BY55 monoclonal antibody delineates within human cord blood and bone marrow lymphocytes distinct cell subsets mediating cytotoxic activity.

Bensussan, Armand; Gluckman, Éliane; Marsafy, Sanaa El; Schiavon, Valérie; Mansur, Indra Gusti; Dausset, J; Boumsell, Laurence; Carosella, Edgardo D.

doi:10.1073/pnas.91.19.9136

Cited by 47 publications

(23 citation statements)

References 25 publications

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“…This confirms our initial findings obtained by flow cytometry using the anti-CD160 mAb BY55, which demonstrated that BY55-reactive lymphocytes corresponded to NK cells and to cytotoxic CD8 ϩ T lymphocytes in bone marrow, cord, and PB (18,42). Furthermore, we reported that the intestinal intraepithelial lymphocytes, which spontaneously exhibit a cytotoxic activity, are reactive with BY55 mAb (20).…”

Section: Discussionsupporting

confidence: 89%

A Soluble Form of the MHC Class I-Specific CD160 Receptor Is Released from Human Activated NK Lymphocytes and Inhibits Cell-Mediated Cytotoxicity

Giustiniani

Marie‐Cardine

Bensussan

2007

The Journal of Immunology

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CD160 is a GPI-anchored lymphocyte surface receptor in which expression is mostly restricted to the highly cytotoxic CD56dimCD16+ peripheral blood NK subset. We previously reported that MHC class I (MHC-I) molecules bind to CD160 receptors on circulating NK lymphocytes and that this interaction triggers their cytotoxic activity and cytokine production. We also observed that CD160 surface expression on NK cells is down-modulated upon activation with PMA or IL-2. In this study, we further report that short-time incubation of NK lymphocytes with IL-15 converts the membrane-bound CD160 to a soluble form through a proteolytic cleavage involving a metalloprotease. Thus, CD160 is no longer detected at the cell surface, but can be immunoprecipitated from the NK cell culture medium. Interestingly, CD160 transcript remains highly expressed during the process of protein shedding. In addition, we demonstrate that CD160 mRNA synthesis can be induced in CD56bright separated lymphocytes following exposure to IL-15. By producing a Flag-tagged soluble CD160 protein, we establish that its binding to MHC-I molecules results in the inhibition of the cytotoxic CD8+ T lymphocyte activity and of the CD160-mediated NK cell cytotoxicity. Thus, we show that activated NK lymphocytes release a soluble form of CD160 that functionally impairs the MHC-I-specific cytotoxic CD8+ T lymphocyte responsiveness.

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Section: Discussionsupporting

confidence: 89%

A Soluble Form of the MHC Class I-Specific CD160 Receptor Is Released from Human Activated NK Lymphocytes and Inhibits Cell-Mediated Cytotoxicity

Giustiniani

Marie‐Cardine

Bensussan

2007

The Journal of Immunology

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“…Accordingly, Treg cells inhibited the expression of secretion of cytotoxic granules detected by surface expression of CD107 30 (data not shown) and CD160, a marker of circulating highly cytotoxic CD8 ϩ T cells. 31,32 At the same time, the effect of Treg cells on IL-2 expression was not significant in conditions of TCR polyclonal stimulation. Keeping in mind that IL-2 is the predominant cytokine secreted by M CD8 ϩ T cells, in line with their highly proliferative and self-renewing capacity, 5 this result confirmed that Treg cells differentially affect M and E CD8 ϩ T cells.…”

Section: Discussionmentioning

confidence: 63%

Regulatory T cells differentially modulate the maturation and apoptosis of human CD8+ T-cell subsets

Nikolova

Lelièvre

Carrière

et al. 2009

Blood

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“…Further, using the original anti-CD160 mAb BY55 to separate circulating CD160 ϩ NK lymphocytes, we demonstrated that the latter cells corresponded to the effector cytotoxic population (8,9). However, because the BY55 anti-CD160 mAb did not inhibit cytotoxicity of the separated peripheral blood NK (PB-NK) lymphocytes, we were unable to assess whether the structure recognized by BY55 mAb was involved in the target cell recognition (8,9). In the present study, we investigated the function of CD160 expressed on NK cells by using another anti-CD160 mAb, CL1-R2, which inhibits the binding of CD160 receptor to its MHC class I ligands (10).…”

mentioning

confidence: 99%

Engagement of CD160 receptor by HLA-C is a triggering mechanism used by circulating natural killer (NK) cells to mediate cytotoxicity

Bouteiller

Barakonyi

Giustiniani

et al. 2002

Proc. Natl. Acad. Sci. U.S.A.

126

134

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Circulating human natural killer (NK) lymphocytes have been functionally defined by their ability to exert cytotoxic activity against MHC class I-negative target cell lines, including K562. Therefore, it was proposed that NK cells recognized the ''missing self.'' We show here that the Ig-like CD160 receptor expressed by circulating CD56 dim؉ NK cells or IL-2-deprived NK cell lines is mainly involved in their cytotoxic activity against K562 target cells. Further, we report that HLA-C molecules that are constitutively expressed by K562 trigger NK cell lysis through CD160 receptor engagement. In addition, we demonstrate, with recombinant soluble HLA-Cw3 and CD160 proteins, direct interaction of these molecules. We also find that CD158b inhibitory receptors partially interfere with CD160-mediated cytotoxicity, whereas CD94͞ CD159a and CD85j have no effect on engagement with their respective ligands. Thus, CD160͞HLA-C interaction constitutes a unique pathway to trigger NK cell cytotoxic activity.

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BY55 monoclonal antibody delineates within human cord blood and bone marrow lymphocytes distinct cell subsets mediating cytotoxic activity.

Cited by 47 publications

References 25 publications

A Soluble Form of the MHC Class I-Specific CD160 Receptor Is Released from Human Activated NK Lymphocytes and Inhibits Cell-Mediated Cytotoxicity

A Soluble Form of the MHC Class I-Specific CD160 Receptor Is Released from Human Activated NK Lymphocytes and Inhibits Cell-Mediated Cytotoxicity

Regulatory T cells differentially modulate the maturation and apoptosis of human CD8+ T-cell subsets

Engagement of CD160 receptor by HLA-C is a triggering mechanism used by circulating natural killer (NK) cells to mediate cytotoxicity

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