Human memory T lymphocytes express increased levels of three cell adhesion molecules (LFA-3, CD2, and LFA-1) and three other molecules (UCHL1, CDw29, and Pgp-1) and have enhanced IFN-gamma production.
10.4049/jimmunol.140.5.1401
Crossref journal-article
Oxford University Press (OUP)
The Journal of Immunology (286)
Abstract

Abstract Studies of cell-surface molecules involved in human T cell interaction reveal that differential expression of each of three adhesion molecules (LFA-3, CD2, and LFA-1) subdivides human peripheral blood T cells into major subpopulations. Systematic analysis of the relationship between expression of these and other markers of T cell subsets demonstrates a single major subset of human peripheral blood T lymphocytes distinguished by enhanced expression of LFA-3, CD2, LFA-1, and three other markers (CDw29 [4B4], UCHL1, and Pgp-1). Large differences in relative expression are observed for UCHL1 (29-fold) and LFA-3 (greater than 8-fold), and smaller differences (2- to 4-fold) are seen for CDw29, CD2, LFA-1, and Pgp-1. Bimodal distribution of LFA-3 is found on both CD4+ cells and on CD8+ cells as well as on B lymphocytes (CD19+). Neonatal T cells (CD3+) are comprised almost exclusively of the subset expressing low LFA-3, CD2, LFA-1, CDw29, and UCHL1. Activation of cord peripheral blood mononuclear leukocytes with PHA leads to uniform enhanced expression of each of these molecules on CD3+ cells. Functional analyses of these T cell subsets were performed after sorting of adult T cells based on differential LFA-3 expression. Only the LFA-3+ subset proliferated in response to the Ag tetanus toxoid, even though the LFA-3- subset proliferated more strongly to PHA. Furthermore, the LFA-3+ subset made greater than fivefold more IFN-gamma than the LFA-3- subset in response to PHA, despite the fact that both subsets made equivalent amounts of IL-2. This phenotypic and functional analysis of resting and activated newborn and adult T cells indicates that human memory T cells express enhanced levels of LFA-3, CD2, LFA-1, UCHL1, CDw29, and Pgp-1; we speculate that the increase in expression of T cell adhesion molecules LFA-3, CD2, and LFA-1 on memory cells is functionally important in their enhanced responsiveness.

Bibliography

Sanders, M. E., Makgoba, M. W., Sharrow, S. O., Stephany, D., Springer, T. A., Young, H. A., & Shaw, S. (1988). Human memory T lymphocytes express increased levels of three cell adhesion molecules (LFA-3, CD2, and LFA-1) and three other molecules (UCHL1, CDw29, and Pgp-1) and have enhanced IFN-gamma production. The Journal of Immunology, 140(5), 1401–1407.

Authors 7
  1. M E Sanders (first)
  2. M W Makgoba (additional)
  3. S O Sharrow (additional)
  4. D Stephany (additional)
  5. T A Springer (additional)
  6. H A Young (additional)
  7. S Shaw (additional)
References 0 Referenced 678

None

Dates
Type When
Created 2 years, 7 months ago (Dec. 31, 2022, 1:34 a.m.)
Deposited 7 months, 3 weeks ago (Jan. 2, 2025, 1:14 p.m.)
Indexed 1 month, 3 weeks ago (July 4, 2025, 6:08 a.m.)
Issued 37 years, 5 months ago (March 1, 1988)
Published 37 years, 5 months ago (March 1, 1988)
Published Print 37 years, 5 months ago (March 1, 1988)
Funders 0

None

@article{Sanders_1988, title={Human memory T lymphocytes express increased levels of three cell adhesion molecules (LFA-3, CD2, and LFA-1) and three other molecules (UCHL1, CDw29, and Pgp-1) and have enhanced IFN-gamma production.}, volume={140}, ISSN={1550-6606}, url={http://dx.doi.org/10.4049/jimmunol.140.5.1401}, DOI={10.4049/jimmunol.140.5.1401}, number={5}, journal={The Journal of Immunology}, publisher={Oxford University Press (OUP)}, author={Sanders, M E and Makgoba, M W and Sharrow, S O and Stephany, D and Springer, T A and Young, H A and Shaw, S}, year={1988}, month=mar, pages={1401–1407} }