Literature DB >> 17339436

The activating NKG2D ligand MHC class I-related chain A transfers from target cells to NK cells in a manner that allows functional consequences.

Fiona E McCann1, Philipp Eissmann, Björn Onfelt, Rufina Leung, Daniel M Davis.   

Abstract

Recently, it has become apparent that surface proteins commonly transfer between immune cells in contact. Inhibitory receptors and ligands exchange between cells during NK cell surveillance and we report here that NK cells also acquire activating ligands from target cells. Specifically, the stress-inducible activating ligand for NKG2D, MHC class I-related chain A (MICA), transferred to NK cells upon conjugation with MICA-expressing target cells. Acquisition of MICA from target cells was dependent on cell contact and occurred after accumulation of MICA at the immunological synapse. Moreover, transfer of MICA was facilitated by specific molecular recognition via NKG2D and augmented by Src kinase signaling. Importantly, MICA associated with its new host NK cell membrane in an orientation that allowed engagement with NKG2D in trans and indeed could down-regulate NKG2D in subsequent homotypic interactions with other NK cells. MICA captured from target cells could subsequently transfer between NK cells and, more importantly, NK cell degranulation was triggered in such NK cell-NK cell interactions. Thus, NK cells can influence other NK cells with proteins acquired from target cells and our data specifically suggest that NK cells could lyse other NK cells upon recognition of activating ligands acquired from target cells. This mechanism could constitute an important function for immunoregulation of NK cell activity.

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Year:  2007        PMID: 17339436     DOI: 10.4049/jimmunol.178.6.3418

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


  32 in total

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Journal:  J Virol       Date:  2008-02-20       Impact factor: 5.103

3.  Trogocytosis in allogeneic transplants: donor cells take on the recipients identity.

Authors:  Ian M Rogers
Journal:  Chimerism       Date:  2013-10-11

4.  Capture of plasma membrane fragments from target cells by trogocytosis requires signaling in T cells but not in B cells.

Authors:  Anne Aucher; Eddy Magdeleine; Etienne Joly; Denis Hudrisier
Journal:  Blood       Date:  2008-04-01       Impact factor: 22.113

5.  Transfer of the human NKG2D ligands UL16 binding proteins (ULBP) 1-3 is related to lytic granule release and leads to ligand retransfer and killing of ULBP-recipient natural killer cells.

Authors:  Sheila López-Cobo; Gema Romera-Cárdenas; Eva M García-Cuesta; Hugh T Reyburn; Mar Valés-Gómez
Journal:  Immunology       Date:  2015-06-25       Impact factor: 7.397

6.  Acquisition of activation receptor ligand by trogocytosis renders NK cells hyporesponsive.

Authors:  Cathrine A Miner; Tusar K Giri; Claire E Meyer; Mark Shabsovich; Sandeep K Tripathy
Journal:  J Immunol       Date:  2015-01-12       Impact factor: 5.422

7.  The HLA-G cycle provides for both NK tolerance and immunity at the maternal-fetal interface.

Authors:  Tamara Tilburgs; J Henry Evans; Ângela C Crespo; Jack L Strominger
Journal:  Proc Natl Acad Sci U S A       Date:  2015-10-12       Impact factor: 11.205

Review 8.  Formation and function of the lytic NK-cell immunological synapse.

Authors:  Jordan S Orange
Journal:  Nat Rev Immunol       Date:  2008-09       Impact factor: 53.106

9.  Tumour-experienced T cells promote NK cell activity through trogocytosis of NKG2D and NKp46 ligands.

Authors:  Carolina I Domaica; Mercedes B Fuertes; Lucas E Rossi; María V Girart; Damián E Avila; Gabriel A Rabinovich; Norberto W Zwirner
Journal:  EMBO Rep       Date:  2009-06-05       Impact factor: 8.807

10.  Natural killer cell signal integration balances synapse symmetry and migration.

Authors:  Fiona J Culley; Matthew Johnson; J Henry Evans; Sunil Kumar; Rupert Crilly; Juan Casasbuenas; Tim Schnyder; Maryam Mehrabi; Mahendra P Deonarain; Dmitry S Ushakov; Veronique Braud; Günter Roth; Roland Brock; Karsten Köhler; Daniel M Davis
Journal:  PLoS Biol       Date:  2009-07-28       Impact factor: 8.029

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