Experts tackle major cardiovascular issues in treating patients with HIV

Now that people infected with HIV are living longer due to effective therapies, it is imperative to understand why their risks from cardiovascular disease are about 50 percent higher than the general population, according to the Canadian Journal of Cardiology


Philadelphia, March 4, 2019

Since the advent of effective antiretroviral therapy (ART), human immunodeficiency virus (HIV) infection has become more like a chronic illness. Now that patients are able to live longer and remain free of developing AIDS, they have begun to encounter new risks from age-related disorders common in the general population, including cardiovascular disease (CVD).

Who is best suited to treat these patients is not clear, since HIV specialists may not have the expertise to manage CVD, and cardiologists may lack adequate training in understanding HIV-related disease processes or treatments. To address these gaps in clinical care, the latest issue of the Canadian Journal of Cardiology presents up-to-date guidance for cardiologists and other clinicians who treat this growing and challenging patient population.

“Survivors of the AIDS epidemic face a variety of new threats to their health, including an increased risk of diabetes, chronic kidney disease, cancer, bone diseases, neurocognitive disorders, and CVD, due to the cumulative effects of exposure to HIV, prolonged immune suppression, chronic inflammation, and the adverse effects of ART,” explains David D. Waters, MD, Division of Cardiology at Zuckerberg San Francisco General Hospital and the Department of Medicine of the University of California, San Francisco, CA, USA.

According to the Centers for Disease Control and Prevention, an estimated 1,122,900 adults and adolescents were living with HIV in the United States by the end of 2015. Of those, 162,500 (15 percent) had not received a diagnosis. Worldwide, an estimated 35 million people have HIV. Although deaths from AIDS-related illnesses have declined dramatically since the 1990s, deaths from CVD in people with HIV have more than doubled over the past two decades. Studies have shown a two-fold greater risk of myocardial infarction (MI) for persons with HIV even after adjusting for CVD risk factors. As more HIV patients age, cardiologists’ services will be in even greater demand.

Cardiologist Priscilla Y. Hsue, MD, University of California, San Francisco (UCSF), Zuckerberg San Francisco Hospital, San Francisco, CA, USA, discusses mechanisms of cardiovascular disease in the setting of HIV infection. According to Dr. Hsue, the types of CVD occurring in HIV have shifted over the years from pericardial effusion and dilated cardiomyopathy to conditions such as atherosclerosis, arrhythmic complications, and heart failure. Factors that contribute to the pathogenesis of CVD in HIV include a preponderance of traditional risk factors (such as hypertension, lipid abnormalities, cigarette smoking, metabolic syndrome, diabetes, and chronic kidney disease), leaky gut and microbial translocation, T-cell activation and cytomegalovirus coinfection, chronic inflammation, platelet abnormalities, and side effects from antiretroviral therapy.

Even in the setting of effectively treated HIV infection, HIV-associated factors are strong contributors to CVD; for example, an association exists between chronic inflammation and CVD in both HIV and non-HIV patients. Dr. Hsue discusses evidence regarding the effectiveness of anti-inflammatory medications in reducing CVD events. She also makes the important point that persons living with HIV represent a unique model of chronic inflammation and thus, “findings gleaned from studies in HIV patients can help to identify anti-atherosclerotic targets that may benefit broader populations.”

Dr. Hsue believes that the cellular mechanisms that underlie “ordinary” atherosclerosis may be amplified in HIV patients. “On a molecular level, monocytes/macrophages, platelet reactivity, and immune cell activation may be heightened in the setting of HIV and contribute to HIV-associated atherosclerosis.” She also cites evidence that HIV-related atherosclerosis is structurally distinct from atherosclerosis in non-HIV individuals.

Infographic showing the various mechanisms leading to atherosclerotic cardiovascular disease with human immunodeficiency virus (HIV) infection.
Mechanisms leading to atherosclerotic cardiovascular disease with human immunodeficiency virus (HIV) infection. This schematic figure illustrates the multiple and complex mechanisms leading to HIV-associated atherosclerosis in people living with HIV. While HIV infection is controlled by antiretroviral medication, HIV is not cured and thus persons living with HIV must take antiretroviral medications chronically.

Chronic inflammation and immune activation are also considered the primary drivers of HIV-associated coronary artery disease (CAD). Arjun Sinha, MD, MS, and Matthew Feinstein, MD, MS, examine the clinical features of CAD in HIV patients.

“Inflammation is now recognized as an important factor in cardiovascular disease, however, the reason for increased inflammation in patients who develop heart disease, especially in those living with HIV, remains unclear,” notes Dr. Sinha, Division of Cardiology, Department of Medicine, Northwestern University Feinberg School of Medicine, Chicago, IL, USA. “Despite treatment with antiretroviral therapy that eradicates the HIV virus from the blood, low levels of the virus remain active in the intestines leading to changes in the intestinal lining and bacteria. How these changes lead to increased inflammation and heart disease is an important area of research as it can have broader implications for the population at large."

Numerous studies have shown increased plaque buildup and heart attacks in people living with HIV. This is despite the fact that the vast majority are well treated with ART. During the initial years of ART, some HIV medications were thought to be the reason behind this increased risk because they would cause weight gain, high cholesterol, and triglycerides. While this was a valid concern, current ARTs do not have those side effects. However, the increased CVD risk remains. “We are learning that even after suppression of the virus in the blood with these newer agents, there is increased inflammation and changes in the immune system that put these individuals at a higher risk of heart attacks. The HIV virus still hides in certain parts of the body such as the intestines likely leading to these problematic changes,” notes Dr. Feinstein, Department of Preventive Medicine, Northwestern University Feinberg School of Medicine, Chicago, IL, USA.

Decision tree showing the clinical and immunologic factors implicated in HIV-associated CAD
Clinical and immunologic factors implicated in HIV-associated CAD.  HDL = high density lipoprotein; IV = intravenous; MI = myocardial infarction, NSTEMI = non-ST- segment elevation myocardial infarction, STEMI = ST-segment elevation myocardial infarction.

The authors also delve into differences in the presentation and outcomes of CAD and acute coronary syndrome between HIV-infected and non-infected patients, including lower age at presentation, more non-calcified plaque, increased risk of 30-day in-hospital mortality and recurrent MI, and higher risk of ST-segment elevation MIs, and the higher risks observed in women vs. men with HIV.

The authors emphasize the importance of early and continuous ART therapy in reducing CVD risk and find that many risk estimation tools developed from general populations underestimate CVD risk in HIV patients. “We also have to become better at predicting the risk of future cardiovascular events in people living with HIV so that we can identify who will benefit from starting therapies that are already available,” comments Dr. Sinha.

This special issue also includes reviews on other cardiovascular concerns for patients with HIV, such as stroke, heart failure, pulmonary hypertension, and arrhythmias. Dr. Timothy Ryan and colleagues consider the role of vascular imaging in the risk assessment of people with HIV. Dr. Pierre Gigere provides an in-depth description of potential drug-drug interactions between ART and CV medications, which is especially important when treating patients who take multiple drugs and have several comorbidities. Dr. Bobby Yanagawa discusses cardiac surgery in HIV patients, including protective measures for the surgical staff.

“People with HIV have significantly higher risk for heart disease, including heart attack and heart failure, than people without HIV. This higher risk remains, even after accounting for demographic factors, common heart disease risk factors, and HIV medications. The majority of people with HIV in high income countries are now over 50 years old. This underscores the importance of understanding WHY people with HIV get heart disease and HOW we can curb the HIV-heart disease epidemic,” says Dr. Feinstein.

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Notes for editors

Acquired Immunodeficiency and Heart Disease
Guest Editors: Girish Dwivedi, MD, DM, PhD, Priscilla Hsue, MD, and David Waters, MD
Canadian Journal of Cardiology, volume 35, issue 3 (March 2019) published by Elsevier.
www.onlinecjc.ca/issue/S0828-282X(18)X0016-6

The featured articles are: “Introduction to Cardiovascular Issues in HIV,” by David D. Waters, MD and Priscilla Y. Hsue, MD (https://doi.org/10.1016/j.cjca.2018.12.009).
Author contact: David D. Waters at David.Waters@ucsf.edu

“Mechanisms of Cardiovascular Disease in the Setting of HIV Infection,” by Priscilla Y. Hsue, MD (https://doi.org/10.1016/j.cjca.2018.12.024).
Author contact: Priscilla Y. Hsue at Priscilla.Hsue@ucsf.edu
This study was funded by NIH (K24AI112393).

“Coronary Artery Disease Manifestations in HIV: What, How, and Why,” by Arjun Sinha, MD, MS, and Matthew J. Feinstein, MD, MS (https://doi.org/10.1016/j.cjca.2018.11.029).
Author contact: Matthew J. Feinstein at matthewjfeinstein@northwestern.edu
Dr. Feinstein reports grant funding from the American Heart Association (16 FTF 31200010) and the National Institutes of Health (P30 AI 117943 Administrative Supplement).

Full text of the articles and editorial is available to credentialed journalists upon request. Contact Eileen Leahy at +1 732 238 3628 or cjcmedia@elsevier.com to obtain copies.

About the Canadian Journal of Cardiology
The Canadian Journal of Cardiology is the official journal of the Canadian Cardiovascular Society. It is a vehicle for the international dissemination of new knowledge in cardiology and cardiovascular science, particularly serving as a major venue for the results of Canadian cardiovascular research and Society guidelines. The journal publishes original reports of clinical and basic research relevant to cardiovascular medicine as well as editorials, review articles, case reports, and papers on health outcomes, policy research, ethics, medical history, and political issues affecting practice. www.onlinecjc.ca

About the Editor-in-Chief
Editor-in-Chief Stanley Nattel, MD, is Paul-David Chair in Cardiovascular Electrophysiology and Professor of Medicine at the University of Montreal and Director of the Electrophysiology Research Program at the Montreal Heart Institute Research Center.

About Elsevier
Elsevier is a global information analytics business that helps scientists and clinicians to find new answers, reshape human knowledge, and tackle the most urgent human crises. For 140 years, we have partnered with the research world to curate and verify scientific knowledge. Today, we’re committed to bringing that rigor to a new generation of platforms. Elsevier provides digital solutions and tools in the areas of strategic research management, R&D performance, clinical decision support, and professional education; including ScienceDirect, Scopus, SciVal, ClinicalKey and Sherpath. Elsevier publishes over 2,500 digitized journals, including The Lancet and Cell, 39,000 e-book titles and many iconic reference works, including Gray's Anatomy. Elsevier is part of RELX, a global provider of information-based analytics and decision tools for professional and business customers. www.elsevier.com

Media contact
Eileen Leahy
Elsevier
+1 732 238 3628
cjcmedia@elsevier.com