Initial HIV-1 Viral Load in French Guiana: Factors Associated with Viral Load Set Point Differences

Overview

Journal IJID Reg

Specialty Infectious Diseases

Date 2024 Dec 18

PMID 39691355

Authors

Aude Lucarelli

Sebastien Rabier

Fanja Vergeade

Myriam El Guedj

Tania Vaz

Hawa Cisse

Loic Epelboin

Philippe Abboud

Paul Le Turnier

Felix Djossou

Celine Michaud

Claudia Delin

Flavia Divino

Karine Verin

Ketty Bienvenu

Antoine Adenis

Mathieu Nacher

Affiliations

Soon will be listed here.

Abstract

Objectives: HIV viral load set points may vary between virus subtypes and host characteristics. The HIV epidemic in French Guiana entails a mix of viruses and populations of cosmopolitan origins. In this epidemiological context, we aimed to determine whether, at the scale of our territory, we could identify differences in HIV-1 viral load setpoints in our hospital cohort.

Methods: The French Guiana hospital cohort was retrospectively analyzed between 1992 and 2023. Bootstrapped (100 replications) quantile (median) regression modeled the initial HIV-1 viral load with age, sex, nationality, and cluster of differentiation (CD) 4 count at diagnosis as independent variables.

Results: After adjusting for period of analysis and CD4 count at diagnosis, bootstrapped quantile regression (median) showed that Haitians (minus 20,088 copies, <0.0001) and Guyanese (minus 14,087, = 0.039) had a significantly lower viral load at HIV diagnosis than French, males had a greater viral load at HIV diagnosis than females (plus 16,430 copies, <0.0001), each additional year of age was associated with more copies (+345 per year, = 0.002). When compared to those with more than 500 CD4 per ml, persons with CD4 counts at diagnosis below 200 per ml had a greater initial viral load (plus 94,932 copies, <0.0001), as did those with 200-350 CD4 per ml (plus 13,088 copies, <0.0001), and those with (350-500 CD4 per ml) (plus 5643 copies, <0.0001). Non-B viruses seemed to have an independently greater viral load at diagnosis than B viruses (plus 58,402, = 0.029).

Conclusions: We show some significant differences in the viral load set point of different groups. For nationalities, we are inclined to attribute this to differences in the frequency of infecting subtypes. This suggests that models of incidence or date of infection based on CD4 decline may be distorted by this situation.

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