The HIV-1 reservoir in eight patients on long-term suppressive antiretroviral therapy is stable with few genetic changes over time

L Josefsson, S Von Stockenstrom… - Proceedings of the …, 2013 - National Acad Sciences
L Josefsson, S Von Stockenstrom, NR Faria, E Sinclair, P Bacchetti, M Killian, L Epling…
Proceedings of the National Academy of Sciences, 2013National Acad Sciences
The source and dynamics of persistent HIV-1 during long-term combinational antiretroviral
therapy (cART) are critical to understanding the barriers to curing HIV-1 infection. To
address this issue, we isolated and genetically characterized HIV-1 DNA from naïve and
memory T cells from peripheral blood and gut-associated lymphoid tissue (GALT) from eight
patients after 4–12 y of suppressive cART. Our detailed analysis of these eight patients
indicates that persistent HIV-1 in peripheral blood and GALT is found primarily in memory …
The source and dynamics of persistent HIV-1 during long-term combinational antiretroviral therapy (cART) are critical to understanding the barriers to curing HIV-1 infection. To address this issue, we isolated and genetically characterized HIV-1 DNA from naïve and memory T cells from peripheral blood and gut-associated lymphoid tissue (GALT) from eight patients after 4–12 y of suppressive cART. Our detailed analysis of these eight patients indicates that persistent HIV-1 in peripheral blood and GALT is found primarily in memory CD4+ T cells [CD45RO+/CD27(+/−)]. The HIV-1 infection frequency of CD4+ T cells from peripheral blood and GALT was higher in patients who initiated treatment during chronic compared with acute/early infection, indicating that early initiation of therapy results in lower HIV-1 reservoir size in blood and gut. Phylogenetic analysis revealed an HIV-1 genetic change between RNA sequences isolated before initiation of cART and intracellular HIV-1 sequences from the T-cell subsets after 4–12 y of suppressive cART in four of the eight patients. However, evolutionary rate analyses estimated no greater than three nucleotide substitutions per gene region analyzed during all of the 4–12 y of suppressive therapy. We also identified a clearly replication-incompetent viral sequence in multiple memory T cells in one patient, strongly supporting asynchronous cell replication of a cell containing integrated HIV-1 DNA as the source. This study indicates that persistence of a remarkably stable population of infected memory cells will be the primary barrier to a cure, and, with little evidence of viral replication, this population could be maintained by homeostatic cell proliferation or other processes.
National Acad Sciences