Hyaluronan‐binding by CD44 reduces the memory potential of activated murine CD8 T cells |
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| Authors: | Sally S M Lee‐Sayer Nina Maeshima Meghan N Dougan Anita Dahiya Arif A Arif Manisha Dosanjh Christopher A Maxwell Pauline Johnson |
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| Institution: | 1. Department of Microbiology and Immunology, University of British Columbia, Vancouver, BC, Canada;2. Department of Pediatrics, British Columbia Children's Hospital Research Institute, University of British Columbia, Vancouver, BC, Canada |
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| Abstract: | Expansion and death of effector CD8 T cells are regulated to limit immunopathology and cells that escape contraction go on to generate immunological memory. CD44, a receptor for the extracellular matrix component hyaluronan, is a marker of activated and memory T cells. Here, we show with a murine model that the increase in CD44 expression and hyaluronan binding induced upon CD8 T cell activation was proportional to the strength of TCR engagement, thereby identifying the most strongly activated T cells. When CD44?/? and CD44+/+ OT‐I CD8 T cells were adoptively transferred into mice challenged with Listeria‐OVA, there was a slight increase in the percentage of CD44+/+ cells at the effector site. However, CD44+/+ cells were out‐competed by CD44?/? cells after the contraction phase in the lymphoid tissues, and the CD44?/? cells preferentially formed more memory cells. The hyaluronan‐binding CD44+/+ CD8 effector T cells showed increased pAkt expression, higher glucose uptake, and were more susceptible to cell death during the contraction phase compared to non‐binding CD44+/+ and CD44?/? OT‐I CD8 T cells, suggesting that CD44 and its engagement with hyaluronan skews CD8 T cells toward a terminal effector differentiation state that reduces their ability to form memory cells. |
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| Keywords: | CD44 Hyaluronan Memory CD8 T cell formation T cell contraction |
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