Immunogenic capacity of macrophage hybridomas

Tzehoval, Esther; Dagan, Shlomo; Eisenbach, Lea; Atsmon, Jacob; Feldman, Michaël

doi:10.1002/eji.1830190115

Cited by 1 publication

(1 citation statement)

References 40 publications

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“…Similarly, these mAb suppress anti-CD3 mAb-induced Tcell activation in a monocyte-dependent manner [ 101. Furthermore, IFN-yinduced elevation in class I Ag expression on MQ hybridoma cells augments their Ag presentation capacity [29]. Therefore, class I Ag on M@ (or APC) play an important role in Ag presentation.…”

Section: Introductory Remarksmentioning

confidence: 99%

Involvement of major histocompatibility complex class I antigens in T cell activation

et al. 1990

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During the last few years ample evidence has been collected indicating a regulatory role for major histocompatibility complex class I antigens (Ag) in T cell activation. However, due to differential effects (stimulatory and inhibitory) of anti-class I antibodies (Ab) observed under different conditions, no coherent scheme of the mechanism of action of these Ag has emerged. Here, we present evidence that the mode of action of anti-class I Ab depends upon the presence or absence of monocytes/macrophages (M phi) in the culture. The Ab inhibit Ag presentation by binding to M phi. Coating of tetanus toxin -pulsed M phi with anti-class I Ab is sufficient to suppress T cell activation. On the contrary, these Ab enhance lectin- as well as phorbol ester-induced T cell activation in the absence of M phi. Cross-linking of class I Ag on T cell surface mobilizes cytoplasmic Ca2+, and also enhances the CD3-induced Ca2+ flux inside the cells indicating a functional relationship between CD3 and class I Ag. Though surface modulation and immunoprecipitation experiments do not indicate any physical association between these two types of molecules on the T cell surface, capping studies show that cross-linking of class I Ag induces an association of these Ag with CD3. Binding of anti-CD3 Ab enhances the strength of association between CD3 and class I Ag, and the former co-caps completely with the latter. Based on these observations we propose that during antigen presentation M phi (or Ag-presenting cells) and T cells, besides interacting via peptide--class II Ag/CD3--T cell receptor complex formation, also interact through class I Ag. The latter interaction may stabilize the contact formation between T cells and Ag-presenting cell and support T cell activation.

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Section: Introductory Remarksmentioning

confidence: 99%