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      NKG2A Expression Is Not per se Detrimental for the Anti-Multiple Myeloma Activity of Activated Natural Killer Cells in an In Vitro System Mimicking the Tumor Microenvironment

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          Abstract

          Natural killer (NK) cell-based immunotherapy is a promising therapy for cancer patients. Inhibitory killer immunoglobulin-like receptors (KIRs) and NKG2A are required for NK cell licensing, but can also inhibit NK cell effector function. Upon reconstitution in a stem cell transplantation setting or after ex vivo NK expansion with IL-2, NKG2A is expressed on a large percentage of NK cells. Since the functional consequences of NKG2A co-expression for activated NK cells are not well known, we compared NKG2A+ vs NKG2A− NK cell subsets in response to K562 cells, multiple myeloma (MM) cell lines and primary MM cells. NK cells were isolated from healthy donors (HLA-C1+C2+Bw4+) and activated overnight with 1,000 U/ml IL-2. NK cell degranulation in subsets expressing KIRs and/or NKG2A was assessed at 21 or 0.6% O 2. Activated NKG2A+ NK cell subsets degranulated more vigorously than NKG2A− subsets both at 21 and 0.6% O 2. This was irrespective of the presence of KIR and occurred in response to HLA-deficient K562 cells as well as HLA competent, lowly expressing HLA-E MM cell lines. In response to primary MM cells, no inhibitory effects of NKG2A were observed, and NKG2A blockade did not enhance degranulation of NKG2A+ subsets. KIR− NK cells expressing NKG2A degranulated less than their NKG2A− counterparts in response to MM cells having high levels of peptide-induced membrane HLA-E, suggesting that high surface HLA-E levels are required for NKG2A to inhibit activated NK cells. Addition of daratumumab, an anti-CD38 to trigger antibody-dependent cell-mediated cytotoxicity, improved the anti-MM response for all subsets and degranulation of the KIR−NKG2A− “unlicensed” subset was comparable to KIR+ or NKG2A+ licensed subsets. This demonstrates that with potent activation, all subsets can contribute to tumor clearance. Additionally, subsets expressing KIRs mismatched with the HLA ligands on the target cell had the highest level of activation in response to MM cell lines as well as against primary MM. Our current study demonstrated that if NK cells are sufficiently activated, e.g., via cytokine or antibody activation, the (co-)expression of NKG2A receptor may not necessarily be a disadvantage for NK cell-based therapy.

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          Targeting natural killer cells and natural killer T cells in cancer.

          Eric Vivier, Sophie Ugolini, Didier Blaise (2012)
          Natural killer (NK) cells and natural killer T (NKT) cells are subsets of lymphocytes that share some phenotypical and functional similarities. Both cell types can rapidly respond to the presence of tumour cells and participate in antitumour immune responses. This has prompted interest in the development of innovative cancer therapies that are based on the manipulation of NK and NKT cells. Recent studies have highlighted how the immune reactivity of NK and NKT cells is shaped by the environment in which they develop. The rational use of these cells in cancer immunotherapies awaits a better understanding of their effector functions, migratory patterns and survival properties in humans.
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            Expression patterns of NKG2A, KIR, and CD57 define a process of CD56dim NK-cell differentiation uncoupled from NK-cell education.

            Niklas Björkström, Peggy Riese, Frank Heuts (2010)
            Natural killer (NK) cells are lymphocytes of the innate immune system that, following differentiation from CD56(bright) to CD56(dim) cells, have been thought to retain fixed functional and phenotypic properties throughout their lifespan. In contrast to this notion, we here show that CD56(dim) NK cells continue to differentiate. During this process, they lose expression of NKG2A, sequentially acquire inhibitory killer cell inhibitory immunoglobulin-like receptors and CD57, change their expression patterns of homing molecules, and display a gradual decline in proliferative capacity. All cellular intermediates of this process are represented in varying proportions at steady state and appear, over time, during the reconstitution of the immune system, as demonstrated in humanized mice and in patients undergoing hematopoietic stem cell transplantation. CD56(dim) NK-cell differentiation, and the associated functional imprint, occurs independently of NK-cell education by interactions with self-human leukocyte antigen class I ligands and is an essential part of the formation of human NK-cell repertoires.
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              Human breast cancer cells enhance self tolerance by promoting evasion from NK cell antitumor immunity.

              Emilie Mamessier, Aude Sylvain, Marie-Laure Thibult (2011)
              NK cells are a major component of the antitumor immune response and are involved in controlling tumor progression and metastases in animal models. Here, we show that dysfunction of these cells accompanies human breast tumor progression. We characterized human peripheral blood NK (p-NK) cells and malignant mammary tumor-infiltrating NK (Ti-NK) cells from patients with noninvasive and invasive breast cancers. NK cells isolated from the peripheral blood of healthy donors and normal breast tissue were used as controls. With disease progression, we found that expression of activating NK cell receptors (such as NKp30, NKG2D, DNAM-1, and CD16) decreased while expression of inhibitory receptors (such as NKG2A) increased and that this correlated with decreased NK cell function, most notably cytotoxicity. Importantly, Ti-NK cells had more pronounced impairment of their cytotoxic potential than p-NK cells. We also identified several stroma-derived factors, including TGF-β1, involved in tumor-induced reduction of normal NK cell function. Our data therefore show that breast tumor progression involves NK cell dysfunction and that breast tumors model their environment to evade NK cell antitumor immunity. This highlights the importance of developing future therapies able to restore NK cell cytotoxicity to limit/prevent tumor escape from antitumor immunity.
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                Author and article information

                Contributors
                Niken M. Mahaweni: URI : https://frontiersin.org/people/u/535484
                Femke A. I. Ehlers: URI : https://frontiersin.org/people/u/551678
                Marcel G. J. Tilanus: URI : https://frontiersin.org/people/u/33090
                Gerard M. J. Bos: URI : https://frontiersin.org/people/u/576079
                Lotte Wieten: URI : https://frontiersin.org/people/u/45824
                Journal
                Journal ID (nlm-ta): Front Immunol
                Journal ID (iso-abbrev): Front Immunol
                Journal ID (publisher-id): Front. Immunol.
                Title: Frontiers in Immunology
                Publisher: Frontiers Media S.A.
                ISSN (Electronic): 1664-3224
                Publication date (Electronic): 22 June 2018
                Publication date Collection: 2018
                Volume: 9
                Electronic Location Identifier: 1415
                Affiliations
                [1] 1Division of Hematology, Department of Internal Medicine, Maastricht University Medical Center+ , Maastricht, Netherlands
                [2] 2GROW School for Oncology and Developmental Biology, Maastricht University , Maastricht, Netherlands
                [3] 3Department of Transplantation Immunology, Tissue Typing Laboratory, Maastricht University Medical Center+ , Maastricht, Netherlands
                [4] 4Department of Clinical Genetics, Maastricht University Medical Center+ , Maastricht, Netherlands
                Author notes

                Edited by: Kate Stringaris, National Institutes of Health (NIH), United States

                Reviewed by: Raynier Devillier, Institut Paoli-Calmettes (IPC), France; Julie Tabiasco, Institut National de la Santé et de la Recherche Médicale (INSERM), France

                *Correspondence: Lotte Wieten, l.wieten@ 123456mumc.nl

                Specialty section: This article was submitted to Cancer Immunity and Immunotherapy, a section of the journal Frontiers in Immunology

                Article
                DOI: 10.3389/fimmu.2018.01415
                PMC ID: 6023990
                PubMed ID: 29988376
                SO-VID: 03be9e5a-0e2e-47e5-af44-9157425abb19
                Copyright © Copyright © 2018 Mahaweni, Ehlers, Sarkar, Janssen, Tilanus, Bos and Wieten.
                License:

                This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

                History
                Date received : 08 March 2018
                Date accepted : 06 June 2018
                Page count
                Figures: 6, Tables: 0, Equations: 0, References: 31, Pages: 12, Words: 7837
                Categories
                Subject: Immunology
                Subject: Original Research

                ScienceOpen disciplines: Immunology
                Keywords: natural killer cell,nkg2a,killer immunoglobulin-like receptor,hla-e,multiple myeloma,tumor microenvironment
                Data availability:
                ScienceOpen disciplines: Immunology
                Keywords: natural killer cell, nkg2a, killer immunoglobulin-like receptor, hla-e, multiple myeloma, tumor microenvironment

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