CD4 T Cell-dependent CD8 T Cell Maturation
Overview
Affiliations
We have investigated the contribution of CD4 T cells to the optimal priming of functionally robust memory CD8 T cell subsets. Intranasal infection of CD4 T cell-deficient (CD4(-/-)) mice with lymphocytic choriomeningitis virus resulted in the elaboration of virus-specific CD8 T cell responses that cleared the infection. However, by comparison with normal mice, the virus-specific CD8 T cells in CD4(-/-) mice were quantitatively and qualitatively different. In normal mice, lymphocytic choriomeningitis virus-specific memory CD8 T cells are CD44(high), many are CD122(high), and a majority of these cells regain expression of CD62L overtime. These cells produce IFN-gamma and TNF-alpha, and a subset also produces IL-2. In the absence of CD4 T cell help, a distinct subset of memory CD8 T cells develops that remains CD62L(low) up to 1 year after infection and exhibits a CD44(int)CD122(low) phenotype. These cells are qualitatively different from their counterparts in normal hosts, as their capacity to produce TNF-alpha and IL-2 is diminished. In addition, although CD4-independent CD8 T cells can contain the infection following secondary viral challenge, their ability to expand is impaired. These findings suggest that CD4 T cell responses not only contribute to the optimal priming of CD8 T cells in chronically infected hosts, but are also critical for the phenotypic and functional maturation of CD8 T cell responses to Ags that are more rapidly cleared. Moreover, these data imply that the development of CD62L(high) central memory CD8 T cells is arrested in the absence of CD4 T cell help.
Helper T cell immunity in humans with inherited CD4 deficiency.
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CD4 and CD8 T cells reduce inflammation and promote bone healing in response to titanium implants.
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PMID: 38554889 PMC: 11045310. DOI: 10.1016/j.actbio.2024.03.022.
CD4 T help promotes influenza virus-specific CD8 T cell memory by limiting metabolic dysfunction.
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PMID: 30787194 PMC: 6410826. DOI: 10.1073/pnas.1808849116.
Tetherin/BST-2: Restriction Factor or Immunomodulator?.
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PMID: 26957198 PMC: 5466165. DOI: 10.2174/1570162x14999160224102752.
Tetherin/BST-2 promotes dendritic cell activation and function during acute retrovirus infection.
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PMID: 26846717 PMC: 4742778. DOI: 10.1038/srep20425.