Impaired natural killer cell self-education and “missing-self” responses in Ly49-deficient mice

Bélanger, Simon; Tu, Megan M.; Rahim, Mir Munir A.; Mahmoud, Ahmad Bakur; Patel, Rajen; Tai, Lee-Hwa; Troke, Angela D.; Wilhelm, Brian T.; Landry, Josette‐Renée; Zhu, Qinzhang; Tung, Kenneth S. K.; Raulet, David H.; Makrigiannis, Andrew P.

doi:10.1182/blood-2012-02-408732

Cited by 58 publications

(71 citation statements)

References 39 publications

(46 reference statements)

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“…Next, we tested if the maintained missing-self killing of tumor cells after blockade of inhibitory receptors could be extended to other tumor models than RMA/RMA-S. For this purpose, we used the NKT lymphoma cell line C1498, from which an MHC I À variant was recently generated (30). The parental C1498 cells have been shown to be more efficiently rejected upon 5E6 F(ab 0 ) 2 treatment (7).…”

Section: Resultsmentioning

confidence: 99%

“…Alternatively, in the case of transfer experiments, the relative survival of target cells is given as a ratio of MHC I À versus MHC I þ inoculated cells. In vivo killing of C1498 À NKT cell lymphoma cells was performed as described by Belanger and colleagues (30), with small changes. Tumor cells were mixed with NK1.1-depleted, BMQC-labeled (10 mmol/L; Invitrogen Molecular Probes) spleen cells of impaired missing self-recognition (IMSR) mice (32) as a reference cell population, and coinjected i.p.…”

Section: Nk Cell Activitymentioning

confidence: 99%

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Retuning of Mouse NK Cells after Interference with MHC Class I Sensing Adjusts Self-Tolerance but Preserves Anticancer Response

Wagner

Wickström

Tallerico

et al. 2016

Cancer Immunology Research

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Natural killer (NK) cells are most efficient if their targets do not express self MHC class I, because NK cells carry inhibitory receptors that interfere with activating their cytotoxic pathway. Clinicians have taken advantage of this by adoptively transferring haploidentical NK cells into patients to mediate an effective graftversus-leukemia response. With a similar rationale, antibody blockade of MHC class I-specific inhibitory NK cell receptors is currently being tested in clinical trials. Both approaches are challenged by the emerging concept that NK cells may constantly adapt or "tune" their responsiveness according to the amount of self MHC class I that they sense on surrounding cells. Hence, these therapeutic attempts would initially result in increased killing of tumor cells, but a parallel adaptation process might ultimately lead to impaired antitumor efficacy. We have investigated this question in two mouse models: inhibitory receptor blockade in vivo and adoptive transfer to MHC class I-disparate hosts. We show that changed self-perception via inhibitory receptors in mature NK cells reprograms the reactivity such that tolerance to healthy cells is always preserved. However, reactivity against cancer cells lacking critical MHC class I molecules (missing self-reactivity) still remains or may even be increased. This dissociation between activity against healthy cells and tumor cells may provide an answer as to why NK cells mediate graftversus-leukemia effects without causing graft-versus-host disease and may also be utilized to improve immunotherapy.

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Section: Resultsmentioning

confidence: 99%

Section: Nk Cell Activitymentioning

confidence: 99%

Retuning of Mouse NK Cells after Interference with MHC Class I Sensing Adjusts Self-Tolerance but Preserves Anticancer Response

Wagner

Wickström

Tallerico

et al. 2016

Cancer Immunology Research

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“…Paradoxically, NK cell licensing and functional potential depend on the expression of self-MHC-I receptors during development (12,13). In agreement with these education models, the absence of Ly49 expression by NK cells in gene-targeted mice results in lack of self-MHC-I education and the loss of the ability to kill MHC-I-deficient cells (14).…”

mentioning

confidence: 65%

“…We were unable to detect any difference in IFN-g production upon stimulation of Ly49G 129 -positive versus -negative NK cells, although we show in the present study that Ly49G 129 can bind to H-2D b . It is possible that the lack of licensing of Ly49G 129 seen previously is due to H-2D b being a weak self-educator as shown in splenocyte rejection assays using H-2K b2/2 , H-2D b2/2 , or H-2K b2/2 H-2D b2/2 mice as donors (14,29). Furthermore, this hypothesis agrees with the observations that Ly49A can bind to H-2D b when the L chain is of mouse origin (24), but that Ly49A + NK cell subsets in H-2 b background mice produce little if any IFN-g upon stimulation, compared with Ly49A + subsets in H-2 d background mice (30); H-2D d is a strong ligand for Ly49A (31).…”

Section: Discussionmentioning

confidence: 99%

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Optimized Tetramer Analysis Reveals Ly49 Promiscuity for MHC Ligands

McFall

Al-Khattabi

et al. 2013

The Journal of Immunology

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Murine Ly49 receptors, which are expressed mainly on NK and NKT cells, interact with MHC class I (MHC-I) molecules with varying specificity. Differing reports of Ly49/MHC binding affinities may be affected by multiple factors, including cis versus trans competition and species origin of the MHC-I L chain (β2-microglobulin). To determine the contribution of each of these factors, Ly49G, Ly49I, Ly49O, Ly49V, and Ly49Q receptors from the 129 mouse strain were expressed individually on human 293T cells or the mouse cell lines MHC-I–deficient C1498, H-2b–expressing MC57G, and H-2k–expressing L929. The capacity to bind to H-2Db– and H-2Kb–soluble MHC-I tetramers containing either human or murine β2-microglobulin L chains was tested for all five Ly49 receptors in all four cell lines. We found that most of these five inhibitory Ly49 receptors show binding for one or both self–MHC-I molecules in soluble tetramer binding assays when three conditions are fulfilled: 1) lack of competing cis interactions, 2) tetramer L chain is of mouse origin, and 3) Ly49 is expressed in mouse and not human cell lines. Furthermore, Ly49Q, the single known MHC-I receptor on plasmacytoid dendritic cells, was shown to bind H-2Db in addition to H-2Kb when the above conditions were met, suggesting that Ly49Q functions as a pan–MHC-Ia receptor on plasmacytoid dendritic cells. In this study, we have optimized the parameters for soluble tetramer binding analyses to enhance future Ly49 ligand identification and to better evaluate specific contributions by different Ly49/MHC-I pairs to NK cell education and function.

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Natural killer cells in inflammatory autoimmune diseases

et al. 2021

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Natural killer (NK) cells are a specialised population of innate lymphoid cells (ILCs) that help control local immune responses. Through natural cytotoxicity, production of cytokines and chemokines, and migratory capacity, NK cells play a vital immunoregulatory role in the initiation and chronicity of inflammatory and autoimmune responses. Our understanding of their functional differences and contributions in disease settings is evolving owing to new genetic and functional murine proof‐of‐concept studies. Here, we summarise current understanding of NK cells in several classic autoimmune disorders, particularly in rheumatoid arthritis (RA), multiple sclerosis (MS), systemic lupus erythematosus (SLE) and type 1 diabetes mellitus (T1DM), but also less understood diseases such as idiopathic inflammatory myopathies (IIMs). A better understanding of how NK cells contribute to these autoimmune disorders may pave the way for NK cell‐targeted therapeutics.

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Impaired natural killer cell self-education and “missing-self” responses in Ly49-deficient mice

Cited by 58 publications

References 39 publications

Retuning of Mouse NK Cells after Interference with MHC Class I Sensing Adjusts Self-Tolerance but Preserves Anticancer Response

Retuning of Mouse NK Cells after Interference with MHC Class I Sensing Adjusts Self-Tolerance but Preserves Anticancer Response

Optimized Tetramer Analysis Reveals Ly49 Promiscuity for MHC Ligands

Natural killer cells in inflammatory autoimmune diseases

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