During their differentiation, thymocytes are subjected to two rounds o
f selection. First, CD4(-)8(-) double-negative (DN) thymocytes with a
functional TCR-beta chain express a alpha(-)beta(+) CD3 complex on the
ir surface and, as a consequence, are selected to mature to the CD4(+)
8(+) double-positive (DP) stage. This round ends after the initial pro
liferation of young DP thymocytes and is termed beta-chain selection.
Second, DP thymocytes are selected on the basis of their alpha(+)beta(
+) CD3 complex. This is termed repertoire selection and the cells are
given three choices: death by neglect selection, death by positive sel
ection, or deletion by negative selection. Using anti-CD3 epsilon mAb
as invariant ligand, signals for beta-chain selection of DN cells incl
uding proliferation of DP cells do not require a Ca2+ response, are in
dependent of CD3 zeta, and are only slightly impaired in the absence o
f p56(lck) (lck). Signals that induce positive selection of DP thymocy
tes require a partial Ca2+ response and CD3 zeta but are independent o
f lck. Deletion of DP thymocytes requires a full-blown Ca2+ response a
nd both, CD3 zeta and lck. Thymic selection thus appears to be governe
d by a gradient of signal intensities.