4.8 Article

Persistent T Cell Repertoire Perturbation and T Cell Activation in HIV After Long Term Treatment

FRONTIERS IN IMMUNOLOGY (2021)

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Journal

FRONTIERS IN IMMUNOLOGY
Volume 12, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fimmu.2021.634489

Keywords

human immunodeficiency virus; T cell repertoire; blood transcriptome; antiretroviral therapy; people living with HIV; chronic inflammation; T cell activation

Categories

Immunology

Funding

  1. Wellcome Trust [207511/Z/17/Z]
  2. Rosetrees Trust [M824]
  3. National Institute for Health Research [DRF-2015-08-210]
  4. NIHR Biomedical Research Funding
  5. MRC [MR/L001756/1] Funding Source: UKRI
  6. Wellcome Trust [207511/Z/17/Z] Funding Source: Wellcome Trust
  7. National Institutes of Health Research (NIHR) [DRF-2015-08-210] Funding Source: National Institutes of Health Research (NIHR)

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In people living with HIV on long term anti-retroviral therapy, the diversity of T cell receptor repertoires remains significantly depleted, skewed by idiosyncratic clones, and associated with persistent T cell activation. Further investigation on thymic function and antigenic drivers of T cell clonal selection in PLHIV are crucial for restoring normal immune function.
Objective In people living with HIV (PLHIV), we sought to test the hypothesis that long term anti-retroviral therapy restores the normal T cell repertoire, and investigate the functional relationship of residual repertoire abnormalities to persistent immune system dysregulation. Methods We conducted a case-control study in PLHIV and HIV-negative volunteers, of circulating T cell receptor repertoires and whole blood transcriptomes by RNA sequencing, complemented by metadata from routinely collected health care records. Results T cell receptor sequencing revealed persistent abnormalities in the clonal T cell repertoire of PLHIV, characterized by reduced repertoire diversity and oligoclonal T cell expansion correlated with elevated CD8 T cell counts. We found no evidence that these expansions were driven by cytomegalovirus or another common antigen. Increased frequency of long CDR3 sequences and reduced frequency of public sequences among the expanded clones implicated abnormal thymic selection as a contributing factor. These abnormalities in the repertoire correlated with systems level evidence of persistent T cell activation in genome-wide blood transcriptomes. Conclusions The diversity of T cell receptor repertoires in PLHIV on long term anti-retroviral therapy remains significantly depleted, and skewed by idiosyncratic clones, partly attributable to altered thymic output and associated with T cell mediated chronic immune activation. Further investigation of thymic function and the antigenic drivers of T cell clonal selection in PLHIV are critical to efforts to fully re-establish normal immune function.

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