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Impact of a factor Xa inhibitor (apixaban) on SIV pathogenesis and response to antiretroviral therapy
Cuiling Xu, Haritha Annapureddy, Lilly Carson, Vansh Khurana, Ranjit Sivanandham, Sindhuja Sivanandham, Tianyu He, Kevin D. Raehtz, Janet Kim, Christie Biber, Norma Arbujas-Silva, Mohammed Daira, Sudhapriya Kandasamy, Matthew J. Feinstein, Irini Sereti, Cristian Apetrei, Ivona Pandrea
Cuiling Xu, Haritha Annapureddy, Lilly Carson, Vansh Khurana, Ranjit Sivanandham, Sindhuja Sivanandham, Tianyu He, Kevin D. Raehtz, Janet Kim, Christie Biber, Norma Arbujas-Silva, Mohammed Daira, Sudhapriya Kandasamy, Matthew J. Feinstein, Irini Sereti, Cristian Apetrei, Ivona Pandrea
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Research Article AIDS/HIV Infectious disease Virology

Impact of a factor Xa inhibitor (apixaban) on SIV pathogenesis and response to antiretroviral therapy

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Abstract

Antiretroviral therapy (ART) has prolonged the life expectancy of persons living with HIV, the majority of whom are now older than 50 years. Aging people with HIV are at increased risk for cardiovascular events driven by HIV-related inflammation and hypercoagulation. Apixaban is a factor Xa inhibitor that reduces cardiovascular risks and treats stroke, deep vein thrombosis, and pulmonary embolism. We assessed apixaban’s impact on key parameters of HIV/SIV pathogenesis in SIV-infected, aged rhesus macaques (RMs) receiving ART. Inflammation, coagulation, T cell subsets, B cells, and macrophages and their immune activation status were monitored throughout the study. We found no significant differences between the apixaban-treated and control groups for virus replication or CD4+ T cell recovery in blood and tissues after ART. Apixaban did not significantly affect D-dimer, immune activation, or inflammation of SIV-infected, ART-treated RMs. Apixaban-treated RMs experienced multiple bleeding episodes, tissue hemorrhages, and myocardial infarctions, as demonstrated by pathological examination of necropsy-collected tissues. Given apixaban’s lack of effect on immune activation, CD4+ T cell restoration, and inflammation, along with increased risk of hemorrhage, factor Xa inhibition may not be an efficient or safe option to target and prevent cardiovascular events in aging people with HIV.

Authors

Cuiling Xu, Haritha Annapureddy, Lilly Carson, Vansh Khurana, Ranjit Sivanandham, Sindhuja Sivanandham, Tianyu He, Kevin D. Raehtz, Janet Kim, Christie Biber, Norma Arbujas-Silva, Mohammed Daira, Sudhapriya Kandasamy, Matthew J. Feinstein, Irini Sereti, Cristian Apetrei, Ivona Pandrea

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Figure 2

Pathological findings in apixaban-treated rhesus macaques.

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Pathological findings in apixaban-treated rhesus macaques.
One RM experi...
One RM experienced an aortic dissection characterized by the tearing of the aorta intima and the dissection of the blood underneath intima. Dissection occurred at a site of an atherosclerotic plaque (A). Several RMs had uncomplicated atherosclerotic plaques located in the abdominal aorta (B). One RM experienced a recent myocardial infarction, as shown by the increased number of immune cells infiltrating the area with necrotic myocardial fibers (C) and the hypertrophic myocardial fibers (large, irregular nuclei) in an attempt to compensate for the loss of necrotic myocardial fibers at the periphery at the infarction area (D). Old myocardial scars were present in several RMs and were characterized by more mature collagen tissue and a paucity of immune cells (E). Small hemorrhages were present in the adipose tissue of the epicardium (F) and in the lung (G). A detailed image (F) shows erythrocytes in the alveolar lumen. Scale bars: 500 μm (A and B), 100 μm (C–G), 50 μm (H). Magnifications: 4× (A and B); 10× (C, E, and G); 20× (D and F); 40× (H).

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