Literature DB >> 16709826

Clustering class I MHC modulates sensitivity of T cell recognition.

David R Fooksman1, Gigi Kwik Grönvall, Qing Tang, Michael Edidin.   

Abstract

T cell recognition of peptide-MHC is highly specific and is sensitive to very low levels of agonist peptide; however, it is unclear how this effect is achieved or regulated. In this study we show that clustering class I MHC molecules on the cell surface of B lymphoblasts enhances their recognition by mouse and human T cells. We increased clustering of MHC I molecules by two methods, cholesterol depletion and direct cross-linking of a dimerizable MHC construct. Imaging showed that both treatments increased the size and intensity of MHC clusters on the cell surface. Enlarged clusters correlated with enhanced lysis and T cell effector function. Enhancements were peptide-specific and greatest at low concentrations of peptide. Clustering MHC class I enhanced recognition of both strong and weak agonists but not null peptide. Our results indicate that the lateral organization of MHC class I on the cell surface can modulate the sensitivity of T cell recognition of agonist peptide.

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Year:  2006        PMID: 16709826      PMCID: PMC1524854          DOI: 10.4049/jimmunol.176.11.6673

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  29 in total

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Authors:  Y Sykulev; M Joo; I Vturina; T J Tsomides; H N Eisen
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Authors:  Y Sykulev; A Brunmark; T J Tsomides; S Kageyama; M Jackson; P A Peterson; H N Eisen
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8.  Modification of membrane cholesterol level affects expression and clustering of class I HLA molecules at the surface of JY human lymphoblasts.

Authors:  A Bodnár; A Jenei; L Bene; S Damjanovich; J Matkó
Journal:  Immunol Lett       Date:  1996-12       Impact factor: 3.685

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Authors:  J Matko; Y Bushkin; T Wei; M Edidin
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Authors:  R D Salter; P Cresswell
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  30 in total

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3.  Engineering macrophages to control the inflammatory response and angiogenesis.

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