The immune synapses reveal aberrant functions of CD8 T cells during chronic HIV infection.
Nadia AnikeevaMaria SteblyankoLeticia Kuri-CervantesMarcus BuggertMichael R BettsYuri SykulevPublished in: Nature communications (2022)
Chronic HIV infection causes persistent low-grade inflammation that induces premature aging of the immune system including senescence of memory and effector CD8 T cells. To uncover the reasons of gradually diminished potency of CD8 T cells from people living with HIV, here we expose the T cells to planar lipid bilayers containing ligands for T-cell receptor and a T-cell integrins and analyze the cellular morphology, dynamics of synaptic interface formation and patterns of the cellular degranulation. We find a large fraction of phenotypically naive T cells from chronically infected people are capable to form mature synapse with focused degranulation, a signature of a differentiated T cells. Further, differentiation of aberrant naive T cells may lead to the development of anomalous effector T cells undermining their capacity to control HIV and other pathogens that could be contained otherwise.
Keyphrases
- antiretroviral therapy
- hiv infected
- low grade
- human immunodeficiency virus
- hiv positive
- high grade
- hiv aids
- regulatory t cells
- dendritic cells
- oxidative stress
- type iii
- endothelial cells
- hepatitis c virus
- genome wide
- working memory
- molecular dynamics simulations
- fatty acid
- drug induced
- single cell
- stress induced
- men who have sex with men
- antimicrobial resistance