4.6 Article

New evidence of direct oral anticoagulation therapy on cardiac valve calcifications, renal preservation and inflammatory modulation

Journal

INTERNATIONAL JOURNAL OF CARDIOLOGY
Volume 345, Issue -, Pages 90-97

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.ijcard.2021.10.025

Keywords

Atrial fibrillation; Cytokine; Rivaroxaban; Warfarin; Calcification; Inflammation

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This study compared the effects of Rivaroxaban and Warfarin on atrial fibrillation patients with chronic kidney disease, finding that long-term use of Rivaroxaban significantly reduced cytokine levels, promoted stability or regression of valve calcification, improved kidney function, and reduced adverse events compared to Warfarin treatment. These results suggest that Rivaroxaban may have anti-inflammatory effects and could contribute to reducing the risk of cardiac valve calcification progression and worsening of renal function.
Background: Rivaroxaban is a direct inhibitor of activated Factor X (FXa), an anti-inflammatory protein exerting a protective effect on the cardiac valve and vascular endothelium. We compare the effect of Warfarin and Rivaroxaban on inflammation biomarkers and their contribution to heart valve calcification progression and renal preservation in a population of atrial fibrillation (AF) patients with chronic kidney disease (CKD) stage 3b - 4. Methods: This was an observational, multicenter, prospective study enrolling 347 consecutive CKD stage 3b - 4 patients newly diagnosed with AF: 247 were treated with Rivaroxaban and 100 with Warfarin. Every 12 months, we measured creatinine levels and cardiac valve calcification via standard trans-thoracic echocardiogram, while plasma levels of inflammatory mediators were quantified by ELISA at baseline and after 24 months. Results: Over a follow-up of 24 months, long-term treatment with Rivaroxaban was associated with a significative reduction of cytokines. Patients treated with Rivaroxaban experienced a more frequent stabilization/regression of valve calcifications comparing with patients treated with Warfarin. Rivaroxaban use was related with an improvement in kidney function in 87.4% of patients, while in those treated with Warfarin was reported a worsening of renal clearance in 98% of cases. Patients taking Rivaroxaban experienced lower adverse events (3.2% vs 49%, p-value <0.001). Conclusions: Our findings suggest that Rivaroxaban compared to Warfarin is associated with lower levels of serum markers of inflammation. The inhibition of FXa may exert an anti-inflammatory effect contributing to reduce the risk of cardiac valve calcification progression and worsening of renal function.

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