Abstract:
:T cell clones are useful models for studying lymphocyte function both at the level of the individual cell and in interacting systems. Murine cytolytic and non- cytolyic T cell clones have been obtained with relative ease, and the particular procedure used to derive and maintain T cell clones may influence profoundly the characteristics of the resulting cells. The method of choice depends on the specific question to be asked. Although some clones have characteristics that would have been expected on the basis of results observed with bulk cell populations, other clones have rather unexpected properties. Although most T cell clones appear to be either cytolytic or non-cytolytic, this distinction is not always absolute. A high proportion of both cytolytic and non-cytolytic T cell clones have dual reactivity. This is true for cells which by other criteria appear to be true clones. The frequency of such cells is high enough to suggest that most if not all T cells may have reactivity for more than one antigenic determinant or that antigenic determinants recognized by T cells are shared widely and unexpectedly. It is not clear whether one or two different antigen receptors account for such dual reactivity. The nature of the T cell receptor for antigen remains obscure. T cell clones, because of their homogeneous nature, should make it easier to answer these important immunological questions. Although it remains to be determined how many distinct molecules account for the numerous biological activities found in the culture supernatants from antigen-stimulated T cell clones, it is clear that these factors influence several different types of cells that are involved directly and indirectly in immune responses. IL-2 stimulates both cytolytic and non-cytolytic T cells to proliferate. BCSF causes polyclonal activation of B cells, and there may be other factors which influence B cell responses to antigenic stimulation. IL-3 apparently stimulates maturation of immature T cells. CSF stimulates production of macrophages from precursor cells found in the bone marrow. Supernatants also stimulate expression of Ia antigens by macrophages, and antigen-presenting cells have been found to bear Ia antigens. Interferon augments natural killer cell activity. Thus, regardless of how many molecules are involved in these effects, activated non-cytolytic T cells appear to be involved in a variety of ways in the modulation of immune responses.(ABSTRACT TRUNCATED AT 400 WORDS)
journal_name
Adv Exp Med Bioljournal_title
Advances in experimental medicine and biologyauthors
Fitch FWdoi
10.1007/978-1-4615-9376-8_20subject
Has Abstractpub_date
1984-01-01 00:00:00pages
347-63eissn
0065-2598issn
2214-8019journal_volume
172pub_type
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