CD45 isoform transitions on multinegative human thymocytes differentiating in vitro mimic patterns predicted for selective events in vivo
- 1 August 1993
- journal article
- Published by Wiley in Immunology & Cell Biology
- Vol. 71 (4) , 289-301
- https://doi.org/10.1038/icb.1993.34
Abstract
Experiments were designed to test the idea that the patterns of CD45 isoform expressed by differentiating human multinegative (MN) thymocytes (CD3- 4- 8- 19- )are regulated by the type of growth or activation stimuli delivered. We have proposed that within the thymus, CD45RA expression is fundamental to maintenance of the thymic generative lineage while a transition to CD45RO indicates entry into the path of intrathymic death. It seems likely that the signal transduction pathways leading to positive selection are different from those leading to negative selection. Upon culture, MN thymocytes proliferate in response to interleukin-2 (IL-2) or anti-CD2/28 and differentiate as defined by acquisition of CD3 as well as CD4 and/or CD8. Even at day 9 of culture, 30–40% of cells remain multinegative. DNA analysis indicates that both CD3- and CD3+ cells are actively cycling. Although the CD3- set includes a substantial number of cycling cells, it continues to express almost exclusively the CD45RA isoform. Among CD3+ progeny, 53–80% have acquired CD45RO while maintaining high expression of CD45RA, although 10–47% are able to maintain exclusive expression of CD45PA despite their more differentiated state. In contrast, stimulation with PHA/PMA, which gives a vigorous proliferative response, appears to inhibit acquisition of CD3 and thus differentiation, while forcing a premature transition from CD45RA to CD45RO. These in vitro systems appear to permit generative thymic development while maintaining a cycling multinegative subset, thus mimicking thymic development in vivo, permitting an exploration of the events in positive and negative selection of human thymocytes. The maintenance of CD45RA expression with co-expression of CD45RO by CD3+ progeny in cultures supplemented with IL-2 or anti-CD2/28, in contrast to the loss of CD45RA after PHA stimulation, shows that the regulation of CD45 isoform expression is closely linked to the nature of the developmental signals received by a thymocyte.Keywords
This publication has 21 references indexed in Scilit:
- Activation signals regulate heat shock transcription factor 1 in human B lymphocytesJournal of Cellular Physiology, 1997
- CD45 isoform switching precedes the activation-driven death of human thymocytes by apoptosisInternational Immunology, 1991
- Glycosylation of CD45: carbohydrate composition and its role in acquisition of CD45RO and CD45RB T cell maturation‐related antigen specificities during biosynthesisEuropean Journal of Immunology, 1990
- Cell generation within human thymic subsets defined by selective expression of CD45 (T200) isoformsHuman Immunology, 1990
- Transition in CD45 isoform expression during differentiation of normal and abnormal B cellsInternational Immunology, 1989
- The Leukocyte Common Antigen FamilyAnnual Review of Immunology, 1989
- Definition of the thymic generative lineage by selective expression of high molecular weight isoforms of CD45 (T200)European Journal of Immunology, 1989
- CD4+ CD8+ cells are rare among in vitro activated mouse or human T lymphocytesCellular Immunology, 1988
- A novel activation pathway for mature thymocytes. Costimulation of CD2 (T,p50) and CD28 (T,p44) induces autocrine interleukin 2/interleukin 2 receptor-mediated cell proliferation.The Journal of Experimental Medicine, 1988
- Triggering CD 28 molecules synergize with CD 2 (T11.1 and T11,2)‐mediated T cell activationEuropean Journal of Immunology, 1988