Cell Reports (Jul 2017)

Mass Cytometric Analysis of HIV Entry, Replication, and Remodeling in Tissue CD4+ T Cells

  • Marielle Cavrois,
  • Trambak Banerjee,
  • Gourab Mukherjee,
  • Nandhini Raman,
  • Rajaa Hussien,
  • Brandon Aguilar Rodriguez,
  • Joshua Vasquez,
  • Matthew H. Spitzer,
  • Nicole H. Lazarus,
  • Jennifer J. Jones,
  • Christina Ochsenbauer,
  • Joseph M. McCune,
  • Eugene C. Butcher,
  • Ann M. Arvin,
  • Nandini Sen,
  • Warner C. Greene,
  • Nadia R. Roan

DOI
https://doi.org/10.1016/j.celrep.2017.06.087
Journal volume & issue
Vol. 20, no. 4
pp. 984 – 998

Abstract

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To characterize susceptibility to HIV infection, we phenotyped infected tonsillar T cells by single-cell mass cytometry and created comprehensive maps to identify which subsets of CD4+ T cells support HIV fusion and productive infection. By comparing HIV-fused and HIV-infected cells through dimensionality reduction, clustering, and statistical approaches to account for viral perturbations, we identified a subset of memory CD4+ T cells that support HIV entry but not viral gene expression. These cells express high levels of CD127, the IL-7 receptor, and are believed to be long-lived lymphocytes. In HIV-infected patients, CD127-expressing cells preferentially localize to extrafollicular lymphoid regions with limited viral replication. Thus, CyTOF-based phenotyping, combined with analytical approaches to distinguish between selective infection and receptor modulation by viruses, can be used as a discovery tool.

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