri op�ratoires est <3% 26.01.08: CEA reduces the risk of recurrent disabling stroke or death (RR 0.52) in patients with severe (70-99% by NASCET criteria) ipsilateral internal carotid artery stenosis {European Carotid Surgery Trialists' Collaborative Group, 1996 #805;North American Symptomatic Carotid Endarterectomy Trial Collaborators, 1991 #804;Cina, 1999 #803}. Patients with less severe ipsilateral carotid stenosis (50-69% by NASCET criteria) may also benefit {Cina, 1999 #803}. Surgery is potentially harmful in patients with mild or moderate degrees of stenosis (<50% by NASCET criteria) {Cina, 1999 #803}. The grading of stenosis should be performed according to NASCET criteria. Although ECST and NASCET use different methods of measurement, it is possible to convert the percentage stenosis derived by one method to the other {Rothwell, 2003 #149}. 26.01.08: CEA reduces the risk of recurrent disabling stroke or death (RR 0.52) in patients with severe (70-99% by NASCET criteria) ipsilateral internal carotid artery stenosis {European Carotid Surgery Trialists' Collaborative Group, 1996 #805;North American Symptomatic Carotid Endarterectomy Trial Collaborators, 1991 #804;Cina, 1999 #803}. Patients with less severe ipsilateral carotid stenosis (50-69% by NASCET criteria) may also benefit {Cina, 1999 #803}. Surgery is potentially harmful in patients with mild or moderate degrees of stenosis (<50% by NASCET criteria) {Cina, 1999 #803}. The grading of stenosis should be performed according to NASCET criteria. Although ECST and NASCET use different methods of measurement, it is possible to convert the percentage stenosis derived by one method to the other {Rothwell, 2003 #149}.

117. Endart�rectomie Carotide Donn�es sp�cifiques L�EAC doit �tre r�alis�e le plus rapidement possible (id�alement dans les deux semaines) apr�s la survenue du dernier �v�nement c�r�brovasculaire1,2 Les patients �g�s (>75 ans), sans insuffisance organique, ni d�compensation cardiaque s�v�re, peuvent �galement b�n�ficier de l�EAC1 Les femmes avec une st�nose symptomatique >70% doivent b�n�ficier d�une EAC. Les femmes avec une st�nose plus mod�r�e doivent �tre trait�es m�dicalement2 26.01.08: CEA should be performed as soon as possible (ideally within 2 weeks) after the last cerebrovascular event {Rothwell, 2004 #802}. Older patients (>75 years) without organ failure or serious cardiac dysfunction benefit from CEA {Rothwell, 2004 #802}. Women with severe (>70%) symptomatic stenosis should undergo CEA, whereas women with more moderate stenosis should be treated medically. Patients with amaurosis fugax, severe stenosis and a high risk profile should be considered for CEA; those with amaurosis fugax and few risk factors do better with medical treatment. Patients with mild-to-moderate intracranial stenosis and severe extracranial stenosis should be considered for CEA. 26.01.08: CEA should be performed as soon as possible (ideally within 2 weeks) after the last cerebrovascular event {Rothwell, 2004 #802}. Older patients (>75 years) without organ failure or serious cardiac dysfunction benefit from CEA {Rothwell, 2004 #802}. Women with severe (>70%) symptomatic stenosis should undergo CEA, whereas women with more moderate stenosis should be treated medically. Patients with amaurosis fugax, severe stenosis and a high risk profile should be considered for CEA; those with amaurosis fugax and few risk factors do better with medical treatment. Patients with mild-to-moderate intracranial stenosis and severe extracranial stenosis should be considered for CEA.

118. Endart�rectomie Carotide Effet du d�lai d�intervention entre le dernier �v�nement symptomatique et la randomisation, sur le RR � 5 ans de survenue d�un infarctus c�r�bral ipsilat�ral et tout AVC p�ri op�ratoire ou tout d�c�s caus� par l�EAC (donn�es combin�es de ECST et de NASCET1) 26.01.08: CEA should be performed as soon as possible (ideally within 2 weeks) after the last cerebrovascular event {Rothwell, 2004 #802}. Older patients (>75 years) without organ failure or serious cardiac dysfunction benefit from CEA {Rothwell, 2004 #802}. Women with severe (>70%) symptomatic stenosis should undergo CEA, whereas women with more moderate stenosis should be treated medically. 26.01.08: CEA should be performed as soon as possible (ideally within 2 weeks) after the last cerebrovascular event {Rothwell, 2004 #802}. Older patients (>75 years) without organ failure or serious cardiac dysfunction benefit from CEA {Rothwell, 2004 #802}. Women with severe (>70%) symptomatic stenosis should undergo CEA, whereas women with more moderate stenosis should be treated medically.

119. M�ta-analyse : ACS Versus EAC Crit�re de jugement : tout AVC p�ri proc�dural ou d�c�s Angioplastie Carotide - Stenting (ACS) 26.01.08: An updated metaanalysis of these studies revealed a significantly higher risk of any stroke and death within 30 days after treatment with CAS, compared with CEA (OR 1.41; 95%CI 1.07-1.87; P=0.016). However, significant heterogeneity was found in this analysis (P=0.035) {Kastrup, 2007 #989}. After the periprocedural period, few ipsilateral strokes occurred after both procedures (Table 9). 26.01.08: An updated metaanalysis of these studies revealed a significantly higher risk of any stroke and death within 30 days after treatment with CAS, compared with CEA (OR 1.41; 95%CI 1.07-1.87; P=0.016). However, significant heterogeneity was found in this analysis (P=0.035) {Kastrup, 2007 #989}. After the periprocedural period, few ipsilateral strokes occurred after both procedures (Table 9).

120. Chirurgie et Angioplastie Recommandations (1/4) L�EAC est recommand�e pour les patients avec une st�nose de 70 � 99% (selon les crit�res de NASCET) (Cat�gorie I, Niveau A). Les EAC doivent �tre r�alis�es seulement dans les centres ayant un taux de complications (AVC et d�c�s) inf�rieur � 6% (Cat�gorie I, Niveau A) Il est recommand� de r�aliser le plus rapidement possible l�EAC apr�s l�infarctus c�r�bral, id�alement dans les deux semaines (Cat�gorie II, Niveau B) 23.01.08 PAR23.01.08 PAR

121. Chirurgie et Angioplastie Recommandations (2/4) Il est recommand� de proposer l�EAC pour certains patients avec une st�nose de 50 � 69%; les hommes avec des sympt�mes h�misph�riques tr�s r�cents pr�sentent probablement un b�n�fice dans cette situation (Cat�gorie III, Niveau C). Les EAC pour les st�noses de 50 � 69% doivent �tre r�alis�es seulement dans les centres ayant un taux de complications (AVC et d�c�s) inf�rieur � 3% (Cat�gorie I, Niveau A) L�EAC n�est pas recommand�e pour les patients avec une st�nose inf�rieure � 50% (Cat�gorie I, Niveau A) 23.01.08 PAR23.01.08 PAR

122. Chirurgie et Angioplastie Recommandations (3/4) Il est recommand� de laisser les patients sous aspirine avant et apr�s toute chirurgie Carotide (Cat�gorie I, Niveau A) Les angioplasties Carotides percutan�es transluminales et/ou les stenting carotidiens sont recommand�s seulement pour certains patients bien pr�cis (Cat�gorie I, Niveau A). Ces proc�dures doivent �tre r�serv�es aux sous-groupes de patients, avec une st�nose Carotide symptomatique s�v�re, suivants : en cas de contre-indication � une EAC, en cas de st�nose situ�e � un endroit chirurgicalement non accessible, en cas de re-st�nose pr�coce apr�s une EAC, en cas de st�nose post-radique (Cat�gorie IV, BPC). 23.01.08 PAR23.01.08 PAR

123. Chirurgie et Angioplastie Recommandations (4/4) Les patients doivent recevoir une association de clopidogrel et d�aspirine juste avant le stenting et au moins encore pendant un mois apr�s la proc�dure (Cat�gorie IV, BPC) Un traitement endovasculaire peut �tre envisag� chez les patients avec une st�nose intracr�nienne symptomatique (Cat�gorie IV, BPC) 23.01.08 PAR23.01.08 PAR

124. Recommendations de l�European Stroke Organisation

Tout sur l AVC en 3 heures

Tout sur l AVC en 3 heures

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