Engagement of the CD3/T cell antigen receptor complex on small, resting T cells is insufficient to trigger cell-mediated cytotoxicity or to induce a proliferative response. In the present study, we have used genetic transfection to demonstrate that interaction of the B7-BB1 B cell activation antigen with the CD28 T cell differentiation antigen costimulates cell-mediated cytotoxicity and proliferation initiated by either anti-CD2 or anti-CD3 monoclonal antibody (mAb). Moreover, a B7-negative Burkitt's lymphoma cell line that fails to stimulate an allogeneic mixed lymphocyte response is rendered a potent stimulator after transfection with B7. The mixed leukocyte reaction proliferative response against the B7 transfectant is inhibited by either anti-CD28 or B7 mAb. We also demonstrate that freshly isolated small, resting human T cells can mediate anti-CD3 or anti-CD2 mAb-redirected cytotoxicity against a murine Fc receptor-bearing mastocytoma transfected with human B7. These preexisting cytotoxic T lymphocytes in peripheral blood are present in both the CD4 and CD8 subsets, but are preferentially within the CD45RO+ "memory" population. While small, resting T cells apparently require costimulation by CD28/B7 interactions, this requirement is lost after T cell activation. Anti-CD3 initiates a cytotoxic response mediated by in vitro cultured T cell clones in the absence of B7 ligand. The existence of functional cytolytic T cells in the small, resting T cell population may be advantageous in facilitating rapid responses to immune challenge.
Skip Nav Destination
Article navigation
1 February 1992
Article|
February 01 1992
CD28 interaction with B7 costimulates primary allogeneic proliferative responses and cytotoxicity mediated by small, resting T lymphocytes.
M Azuma,
M Azuma
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
Search for other works by this author on:
M Cayabyab,
M Cayabyab
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
Search for other works by this author on:
D Buck,
D Buck
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
Search for other works by this author on:
J H Phillips,
J H Phillips
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
Search for other works by this author on:
L L Lanier
L L Lanier
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
Search for other works by this author on:
M Azuma
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
M Cayabyab
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
D Buck
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
J H Phillips
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
L L Lanier
Department of Immunology, DNAX Research Institute for Molecular and Cellular Biology, Palo Alto, California 94304.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1992) 175 (2): 353–360.
Citation
M Azuma, M Cayabyab, D Buck, J H Phillips, L L Lanier; CD28 interaction with B7 costimulates primary allogeneic proliferative responses and cytotoxicity mediated by small, resting T lymphocytes.. J Exp Med 1 February 1992; 175 (2): 353–360. doi: https://doi.org/10.1084/jem.175.2.353
Download citation file:
Sign in
Don't already have an account? Register
Client Account
You could not be signed in. Please check your email address / username and password and try again.
Could not validate captcha. Please try again.
Sign in via your Institution
Sign in via your InstitutionEmail alerts
Advertisement