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Activation of LFA-1 through a Ca2+-dependent epitope stimulates lymphocyte adhesion
- Source :
- Journal of Cell Biology, 112, 2, pp. 345-354, The Journal of Cell Biology, Journal of Cell Biology, 112, 345-354. Rockefeller univ press, Journal of cell biology, 112(2), 345-354. Rockefeller University Press, van Kooyk, Y, Weder, P, Hogervorst, F, Verhoeven, A J, van Seventer, G, te Velde, A A, Borst, J, Keizer, G D & Figdor, C G 1991, ' Activation of LFA-1 through a Ca2(+)-dependent epitope stimulates lymphocyte adhesion ', Journal of Cell Biology, vol. 112, no. 2, pp. 345-54 ., Journal of Cell Biology, 112(2), 345-54. Rockefeller University Press, Scopus-Elsevier
- Publication Year :
- 1991
- Publisher :
- Rockefeller univ press, 1991.
-
Abstract
- The leukocyte function-associated molecule-1 (LFA-1) plays a key role in cell adhesion processes between cells of the immune system. We investigated the mechanism that may regulate LFA-1-ligand interactions, which result in cell-cell adhesion. To this end we employed an intriguing anti-LFA-1 alpha mAb (NKI-L16), capable of inducing rather than inhibiting cell adhesion. Aggregation induced by NKI-L16 or Fab fragments thereof is not the result of signals transmitted through LFA-1. The antibody was found to recognize a unique Ca2(+)-dependent activation epitope of LFA-1, which is essentially absent on resting lymphocytes, but becomes induced upon in vitro culture. Expression of this epitope correlates well with the capacity of cells to rapidly aggregate upon stimulation by PMA or through the TCR/CD3 complex, indicating that expression of the NKI-L16 epitope is essential for LFA-1 to mediate adhesion. However, expression of the NKI-L16 epitope in itself is not sufficient for cell binding since cloned T lymphocytes express the NKI-L16 epitope constitutively at high levels, but do not aggregate spontaneously. Based on these observations we propose the existence of three distinct forms of LFA-1: (a) an inactive form, which does not, or only partially exposes the NKI-L16 epitope, found on resting cells; (b) an intermediate, NKI-L16+ form, expressed by mature or previously activated cells; and (c) an active (NKI-L16+) form of LFA-1, capable of high affinity ligand binding, obtained after specific triggering of a lymphocyte through the TCR/CD3 complex, by PMA, or by binding of NKI-L16 antibodies.
- Subjects :
- medicine.drug_class
Monoclonal antibody
Lymphocyte Activation
Epitope
Fluorescence
Cell Line
Epitopes
stomatognathic system
medicine
Cell Adhesion
Humans
Lymphocyte function-associated antigen 1
Lymphocytes
Cell adhesion
GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries)
Cell Aggregation
biology
T-cell receptor
Temperature
Antibodies, Monoclonal
Cell Biology
T lymphocyte
Articles
Molecular biology
Precipitin Tests
Cell aggregation
Lymphocyte Function-Associated Antigen-1
Kinetics
biology.protein
Calcium
Antibody
Signal Transduction
Subjects
Details
- Language :
- English
- ISSN :
- 00219525
- Database :
- OpenAIRE
- Journal :
- Journal of Cell Biology, 112, 2, pp. 345-354, The Journal of Cell Biology, Journal of Cell Biology, 112, 345-354. Rockefeller univ press, Journal of cell biology, 112(2), 345-354. Rockefeller University Press, van Kooyk, Y, Weder, P, Hogervorst, F, Verhoeven, A J, van Seventer, G, te Velde, A A, Borst, J, Keizer, G D & Figdor, C G 1991, ' Activation of LFA-1 through a Ca2(+)-dependent epitope stimulates lymphocyte adhesion ', Journal of Cell Biology, vol. 112, no. 2, pp. 345-54 ., Journal of Cell Biology, 112(2), 345-54. Rockefeller University Press, Scopus-Elsevier
- Accession number :
- edsair.doi.dedup.....dd2ff09a7392bc2a4fbee83ac673552e