| Literature DB >> 30174820 |
Carlos Estevez-Fraga1, Maria Molina-Sanchez2, Rodrigo Alvarez-Velasco1, Pablo Agüero-Rabes3, Leticia Crespo-Araico4, Elena Viedma-Guiard5, Antonio Cruz-Culebras1, Consuelo Matute1, Rocio Vera1, Alicia De Felipe-Mimbrera1, Jaime Masjuan Vallejo1.
Abstract
INTRODUCTION: Patients treated with vitamin K antagonists (VKA) are at increased risk of intracranial haemorrhage (ICH). The purpose of our study was to determine the quality of previous anticoagulation control in patients with VKA-associated ICH.Entities:
Year: 2018 PMID: 30174820 PMCID: PMC6098890 DOI: 10.1155/2018/5613103
Source DB: PubMed Journal: Stroke Res Treat
Baseline characteristics.
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|---|---|
| Age, median (range) years | 79 (56-93) |
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| Sex (female) | 26 (42%) |
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| (i) 0-3 | 41 (91%) |
| (ii) 4-5 | 4 (9%) |
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| Arterial hypertension N (%) | 4 (9%) |
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| Diabetes mellitus N (%) | 13 (25%) |
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| Dyslipidemia N (%) | 23 (43%) |
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| (i) TIA N (%) | 7 (13.21%) |
| (ii) Ischaemic N (%) | 2 (5%) |
| (iii) Haemorrhagic N (%) | 3 (6.5%) |
| (iv) Both N (%) | 2 (5%) |
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| HASBLED median (p25-p75) | 2.5 (2-3) |
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| CHAD2S2-VASc median (p25-p75) | 4 (3-5) |
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| (i) Atrial fibrillation N (%) | 48 (90.6%) |
| (ii) Mechanical heart valves N (%) | 5 (9.4%) |
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| (i) Antiplatelet agents N (%) | 3 (6.5%) |
| (ii) Statins N (%) | 19 (43.2%) |
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| Leukoaraiosis N (%) | 24 (47%) |
TIA: transient ischaemic attack. VKA: vitamin K antagonist.
Characteristics of ICH.
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|---|---|
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| 7 (1-38) |
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| 160 (110-242) |
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| 81.5 (40-146) |
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| 79 (41-150) |
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| 137 (76-280) |
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| 23.7 (mean=15) |
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| 13 (0-42) |
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| 16 (0-42) |
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| 2 (0-16) |
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| (i) None | 51 (96%) |
| (ii) Cavernoma N (%) | 2 (4%) |
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| 27 (51%) |
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| 29 (64.4%) |
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| 20 (38.4%) |
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| 2 (4%) |
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| 27 (61.4%) |
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| 22 (50%) |
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| 13 (59%) |
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| 11 (25%) |
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| (i) 0-3 | 13 (29%) |
| (ii) 4-6 | 40 (71%) |
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| (i) Deep | 20 (38%) |
| (ii) Lobar | 15 (29%) |
| (iii) Intraparenchymal extensive | 9 (17%) |
| (iv) Intraventricular | 1 (2%) |
| (v) Brainstem | 6 (11.5%) |
| (vi) Cerebellum | 2 (4%) |
ICH: intracranial haemorrhage. SBP: systolic blood pressure. DBP: diastolic blood pressure. HR: heart rate. NIHSS: National Institutes of Health Stroke Scale. mRS: Modified Rankin Scale. Values are shown as median (range) unless otherwise specified.
Treatment.
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|---|---|
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| (i) None | 16 (30.8%) |
| (ii) Vitamin K | 6 (11.5%) |
| (iii) Prothrombin | 0 (0%) |
| (iv) Prothrombin and vitamin K | 26 (50%) |
| (v) Surgical | 4 (7.7%) |
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| (i) None | 10 (41.6%) |
| (ii) Antiplatelet agents | 3 (12.5%) |
| (iii) VKAs | 2 (8.3%) |
| (iv) VKAs and antiplatelet agents | 0 (0%) |
| (v) Dabigatran | 2 (8.3%) |
| (vi) Rivaroxaban | 0 (0%) |
| (vii) Apixaban | 0 (0%) |
| (viii) NOAC and aspirin | 0 (0%) |
| (ix) LAA closure | 5 (20.8) |
| (x) Prophylactic heparin | |
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| (i) None | 0 (0%) |
| (ii) Antiplatelet agents | 2 (9.1%) |
| (iii) VKAs | 2 (9.1%) |
| (iv) VKAs and antiplatelet agents | 0 (0%) |
| (v) Dabigatran | 4 (18.2%) |
| (vi) Rivaroxaban | 7 (31.8 %) |
| (vii) Apixaban | 2 (9.1%) |
| (viii) NOAC and aspirin | 0 (0%) |
| (ix) LAA closure | 3 (13.6%) |
| (x) Prophylactic heparin | 1 (4.5%) |
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| 15/22 |
VKA: Vitamin K antagonist. NOAC: novel oral anticoagulant. LAA: left atrial appendage.
Differences between patients who died and survivors.
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|---|---|---|---|
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| 78 | 80 | n.s. |
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| 170 | 156 | n.s. |
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| 89 | 81 | n.s. |
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| 83 | 79 | n.s. |
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| 160 | 132 | n.s. |
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| 2.8 | 2.4 | n.s. |
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| 3.5 | 4.23 | n.s. |
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| 25 | 6.1 | p<0.05 |
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| 39% | 47% | n.s. |
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| 56% | 33% | n.s. |
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| (i) Deep | 18.5% | 41.6% | n.s. |
| (ii) Lobar | 29.6% | 45.8% | n.s. |
| (iii) Intraparenchymal extensive | 14.8% | 8.3% | n.s. |
| (iv) Intraventricular | 33.3% | 0 | n.s. |
| (v) Brainstem | 0 % | 8.3% | n.s. |
| (vi) Cerebellum | 3.7% | 0 % | n.s. |
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| 33.9 | 12.5 | p<0.05 |
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| 3.3 | 2.5 | p<0.05 |
n.s.: not statistically significant differences. SBP: systolic blood pressure. DBP: diastolic blood pressure. HR: heart rate. VKA: vitamin K antagonist. NIHSS: National Institutes of Health Stroke Scale.