NK resistance of tumor cells from multiple myeloma and chronic lymphocytic leukemia patients: implication of HLA-G

Maki, Guitta; Hayes, Gregory M.; Naji, Abderrahim; Tyler, Timothy; Carosella, Edgardo D.; Rouas‐Freiss, Nathalie; Gregory, Stephanie A.

doi:10.1038/leu.2008.15

Cited by 83 publications

(71 citation statements)

References 45 publications

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“…First, it is conceivable that host immune function may contribute to the control of the disease; for example, B-CLL relapse reflects escape to innate immunity through proper deficit in natural killer (NK) or Tgd cell function, which can be further worsened by treatment. [6][7][8] Second, in the perspective of maintenance therapy with monoclonal antibodies, 9 including rituximab (RTX), it is important to know whether antibody-dependent cellular cytotoxicity (ADCC) capacity of natural effector cells is preserved during the post-FCR period. For this reason, we have measured at different times immune cell counts (NK, CD4, CD8, Tgd), in vitro nonleukemic peripheral blood lymphocyte (PBL) cytotoxicity with or without interleukin (IL)-2, reflecting NK and lymphokine activated killer (LAK) function, respectively, as well as RTX-dependent PBL ADCC against autologous leukemic cells.…”

Section: Introductionmentioning

confidence: 99%

Immune recovery after fludarabine–cyclophosphamide–rituximab treatment in B-chronic lymphocytic leukemia: implication for maintenance immunotherapy

et al. 2010

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Thirty B-cell chronic lymphocytic leukemia patients were treated with fludarabine-cyclophosphamide-rituximab (FCR) and immune cell counts (natural killer (NK) cells, CD4, CD8, Tcd and monocytes) were monitored from the end of treatment (EOT) up to 36 months (M36). Moreover, nonleukemic peripheral blood lymphocyte cytotoxicity (PBL/CTC) as well as rituximab (RTX)-dependent PBL/CTC was also measured at the initiation of therapy, EOT and M12. These parameters were correlated with post-FCR monitoring of the minimal residual disease (MRD) level in blood using a four-color flow cytometry technique. FCR induced a profound and sustained depletion of all T-cell populations, Tcd being the most affected, whereas NK cells were relatively preserved. Both basal and interleukin-2-stimulated nonleukemic PBL/CTC against MEC-2, a CLL cell line, increased during the post-FCR period. There was no correlation between immune recovery parameters and MRD progression profile, except that patients with high post-FCR CD4 þ counts experienced rapid MRD progression. MRD at M12 predicts clinical relapse. The limited data show RTX-mediated LBL/CTC activity against autologous B-cell cells in individuals with o1% residual disease at M12, opening avenues for immunomodulation post-FCR with anti-CD20 antibodies. To conclude, our study suggests that MRD increase at M12 precedes disease evolution post-FCR, and should be assessed as a surrogate marker for proactive management of CLL relapse.

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Section: Introductionmentioning

confidence: 99%

Immune recovery after fludarabine–cyclophosphamide–rituximab treatment in B-chronic lymphocytic leukemia: implication for maintenance immunotherapy

et al. 2010

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“…As shown for B-CLL and ALL, HLA-G may protect the tumor cells by blocking immune effectors, decreasing the absolute T-and NK-cell counts or inducing Treg. For therapeutic intervention, patients with B-cell malignancies would benefit from a blocking of HLA-G functions to restore anti-tumor immunity, as recently demonstrated [7]. For other B-cell malignancies, however, HLA-G expression does not directly correlate with worse prognosis.…”

Section: Discussionmentioning

confidence: 99%

“…Patients having this genotype revealed a reduced overall survival [6]. Here, HLA-G expression correlated with the number of regulatory T-cells (Tregs) [6] and is involved in the protection of B-CLL cells from NK-mediated killing [6,7]. In multiple myeloma (MM) HLA-G expression on malignant plasma cells was also associated with a poor prognosis [8].…”

Section: First Situation: Hla-g Expression Is Related To Worse Prognosismentioning

confidence: 98%

“…There is no data on HLA-G or ILT2 expression by tissue CLL. However, if tissue CLL cells express HLA-G but not ILT2, HLA-G would inhibit T-or NK-cells exactly as evidenced recently [6,7]. In this configuration, the overall effect of HLA-G would indeed impair the anti-tumor response, and a correlation between HLA-G presence and bad prognosis would be observed.…”

Section: Differences In Ilt2 Expression and Function By Tumor Cellsmentioning

confidence: 99%

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A controversy on HLA-G and B-cell malignancies?

Carosella

Rebmann²

2016

J Immunother Appl

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“…Complete remissions in HSCT are achieved through the graft versus leukemia (GvL) effect 5 mediated mainly by NK cells. 6 NK cells utilize sets of "activating" and "inhibitory" receptors to sense various kinds of danger signals. 7,8 The major activating receptors on NK cells include FcgRIIIa (CD16a), NKG2D and the natural cytotoxicity receptors (NCRs) such as NKp30, NKp44 and NKp46.…”

Section: Introductionmentioning

confidence: 99%

Mono- and dual-targeting triplebodies activate natural killer cells and have anti-tumor activityin vitroandin vivoagainst chronic lymphocytic leukemia

et al. 2016

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Chronic lymphocytic leukemia (CLL) is the most common form of leukemia that affects B lymphocytes in adults. Natural killer (NK) cells in CLL patients are intrinsically potent but display poor in situ effector functions. NKG2D is an activating receptor found on NK and CD8 C T cells and plays a role in immunosurveillance of CLL. In this study, we developed mono-and dual-targeting triplebodies utilizing a natural ligand for human NKG2D receptor (ULBP2) to retarget NK cells against tumor cells. Triplebodies in both formats showed better ability to induce NK-cell-dependent killing of target cells compared to bispecific counterparts. A mono-targeting triplebody ULBP2-aCD19-aCD19 successfully triggered NK cell effector functions against CLL cell line MEC1 and primary tumor cells in allogenic and autologous settings. Additionally, a dual-targeting triplebody ULBP2-aCD19-aCD33 specific for two distinct tumor-associated antigens was developed to target antigen loss variants, such as mixed lineage leukemia (MLL). Of note, this triplebody exhibited cytotoxic activity against CD19/CD33 double positive cells and retained its binding features even in the absence of one of the tumor antigens. Further, ULBP2-aCD19-aCD19 showed significant in vivo activity in immune-deficient (NSG) mouse model transplanted with CLL cell line as target cells and human immune cells as an effector population providing a proof-of-principle for this therapeutic concept.

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NK resistance of tumor cells from multiple myeloma and chronic lymphocytic leukemia patients: implication of HLA-G

Cited by 83 publications

References 45 publications

Immune recovery after fludarabine–cyclophosphamide–rituximab treatment in B-chronic lymphocytic leukemia: implication for maintenance immunotherapy

Immune recovery after fludarabine–cyclophosphamide–rituximab treatment in B-chronic lymphocytic leukemia: implication for maintenance immunotherapy

A controversy on HLA-G and B-cell malignancies?

Mono- and dual-targeting triplebodies activate natural killer cells and have anti-tumor activityin vitroandin vivoagainst chronic lymphocytic leukemia

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