Relationship between Modern ART Regimens and Immunosenescence Markers in Patients with Chronic HIV Infection
Author:
Grozdeva Rusina1, Ivanov Daniel1ORCID, Strashimirov Dimitar1ORCID, Kapincheva Nikol1, Yordanova Ralitsa1ORCID, Mihailova Snejina2, Georgieva Atanaska2, Alexiev Ivailo3ORCID, Grigorova Lyubomira3ORCID, Partsuneva Alexandra3, Dimitrova Reneta3ORCID, Gancheva Anna3, Kostadinova Asya3, Naseva Emilia45ORCID, Yancheva Nina1ORCID
Affiliation:
1. Department of Infectious Diseases, Parasitology and Tropical Medicine, Medical University Sofia, 1431 Sofia, Bulgaria 2. Central Laboratory of Clinical Immunology, University Hospital Alexandrovska, 1431 Sofia, Bulgaria 3. National Reference Laboratory of HIV, National Center of Infectious and Parasitic Diseases (NCIPD), 1504 Sofia, Bulgaria 4. Department of Health Economics, Faculty of Public Health “Prof. Tsekomir Vodenicharov, MD, DSc”, Medical University of Sofia, 1527 Sofia, Bulgaria 5. Medical Faculty, Sofia University St. Kliment Ohridski, 1407 Sofia, Bulgaria
Abstract
The increased life expectancy of PLHIV (People Living with HIV) and the successful highly combined antiretroviral therapy (cART) poses new clinical challenges regarding aging and its co-morbid condition. It is commonly believed that HIV infection “accelerates” aging. Human immunodeficiency virus type 1 (HIV-1) infection is characterized by inflammation and immune activation that persists despite cART, and that may contribute to the development of co-morbid conditions. In this regard, we aimed to compare current cART regimens in light of premature aging to evaluate differences in their ability to reduce immune activation and inflammation in virologically suppressed patients. We studied a panel of biomarkers (IFN-γ, IL-1β, IL-12p70, IL-2, IL-4, IL-5, IL-6, IL-13, IL-18, GM-CSF, TNF-α, C-reactive protein, D-dimer, soluble CD14), which could provide a non-invasive and affordable approach to monitor HIV-related chronic inflammation. The results of the current study do not provide hard evidence favoring a particular cART regimen, although they show a less favorable regimen profile containing a protease inhibitor. Our data suggest an incomplete reduction of inflammation and immune activation in terms of the effective cART. It is likely that the interest in various biomarkers related to immune activation and inflammation as predictors of clinical outcomes among PLHIV will increase in the future.
Funder
Medical University Sofia
Reference41 articles.
1. Joint United Nations Programme on HIV/AIDS (2023). The Path That Ends AIDS: UNAIDS Global AIDS Update 2023, Joint United Nations Programme on HIV/AIDS. 2. Centers for Disease Control (CDC) (2018). Monitoring Selected National HIV Prevention and Care Objectives by Using HIV Surveillance Data: United States and 6 Dependent Areas–2013, HIV Surveillance Supplemental Report; Centers for Disease Control (CDC). 3. Premature age-related comorbidities among HIV-infected persons compared with the general population;Guaraldi;Clin. Infect. Dis.,2011 4. Rickabaugh, T.M., Baxter, R.M., Sehl, M., Sinsheimer, J.S., Hultin, P.M., Hultin, L.E., Quach, A., Martinez-Maza, O., Horvath, S., and Vilain, E. (2015). Acceleration of age-associated methylation patterns in HIV-1-infected adults. PLoS ONE, 10. 5. Morbidity in older HIV-infected patients: Impact of long-term antiretroviral use;Guaraldi;AIDS Rev.,2014
|
|