Enhanced surface TCR replenishment mediated by CD28 leads to greater TCR engagement during primary stimulation

doi:10.1093/intimm/12.6.833

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International Immunology, Vol. 12, No. 6, 833-842, June 2000
© 2000 Japanese Society for Immunology

Enhanced surface TCR replenishment mediated by CD28 leads to greater TCR engagement during primary stimulation

Adam G. Schrum, Andrew D. Wells and Laurence A. Turka

University of Pennsylvania, 701 Clinical Research Bldg, 415 Curie Boulevard, Philadelphia, PA 19104, USA

Correspondence to: L. A. Turka

When T cells are stimulated with high concentrations of strongTCR agonist, engaged TCR are internalized and degraded, resultingin greatly reduced surface TCR levels for up to several dayspost-stimulation. It has been noted that surface TCR levelsrise subsequently, even in the presence of continuing stimulation,but the role of CD28 co-stimulation in surface TCR replenishmenthas not been investigated. Here, we have examined the returnof surface TCR following activation, the availability of theseTCR for antigenic engagement and the role of CD28 in that process.We report that within 24 h of stimulation, the level of surfaceTCR expression becomes dependent on the degree of CD28 signalingprovided during T cell activation. In addition, when cells areremoved from stimulus after 24 h, surface TCR expression recoversto a stable level which exceeds that of unstimulated cells andis proportional to the degree of CD28 co-stimulation. TCR thatreplenish the plasma membrane during T cell activation can bedown-regulated by receptor occupancy with the same efficiencyas TCR on freshly stimulated cells. Thus, as a result of enhancedsurface TCR replenishment, CD28-co-stimulated cells can engageand down-regulate more TCR than co-stimulation-deprived cellsin the face of ongoing stimulation. Furthermore, engagementof newly expressed TCR on activated T cells re-induces CD69,suggesting participation of these replenishing TCR in continuedT cell signaling. These data identify the augmentation of surfaceTCR replenishment during activation as a novel mechanism thatlikely contributes to the enhanced antigenic sensitivity ofCD28-co-stimulated T cells.

Keywords: cellular activation, co-stimulatory molecules, T lymphocytes

Transmitting editor: C. B. Thompson

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