Defining Kinetic Properties of HIV-Specific CD8⁺ T-Cell Responses in Acute Infection

Yiding Yang; Vitaly V Ganusov

doi:10.3390/microorganisms7030069

Defining Kinetic Properties of HIV-Specific CD8⁺ T-Cell Responses in Acute Infection

Microorganisms. 2019 Mar 4;7(3):69. doi: 10.3390/microorganisms7030069.

Authors

Yiding Yang¹, Vitaly V Ganusov^{2

3

4}

Affiliations

¹ Department of Microbiology, University of Tennessee, Knoxville, TN 37996, USA. yidingyang@gmail.com.
² Department of Microbiology, University of Tennessee, Knoxville, TN 37996, USA. vitaly.ganusov@gmail.com.
³ National Institute for Mathematical and Biological Synthesis, University of Tennessee, Knoxville, TN 37996, USA. vitaly.ganusov@gmail.com.
⁴ Department of Mathematics, University of Tennessee, Knoxville, TN 37996, USA. vitaly.ganusov@gmail.com.

Abstract

Multiple lines of evidence indicate that CD8 + T cells are important in the control of HIV-1 (HIV) replication. However, CD8 + T cells induced by natural infection cannot eliminate the virus or reduce viral loads to acceptably low levels in most infected individuals. Understanding the basic quantitative features of CD8 + T-cell responses induced during HIV infection may therefore inform us about the limits that HIV vaccines, which aim to induce protective CD8 + T-cell responses, must exceed. Using previously published experimental data from a cohort of HIV-infected individuals with sampling times from acute to chronic infection we defined the quantitative properties of CD8 + T-cell responses to the whole HIV proteome. In contrast with a commonly held view, we found that the relative number of HIV-specific CD8 + T-cell responses (response breadth) changed little over the course of infection (first 400 days post-infection), with moderate but statistically significant changes occurring only during the first 35 symptomatic days. This challenges the idea that a change in the T-cell response breadth over time is responsible for the slow speed of viral escape from CD8 + T cells in the chronic infection. The breadth of HIV-specific CD8 + T-cell responses was not correlated with the average viral load for our small cohort of patients. Metrics of relative immunodominance of HIV-specific CD8 + T-cell responses such as Shannon entropy or the Evenness index were also not significantly correlated with the average viral load. Our mathematical-model-driven analysis suggested extremely slow expansion kinetics for the majority of HIV-specific CD8 + T-cell responses and the presence of intra- and interclonal competition between multiple CD8 + T-cell responses; such competition may limit the magnitude of CD8 + T-cell responses, specific to different epitopes, and the overall number of T-cell responses induced by vaccination. Further understanding of mechanisms underlying interactions between the virus and virus-specific CD8 + T-cell response will be instrumental in determining which T-cell-based vaccines will induce T-cell responses providing durable protection against HIV infection.

Keywords: CD8+ T cells; acute HIV infection; competition; immune response; mathematical model; multiple epitopes; vaccines.

Abstract

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