Anti-CD3 monoclonal antibodies (mAbs) are potent immunosuppressive agents used in clinical transplantation. However, the activation-related adverse side effects associated with these mAbs have prompted the development of less toxic nonmitogenic anti-CD3 mAb therapies. At present, the functional and biochemical consequences of T cell exposure to nonmitogenic anti-CD3 is unclear. In this study, we have examined the early signaling events triggered by a nonmitogenic anti-CD3 mAb. Like the mitogenic anti-CD3 mAb, nonmitogenic anti-CD3 triggered changes in the T cell receptor (TCR) complex, including ζ chain tyrosine phosphorylation and ZAP-70 association. However, unlike the mitogenic anti-CD3 stimulation, nonmitogenic anti-CD3 was ineffective at inducing the highly phosphorylated form of ζ (p23) and tyrosine phosphorylation of the associated ZAP-70 tyrosine kinase. This proximal signaling deficiency correlated with minimal phospholipase Cγ-1 phosphorylation and failure to mobilize detectable Ca2+. Not only did biochemical signals delivered by nonmitogenic anti-CD3 resemble altered peptide ligand signaling, but exposure of Th1 clones to nonmitogenic anti-CD3 also resulted in functional anergy. Finally, a bispecific anti-CD3 × anti-CD4 F(ab)′2 reconstituted early signal transduction events and induced proliferation, suggesting that defective association of lck with the TCR complex may underlie the observed signaling differences between the mitogenic and nonmitogenic anti-CD3.
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21 April 1997
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April 21 1997
Nonmitogenic Anti-CD3 Monoclonal Antibodies Deliver a Partial T Cell Receptor Signal and Induce Clonal Anergy
Judith A. Smith,
Judith A. Smith
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
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J. Yun Tso,
J. Yun Tso
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
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Marcus R. Clark,
Marcus R. Clark
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
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Michael S. Cole,
Michael S. Cole
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
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Jeffrey A. Bluestone
Jeffrey A. Bluestone
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
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Judith A. Smith
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
J. Yun Tso
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
Marcus R. Clark
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
Michael S. Cole
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
Jeffrey A. Bluestone
From the *Ben May Institute for Cancer Research, Committee on Immunology, Department of Pathology; §Department of Medicine, University of Chicago, Illinois 60637; and ‡Protein Design Laboratories, Mountain View, California 94043
Address correspondence to Dr. Jeffrey A. Bluestone, Committee on Immunology, 5841 S. Maryland Avenue, MC 1089, Chicago, IL 60637.
1Abbreviations used in this paper: APL, altered peptide ligands; IP3, inositol– triphosphate; PCC, pigeon cytochrome C; PLCγ-1, phospholipase Cγ-1.
Received:
October 24 1996
Revision Received:
February 04 1997
Online ISSN: 1540-9538
Print ISSN: 0022-1007
1997
J Exp Med (1997) 185 (8): 1413–1422.
Article history
Received:
October 24 1996
Revision Received:
February 04 1997
Citation
Judith A. Smith, J. Yun Tso, Marcus R. Clark, Michael S. Cole, Jeffrey A. Bluestone; Nonmitogenic Anti-CD3 Monoclonal Antibodies Deliver a Partial T Cell Receptor Signal and Induce Clonal Anergy. J Exp Med 21 April 1997; 185 (8): 1413–1422. doi: https://doi.org/10.1084/jem.185.8.1413
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