Awardee OrganizationUNIVERSITY OF CALIFORNIA-IRVINE
Description
Abstract Text
Contact with antigen-presenting cells initiates an activation
cascade within T lymphocytes, including a rise in cytosolic calcium,
lymphokine production, and cell division. Calcium imaging combined
with an optical trap enabled the T-cell contact requirements and
polarity to be investigated at the single-cell level. Anti-CD3
mAb-coated beads induced calcium signaling with ~ ten-fold higher
frequency upon contact with the leading edge of the T cell, compared
with the trailing edge. Engagement of at least 340 T cell receptors
(~1% of the total on the cell) was required to initiate Ca2+
signaling, and the minimal contact area was ~3 (m2. Our results
indicate that ~1000 TCRs are required to generate a long-lasting
[Ca2+]i signal which might be required for gene expression. We expect
this approach can be combined with ligands for accessory molecules or
with downstream assays for gene expression in order to examine species
and clonal-specific variations in the T cell resp onse and deepen our
understanding of the relationship between early activation events and
gene expression.
No Sub Projects information available for 3P41RR001192-20S1 0018
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