BMC Infectious Diseases (Jan 2024)

Mitochondrial disturbance related to increased caspase-1 of CD4+T cells in HIV-1 infection

  • Fengting Yu,
  • Chengjie Ma,
  • Xia Jin,
  • Hongxin Zhao,
  • Jiang Xiao,
  • Li Li,
  • Shujing Song,
  • Xiaohui Xie,
  • Siyuan Yang,
  • Yunxia Tang,
  • Linghang Wang,
  • Fujie Zhang

DOI
https://doi.org/10.1186/s12879-023-08485-5
Journal volume & issue
Vol. 24, no. 1
pp. 1 – 11

Abstract

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Abstract Background In HIV-1 infection, more than 95% of CD4+T cells die of caspase-1 mediated pyroptosis. What governs the increased susceptibility of CD4+T cells to pyroptosis is poorly understood. Methods Blood samples were obtained from 31 untreated HIV-infected patients (UNT), 29 antiretroviral therapy treated HIV-infected patients (ART), and 21 healthy control donors (HD). Plasma levels of IL-18 and IL-1β, caspase-1 expression, mitochondrial mass (MM) and mitochondrial fusion/fisson genes of CD4+T subsets were measured. Results A significantly higher IL-18 level in plasma and MM level of CD4+T cells were found in HIV-infected patients (UNT and ART) compared to HD, and the MMhigh phenotype was manifested, related to increased caspase-1 expression. Moreover, the increased MM was more pronounced in the early differentiated and inactivated CD4+T cells. However, higher MM was not intrinsically linked to T cell differentiation disorder or excessive activation of the CD4+T cells. Mechanistically, the increased MM was significantly correlated with an elevated level of expression of the mitochondrial fusion gene mitofusin1. Conclusion An increase in MM was associated with heightened sensitivity of CD4+T cells to pyroptosis, even in early differentiated and inactivated CD4+T cells, in patients with HIV-1 infection, regardless of whether patients were on antiretroviral therapy or not. These new revelations have uncovered a previously unappreciated challenge to immune reconstitution with antiretroviral therapy.

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