Secondary Prevention Strategies for Ischemic Stroke in Antiphospholipid Syndrome
Abstract
1. Introduction
2. Methods
2.1. Search Strategy
2.2. Data Extraction and Quality Assessment
3. Results
3.1. Direct Oral Anticoagulants (DOACS) vs. Vitamin K Antagonists (VKAS)
3.1.1. Thrombosis and Bleeding Occurrence
3.1.2. INR Levels Target
3.1.3. Guidelines
3.2. Antiplatelet Therapy
3.2.1. Thrombosis and Bleeding Occurrence
3.2.2. Guidelines
3.3. Statin Therapy
3.4. Patent Foramen Ovale (PFO) Closure
Guidelines
3.5. Lifestyle Modifications
3.6. Risk Stratification
Guidelines
4. Discussion
Future Directions
5. Conclusions
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
References
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| Study | Drug (DOAC) | Population and N | Follow-Up | Thrombosis Recurrence | Major Bleeding |
|---|---|---|---|---|---|
| Moore et al. (RAPS), 2016 [10] | Rivaroxaban | VTE-APS, n = 116 | 210 days | 0% both | 0% both |
| Pengo et al., TRAPS, 2018 [11] | Rivaroxaban (20/15 mg) | Triple-positive APS, n = 120 | 569 days | 19% vs. 3% (HR ≈ 6.7; increase risk in rivaroxaban patients for arterial strokes/MI) | 7% vs. 3% |
| Ordi-Ros et al., 2019 [14] | Rivaroxaban (20/15 mg) | APS, n = 190 | 3 years | 11.6% vs. 6.3% (RR ≈ 1.83; strokes only DOAC) | 6.3% vs. 7.4% |
| Woller et al., ASTRO-APS, 2021 [12] | Apixaban (2.5 or mg BID) | APS, n = 48 | 12 months | 6 events vs. 0 | 0 vs. 1 |
| Study and Design | Therapy | Population | Follow-Up | Thrombosis Recurrence | Major Bleeding |
|---|---|---|---|---|---|
| Okuma et al., 2009: Double-blind RCT [22] | Aspirin 100 mg vs. Aspirin + Warfarin (INR 2.0–3.0) | APS with prior stroke (n = 20) | 3.9 years | Higher recurrence in aspirin-only group | Similar between groups |
| Jackson et al., 2017: Retrospective cohort [23] | SAPT vs. VKA vs. VKA + ASP | APS with arterial thrombosis (n = 139) | 4.24 years | 37.2% (SAPT) vs. 23.7% (VKA) vs. 6.9% (Combo) | Not reported |
| Ohnishi et al., 2019: Retrospective cohort [24] | SAPT, DAPT, VKA (1.5–2.5), VKA + SAPT | APS with arterial thrombosis (n = 90) | 8 years | 1.8 (DAPT), 3.7 (Combo), 5.5 (SAPT), 11.6 (VKA)/100 PY | No significant difference |
| Yang et al., 2025: Retrospective cohort [25] | SAPT, DAPT, Warfarin, DOAC | aPL or APS with prior ischemic stroke or TIA (n = 167) | 2.5 years in all groups except the DOAC group (0.5 year) | Composite outcome HR 0.24 (SAPT), HR 0.25 (DAPT) vs. Warfarin | |
| Attachaipanich et al., 2023: Network meta-analysis [26] | SAPT, DAPT, VKA, VKA + SAPT, DOAC | APS with arterial thrombosis (13 studies, n = 719) | Varies | RR 0.41 (VKA + SAPT), RR 0.29 (DAPT) vs. SAPT | No significant difference |
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Naftali, J.; Finkelshtain, S.; Auriel, E. Secondary Prevention Strategies for Ischemic Stroke in Antiphospholipid Syndrome. J. Clin. Med. 2025, 14, 8026. https://doi.org/10.3390/jcm14228026
Naftali J, Finkelshtain S, Auriel E. Secondary Prevention Strategies for Ischemic Stroke in Antiphospholipid Syndrome. Journal of Clinical Medicine. 2025; 14(22):8026. https://doi.org/10.3390/jcm14228026
Chicago/Turabian StyleNaftali, Jonathan, Sheree Finkelshtain, and Eitan Auriel. 2025. "Secondary Prevention Strategies for Ischemic Stroke in Antiphospholipid Syndrome" Journal of Clinical Medicine 14, no. 22: 8026. https://doi.org/10.3390/jcm14228026
APA StyleNaftali, J., Finkelshtain, S., & Auriel, E. (2025). Secondary Prevention Strategies for Ischemic Stroke in Antiphospholipid Syndrome. Journal of Clinical Medicine, 14(22), 8026. https://doi.org/10.3390/jcm14228026

