Your search keyword '"Capuano, Cristina"' showing total 4 results

1. KLRG1 is reduced on NK cells in SLE patients, inversely correlates with disease activity and is modulated by hydroxychloroquine in vitro.

Author

Novelli, Lucia, Barbati, Cristiana, Capuano, Cristina, Recalchi, Serena, Ceccarelli, Fulvia, Vomero, Marta, Alessandri, Cristiano, Morrone, Stefania, and Conti, Fabrizio

Subjects

SYSTEMIC lupus erythematosus, KILLER cells, MONONUCLEAR leukocytes, KILLER cell receptors, HYDROXYCHLOROQUINE, T cells

Abstract

Objectives: Killer cell lectin-like receptor G 1 (KLRG1), a transmembrane receptor with inhibitory capacity expressed in human immune cells, emerged as a novel susceptibility gene for systemic lupus erythematosus (SLE). The aim of this study was to investigate the expression of KLRG1 in SLE patients compared to healthy controls (HC) on both NK and T cells and to evaluate its possible involvement in SLE pathogenesis. Methods: Eighteen SLE patients and twelve healthy controls were enrolled. Peripheral blood mononuclear cells (PBMCs) from these patients were phenotypically characterized by immunofluorescence and flow cytometry. The effect of the hydroxychloroquine (HCQ) in vitro on KLRG1 expression and its signaling mediated functions in NK cells were analyzed. Results: KLRG1 expression was significantly reduced on the analyzed immune cell populations in SLE patients compared to HC, especially on total NK cells. Moreover, expression of KLRG1 on total NK cells inversely correlated with the SLEDAI-2K. A direct association between KLRG1 expression on NK cells and patients' treatment with HCQ was observed. In vitro treatment with HCQ increased KLRG1 expression on NK cells. In HC, KLRG1+ NK cells showed reduced degranulation and IFNγ production, while in SLE patient, this inhibition occurred only for the IFNγ production. Conclusion: With this study we revealed a reduced expression and an impaired function of KLRG1 on NK cells in SLE patients. These results suggest a possible role of KLRG1 in the pathogenesis of SLE and as a novel biomarker of this disease. [ABSTRACT FROM AUTHOR]

Published

2023

2. Editorial: Modulation of antibody-mediated effector functions in natural killer cells: protective and detrimental effects in infectious diseases.

Author

Galandrini, Ricciarda, Sachiyo Yoshio, and Capuano, Cristina

Subjects

KILLER cells, IMMUNE response, COMMUNICABLE diseases, EXPERIMENTAL medicine, MEDICAL sciences

Abstract

This article, titled "Editorial: Modulation of antibody-mediated effector functions in natural killer cells: protective and detrimental effects in infectious diseases," discusses the role of natural killer (NK) cells in antibody-mediated immune responses to viral infections. The authors explore the balance between protective and harmful effects of NK cell-mediated antibody functions, particularly in the context of severe respiratory viral infections such as influenza, COVID-19, and respiratory syncytial virus disease. The article also examines the impact of COVID-19 vaccination on NK cell effector functions and discusses the mechanisms by which modified antibodies, such as afucosylated monoclonal antibodies, enhance NK cell-mediated killing of infected cells. Overall, the article provides insights into the complex interactions between antibodies, NK cells, and viral infections, highlighting the potential for both beneficial and detrimental effects. [Extracted from the article]

Published

2024

3. c-Cbl regulates MICA- but not ULBP2-induced NKG2D down-modulation in human NK cells.

Author

Molfetta, Rosa, Quatrini, Linda, Capuano, Cristina, Gasparrini, Francesca, Zitti, Beatrice, Zingoni, Alessandra, Galandrini, Ricciarda, Santoni, Angela, and Paolini, Rossella

Abstract

The NKG2D activating receptor on human NK cells mediates 'altered self' recognition, as its ligands (NKG2DLs) are upregulated on target cells in a variety of stress conditions. Evidence collected in the past years shows that, even though expression of NKG2DLs acts as a danger signal that renders tumor cells susceptible to cytotoxicity, chronic exposure to soluble or membrane-bound NKG2DLs can lead to down-modulation of receptor expression and impairment of NKG2D-mediated cell functions. Here, we evaluated whether different cell-bound NKG2DLs, namely MICA and ULBP2, are equivalently able to induce NKG2D down-modulation on human NK cells. We found that although both ligands reduce NKG2D surface expression, MICA promotes a stronger receptor down-modulation than ULBP2, leading to a severe impairment of NKG2D-dependent NK-cell cytotoxicity. We also provide evidence that the ubiquitin pathway and c-Cbl direct MICA-induced but not ULBP2-induced NKG2D internalization and degradation, thus identifying a molecular mechanism to explain the differential effects of MICA and ULBP2 on NKG2D expression. A better understanding of the molecular mechanisms employed by the different NKG2DLs to control NKG2D surface expression could be useful for the development of anti-tumor strategies to restore a normal level of NKG2D receptors on human NK cells. [ABSTRACT FROM AUTHOR]

Published

2014

4. Obinutuzumab-mediated high-affinity ligation of FcγRIIIA/CD16 primes NK cells for IFNγ production.

Author

Capuano, Cristina, Pighi, Chiara, Molfetta, Rosa, Paolini, Rossella, Battella, Simone, Palmieri, Gabriella, Giannini, Giuseppe, Belardinilli, Francesca, Santoni, Angela, and Galandrini, Ricciarda

Subjects

*KILLER cells, *INTERLEUKIN-18, *IMMUNE response

Abstract

Natural killer (NK) cell-mediated antibody-dependent cellular cytotoxicity (ADCC), based on the recognition of IgG-opsonized targets by the low-affinity receptor for IgG FcγRIIIA/CD16, represents one of the main mechanisms by which therapeutic antibodies (mAbs) mediate their antitumor effects. Besides ADCC, CD16 ligation also results in cytokine production, in particular, NK-derived IFNγ is endowed with a well-recognized role in the shaping of adaptive immune responses. Obinutuzumab is a glycoengineered anti-CD20 mAb with a modified crystallizable fragment (Fc) domain designed to increase the affinity for CD16 and consequently the killing of mAb-opsonized targets. However, the impact of CD16 ligation in optimized affinity conditions on NK functional program is not completely understood. Herein, we demonstrate that the interaction of NK cells with obinutuzumab-opsonized cells results in enhanced IFNγ production as compared with parental non-glycoengineered mAb or the reference molecule rituximab. We observed that affinity ligation conditions strictly correlate with the ability to induce CD16 down-modulation and lysosomal targeting of receptor-associated signaling elements. Indeed, a preferential degradation of FcϵRIγ chain and Syk kinase was observed upon obinutuzumab stimulation independently from CD16-V158F polymorphism. Although the downregulation of FcϵRIγ/Syk module leads to the impairment of cytotoxic function induced by NKp46 and NKp30 receptors, obinutuzumab-experienced cells exhibit an increased ability to produce IFNγ in response to different stimuli. These data highlight a relationship between CD16 aggregation conditions and the ability to promote a degradative pathway of CD16-coupled signaling elements associated to the shift of NK functional program. [ABSTRACT FROM AUTHOR]

Published

2017