Anticoagulation for Left Ventricle Thrombus—Case Series and Literature Review for Use of Direct Oral Anticoagulants
Abstract
:1. Introduction
2. Case Summary
2.1. Case 1
2.2. Case 2
3. LV Thrombus—An Overview
4. Clinical Experience of Combination of OACs with Antiplatelets
5. DOACs in LV Thrombus—The Clinical Experience
5.1. Case Reports
5.2. Observational Studies and Case Series
5.3. Randomized Controlled Trial Experience
5.4. Meta-Analysis and Systematic Reviews
Author (Year) | Sample Size | Study Drug | End Points | Results | Safety |
---|---|---|---|---|---|
Leow et al. (2018) [37] | 36 | Rivaroxaban (47.2%) Apixaban (25.0%) Dabigatran (27.8%) | Thrombus resolution and time to resolution. | Thrombus resolution was observed in 87.9%, and median duration of treatment to resolution was 30.0 days (IQR = 22.5–47.0). | 1 nonfatal bleeding event (3.0%); no embolic events. |
Kajy et al. (2020) [38] | 41 | Rivaroxaban (51.2%) Apixaban (26.8%) Dabigatran (22%) | Thrombus resolution and time to resolution. | Thrombus resolution—81% (R), 100% (A), and 88.9% (D). Median time of resolution—40 days (R), 36 days (A), and 24 days (D). | One nonfatal bleeding event and one stroke event were reported while on a DOAC. |
Al-abcha et al. (2020) [39] | 857 | VKAs = 480; DOACs = 220 | Primary outcome was thrombus resolution, and the secondary outcomes were major bleeding and stroke or systemic embolism (SSE). | Similar rate of thrombus resolution (odds ratio (OR) 0.97; p = 0.90). | Major bleeding (OR 0.62; p = 0.27) and systemic embolism (OR 1.86; p = 0.05) were not different between groups. |
Chen et al. (2021) [40] | 2467 | Among DOAC users, apixaban (50.0%), rivaroxaban (40.8%), dabigatran (8.8%), and edoxaban (0.4%); among VKA warfarin (98.5%) was predominantly prescribed | Stroke or systemic embolism; thrombus resolution. | For prevention of stroke or systemic embolism (VKA vs. DOAC—RR: 0.96, 95% confidence interval (CI): 0.80–1.16, p = 0.68); for thrombus resolution (VKA vs. NOAC—RR: 0.88, 95% CI: 0.72–1.09, p = 0.26); for risk of stroke (VKA vs. DOAC—RR: 0.68, 95% CI: 0.47–1.00, p = 0.048). | For risk of any bleeding; no difference between VKAs and DOACs (RR: 0.94, 95% CI: 0.67–1.31, p = 0.70); for clinically relevant bleedings—lower risk with DOAC users (RR: 0.35, 95% CI: 0.13–0.92, p = 0.03) compared with VKA users. |
Burmister et al. (2021) [41] | 2153 | 570 on DOACs vs. 1583 on VKAs) | LV thrombus resolution, thromboembolic events, and thromboembolic stroke. | Thrombus resolution was significantly higher in DOACs compared with VKAs (RR: 1.18 (95% CI: 1.04–1.35); p = 0.01, I2 = 25%); no significant difference existed between DOACs and VKAs regarding overall thromboembolic events (RR: 1.10 (95% CI: 0.75–1.62); p = 0.61) or embolic strokes (RR: 0.63 (95% CI: 0.39–1.02); p = 0.06). | No difference in all-cause death (RR-0.84, p = 0.53) or bleeding (RR-1.00, p = 0.9). |
Trongtorsak (2021) [42] | 1771 | DOACs—426 and VKAs—1345 | Stroke, systemic embolism. Thrombus resolution, bleeding. | No significant differences in rates of systemic embolism or LV thrombus resolution. | Bleeding similar between two groups. |
Shah et al. (2021) [43] | 867 | Systemic embolism and LV thrombus resolution. | Systemic embolic events (SEE)—2.7%; thrombus—86.6%. | Bleeding (composite of major and minor) and major bleeding—5.6% and 1.1%, respectively. | |
Abdelaziz et al. (2021) [44] | 700 | VKAs = 480; DOACs = 220. | Stroke or systemic embolism (SSE). Secondary outcomes were thrombus resolution, bleeding, and death. | For stroke or systemic embolism (SSE), lower rates with VKAs compared with DOACs (5.2% vs. 9%; OR = 0.54, p = 0.05). | Rates of thrombus resolution (OR = 1.00, p = 0.99) and bleeding (OR = 1.62, p = 0.27) and death (OR = 1.09, p = 0.79) were similar. |
Tetsuji Ketano et al. (2021) [47] | 2612 | VKAs = 2004; DOACs = 608 | Thrombus resolution, stroke, any thromboembolism, and major bleeding. | No difference in thrombus resolution (0.75 for VKAs vs. 0.75 for DOACs), stroke (0.06 for VKAs vs. 0.02 for DOACs), or any embolism (0.08 for VKAs vs. 0.03 for DOACs). | OR for major bleeding -0.06 & 0.03 for VKAs DOAC respectively. |
Saleh et al. (2021) [45] | 2395 | Primary—thrombus resolution; secondary—occurrence of major bleeding and stroke or systemic embolization (SSE). | The rates of thrombus resolution for VKAs and DOACs were equal (71.9% vs. 71.4%; p = 0.36). Systemic embolism was also similar between arms (21.3% and 15.6%, respectively; p = 0.57). | Major bleeding rates were similar between DOACs and VKAs. (8.2% vs. 7.1%, p = 0.57, OR = 0.87). | |
Shu Fang et al. (2022) [46] | 2262 | VKAs = 1575; NOACs = 570 | Thrombus resolution, stroke/SSE, bleeding, and mortality. | The rate for SSE (OR 1.01, p = 0.95) and that for thrombus resolution (OR = 1.15) were similar. | Similar bleeding risk(OR = 0.78). |
H. da Silva Ferraira (2022) [48] | 2432 | DOACs = 618; NOACs = 1814 | Stroke/SSE and bleeding events. | DOACs vs. VKAs (OR = 0.86). | 8.7% for DOACs vs. 8.3% for VKAs. |
5.5. Use of Anticoagulation for Prevention of LV Thrombus Formation
5.6. A Note of Dissent
6. Future Directions
7. Choice for Anticoagulation—Practical Considerations and Guidelines
7.1. Utilizing Risk Scores for Decision-Making
7.2. Suggested Algorithm
7.3. Guideline Track
8. Conclusions
Funding
Conflicts of Interest
References
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Trial | Year | Drugs Compared | Number | Follow-Up | Primary End Points |
---|---|---|---|---|---|
WOEST | 2013 | VKA + C, VKA + DAPT | 563 | 12 months | Total number of TIMI bleeding events |
ISAR-TRIPLE | 2015 | VKA + A, VKA + DAPT | 614 | 9 months | Composite of death, MI, definite stent thrombosis, stroke, and TIMI major bleeding |
PIONEER- AF PCI | 2016 | Rivaroxaban (2.5/5) + C, VKA + DAPT | 1415 | 12 months | A composite of major bleeding or minor bleeding event according to the TIMI or bleeding requiring medical attention. |
REDUAL PCI | 2017 | Dabigatran (110/150) + C, VKA + DAPT | 2725 | 24 months | A composite of major or clinically relevant nonmajor bleeding event according to ISTH |
AUGUSTUS PCI | 2019 | VKA + C, Apixaban + C, VKA + DAPT | 4614 | 6 months | A composite of major or clinically relevant nonmajor bleeding event according to ISTH |
ENTRUST AF PCI | 2019 | Edoxaban + C, VKA + DAPT | 1506 | 12 months | Major or clinically relevant nonmajor bleeding event according to ISTH |
Study | Number of Patients | Anticoagulant Profile | End Points | Follow-Up | Outcome |
---|---|---|---|---|---|
Robinson et al. (2018) [27] | 84 | No OAC: 16 patients Warfarin: 40 patients NOACs: 35 patients Other OACs: 7 patients | Survival free of stroke and systemic embolism | 1 year | No difference 88% vs. 77.9%, p = 0.719. |
Jaidka et al. (2018) [28] | 49 | Warfarin: 37 patients NOACS: 12 patients | Thrombus resolution, embolic events, bleeding events | 6 months | No difference in bleeding or embolic events. Thrombus resolution also not different between VKAs and NOACs (69.2% vs. 88.9%; p = 0.245). |
Fleddermann et al. (2019) [29] | 52 | Only NOAC—apixaban = 26 Rivaroxaban = 24 Dabigatran = 2 | Rate of LV thrombus resolution; bleeding | 264 days | 83% had resolution of LV thrombus on follow-up echocardiogram. 1 cardioembolic event and 4 bleeding events requiring transfusion. |
Daher et al. (2020) [30] | 59 | Warfarin: 42 patients NOACS: 17 patients | Rate of LV thrombus resolution | 3 months | Thrombus resolution was similar in patients on NOACs (70.6%) and those on VKAs (71.4%; p = 0.9). |
Jones et al. (2020) [31] | 101 | Warfarin: 60 patients NOACS: 41 patients | Primary—rate of LV thrombus resolution; secondary—rate of bleeding | 2.2 years | Thrombus resolution earlier and greater with NOACs (82% vs. 64.4%, p = 0.0018). Bleeding rates lower with NOACs (0% vs. 6.7%, p = 0.030). No difference in rates of systemic thromboembolism (5% vs. 2.4%, p = 0.388). |
Guddeti et al. (2020) [32] | 99 | Warfarin: 80 patients NOACS: 19 patients | Occurrence of ischemic stroke, bleeding, and thrombus resolution | 1 year | No difference between stroke within 1 year or bleeding between two groups (numerically higher event in warfarin group); thrombus resolution was similar between groups (80% vs. 81%, p = 0.9). |
Alcalai et al. (2020) [33] | 25 | Warfarin: 12 patients Apixaban: 13 patients | Primary end point: thrombus resolution Secondary end point: systemic embolism, major bleeding, and death from any cause | 3 months | Complete thrombus resolution in all patients with warfarin and 12 out of 13 patients in apixaban group. 2 major bleeding events in warfarin group and none in apixaban group. |
Robinson et al. (2020) [34] | 514 | Warfarin: 300 patients NOACs (apixaban in majority): 185 patients No OAC: 93 patients 64 switched regimens | Stroke and systemic embolism (SSE) | ~1 year (351 days) | NOAC use associated with higher SSE risk compared with VKA use (HR—2.64–2.71); prior stroke or embolism also associated with higher SSE risk. |
Albabtain et al. (2021) [35] | 63 | Warfarin: 35 patients NOAC (rivaroxaban): 28 patients | Time to thrombus resolution, bleeding, stroke, and mortality | 9.5 months | Median time to thrombus resolution faster with NOACs (9 months vs. 3 months, p = 0.019); no difference in embolism, bleeding, or mortality. |
Methods |
---|
Use of lower doses of aspirin |
Proton pump inhibitor use |
Avoid potent P2Y12 inhibitor—ticagrelor and prasugrel |
Shorten the duration of DAPT |
De-escalation of DAPT |
Radial access in case of PCI |
Sparing use of glycoprotein IIb/IIIa |
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Pradhan, A.; Bhandari, M.; Vishwakarma, P.; Salimei, C.; Iellamo, F.; Sethi, R.; Perrone, M.A. Anticoagulation for Left Ventricle Thrombus—Case Series and Literature Review for Use of Direct Oral Anticoagulants. J. Cardiovasc. Dev. Dis. 2023, 10, 41. https://doi.org/10.3390/jcdd10020041
Pradhan A, Bhandari M, Vishwakarma P, Salimei C, Iellamo F, Sethi R, Perrone MA. Anticoagulation for Left Ventricle Thrombus—Case Series and Literature Review for Use of Direct Oral Anticoagulants. Journal of Cardiovascular Development and Disease. 2023; 10(2):41. https://doi.org/10.3390/jcdd10020041
Chicago/Turabian StylePradhan, Akshyaya, Monika Bhandari, Pravesh Vishwakarma, Chiara Salimei, Ferdinando Iellamo, Rishi Sethi, and Marco Alfonso Perrone. 2023. "Anticoagulation for Left Ventricle Thrombus—Case Series and Literature Review for Use of Direct Oral Anticoagulants" Journal of Cardiovascular Development and Disease 10, no. 2: 41. https://doi.org/10.3390/jcdd10020041
APA StylePradhan, A., Bhandari, M., Vishwakarma, P., Salimei, C., Iellamo, F., Sethi, R., & Perrone, M. A. (2023). Anticoagulation for Left Ventricle Thrombus—Case Series and Literature Review for Use of Direct Oral Anticoagulants. Journal of Cardiovascular Development and Disease, 10(2), 41. https://doi.org/10.3390/jcdd10020041