Frontiers in Immunology (Aug 2018)

KIR3DL1-Negative CD8 T Cells and KIR3DL1-Negative Natural Killer Cells Contribute to the Advantageous Control of Early Human Immunodeficiency Virus Type 1 Infection in HLA-B Bw4 Homozygous Individuals

  • Xin Zhang,
  • Xin Zhang,
  • Xiaofan Lu,
  • Xiaofan Lu,
  • Christiane Moog,
  • Christiane Moog,
  • Lin Yuan,
  • Lin Yuan,
  • Zhiying Liu,
  • Zhiying Liu,
  • Zhen Li,
  • Zhen Li,
  • Wei Xia,
  • Wei Xia,
  • Yuefang Zhou,
  • Yuefang Zhou,
  • Hao Wu,
  • Hao Wu,
  • Tong Zhang,
  • Tong Zhang,
  • Bin Su,
  • Bin Su

DOI
https://doi.org/10.3389/fimmu.2018.01855
Journal volume & issue
Vol. 9

Abstract

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Bw4 homozygosity in human leukocyte antigen class B alleles has been associated with a delayed acquired immunodeficiency syndrome (AIDS) development and better control of human immunodeficiency virus type 1 (HIV-1) viral load (VL) than Bw6 homozygosity. Efficient CD8 T cell and natural killer (NK) cell functions have been described to restrain HIV-1 replication. However, the role of KIR3DL1 expression on these cells was not assessed in Bw4-homozygous participants infected with HIV-1 CRF01_A/E subtype, currently the most prevalent subtype in China. Here, we found that the frequency of KIR3DL1-expressing CD8 T cells of individuals homozygous for Bw6 [1.53% (0–4.56%)] was associated with a higher VL set point (Spearman rs = 0.59, P = 0.019), but this frequency of KIR3DL1+CD8+ T cells [1.37% (0.04–6.14%)] was inversely correlated with CD4 T-cell count in individuals homozygous for Bw4 (rs = −0.59, P = 0.011). Moreover, CD69 and Ki67 were more frequently expressed in KIR3DL1−CD8+ T cells in individuals homozygous for Bw4 than Bw6 (P = 0.046 for CD69; P = 0.044 for Ki67), although these molecules were less frequently expressed in KIR3DL1+CD8+ T cells than in KIR3DL1−CD8+ T cells in both groups (all P < 0.05). KIR3DL1−CD8+ T cells have stronger p24-specific CD8+ T-cell responses secreting IFN-γ and CD107a than KIR3DL1+CD8+ T cells in both groups (all P < 0.05). Thus, KIR3DL1 expression on CD8 T cells were associated with the loss of multiple functions. Interestingly, CD69+NK cells lacking KIR3DL1 expression were inversely correlated with HIV-1 VL set point in Bw4-homozygous individuals (rs = −0.52, P = 0.035). Therefore, KIR3DL1−CD8+ T cells with strong early activation and proliferation may, together with KIR3DL1−CD69+NK cells, play a protective role during acute/early HIV infection in individuals homozygous for Bw4. These findings highlight the superior functions of KIR3DL1−CD8+ T cells and KIR3DL1−CD69+NK cells being a potential factor contributing to delayed disease progression in the early stages of HIV-1 infection.

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