Dependence of T Cell Antigen Recognition on the Dimensions of an Accessory Receptor–Ligand Complex

doi:10.1084/jem.190.1.31

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J. Exp. Med., Volume 190, Number 1, July 5, 1999 31-42
Copyright © 1999 by The Rockefeller University Press.

Dependence of T Cell Antigen Recognition on the Dimensions of an Accessory Receptor–Ligand Complex

Martin K. Wild^a, Anna Cambiaggi^a, Marion H. Brown^a, Elizabeth A. Davies^a, Hiroshi Ohno^b, Takashi Saito^c, and P. Anton van der Merwe^a
^a From the Sir William Dunn School of Pathology, University of Oxford, Oxford OX1 3RE, United Kingdom
^b Division of Molecular Membrane Biology, Cancer Research Institute, Kanazawa University, Kanazawa 920-0934, Japan
^c Department of Molecular Genetics, Chiba University Graduate School of Medicine, Chuo-ku, Chiba 260-8670, Japan

Correspondence to: P. Anton van der Merwe

The T cell antigen receptor (TCR) and its ligand peptide–majorhistocompatibility complex (MHC) are small (~7 nm) comparedwith other abundant cell surface molecules such as integrins,CD43, and CD45 (23–50 nm). We have proposed that moleculesat the T cell/antigen-presenting cell (APC) interface segregateaccording to size, with small "accessory" molecules (e.g., CD2,CD4, CD8, CD28, and CD154) contributing to the formation ofa close-contact zone, within which the TCR engages peptide–MHC,and from which large molecules are excluded (Davis, S.J., andP.A. van der Merwe. 1996. Immunol. Today. 17:177–187).One prediction of this model is that increasing the size ofthese small accessory molecules will disrupt their function.Here, we test this prediction by varying the dimensions of theCD2 ligand, CD48, and examining how this affects T cell antigenrecognition. Although the interaction of CD2 on T cells withwild-type or shortened forms of CD48 on APCs enhances T cellantigen recognition, the interaction of CD2 with elongated formsof CD48 is strongly inhibitory. Further experiments indicatedthat elongation of the CD2/CD48 complex inhibited TCR engagementof peptide–MHC, presumably by preventing the formationof sufficiently intimate contacts at the T cell/APC interface.These findings demonstrate the importance of small size in CD2/CD48function, and support the hypothesis that T cell antigen recognitionrequires segregation of cell surface molecules according tosize.

Key Words: T cell receptor, CD2, CD48, T cell activation, plasma membrane

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