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2. Identification of CD160-TM as a tumor target on triple negative breast cancers: possible therapeutic applications.

Author

Scheffges, Claire, Devy, Jérôme, Giustiniani, Jérôme, Francois, Stessy, Cartier, Lucille, Merrouche, Yacine, Foussat, Arnaud, Potteaux, Stéphane, Bensussan, Armand, and Marie-Cardine, Anne

Subjects
HORMONE receptor positive breast cancer, TRIPLE-negative breast cancer, ANTIBODY-dependent cell cytotoxicity, CELLULAR recognition, KILLER cells
Abstract

Background: Despite major therapeutic advances, triple-negative breast cancer (TNBC) still presents a worth prognosis than hormone receptors-positive breast cancers. One major issue relies in the molecular and mutational heterogeneity of TNBC subtypes that is reinforced by the absence of reliable tumor-antigen that could serve as a specific target to further promote efficient tumor cell recognition and depletion. CD160 is a receptor mainly expressed by NK lymphocytes and presenting two isoforms, namely the GPI-anchored form (CD160-GPI) and the transmembrane isoform (CD160-TM). While CD160-GPI is constitutively expressed on resting cells and involved in the generation of NK cells' cytotoxic activity, CD160-TM is neo-synthesized upon activation and promotes the amplification of NK cells' killing ability. Methods: CD160 expression was assessed by immunohistochemistry (IHC) and flow cytometry on TNBC patient biopsies or cell lines, respectively. Antibody (Ab)-mediated tumor depletion was tested in vitro by performing antibody-dependent cell cytotoxicity (ADCC) and phagocytosis (ADCP) assays, and in vivo on a TNBC mouse model. Results: Preliminary data obtained by IHC on TNBC patients' tumor biopsies revealed an unconventional expression of CD160 by TNBC tumor cells. By using a specific but conformation-dependent anti-CD160-TM Ab, we established that CD160-TM, but not CD160-GPI, was expressed by TNBC tumor cells. A conformation-independent anti-CD160-TM mAb (22B12; muIgG2a isotype) was generated and selected according to pre-defined specificity and functional criterions. In vitro functional assays demonstrated that ADCC and ADCP could be induced in the presence of 22B12, resulting in TNBC cell line apoptosis. The ability of 22B12 to exert an in vivo anti-tumor activity was also demonstrated on a TNBC murine model. Conclusions: Our data identify CD160-TM as a tumor marker for TNBC and provide a rational for the use of anti-CD160-TM antibodies as therapeutic tools in this tumor context. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Syndrome de Sézary.

Author

de Masson, Adèle, Moins-Teisserenc, Hélène, Ram-Wolff, Caroline, Giustiniani, Jérôme, Bagot, Martine, Battistella, Maxime, and Bensussan, Armand

Abstract

Copyright of Hematologie is the property of John Libbey Eurotext Ltd. and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2024
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4. The HLA-B*57:01 allele corresponds to a very large MHC haploblock likely explaining its massive effect for HIV-1 elite control.

Author

Rahmouni, Myriam, De Marco, Lorenzo, Spadoni, Jean-Louis, Tison, Maxime, Medina-Santos, Raissa, Labib, Taoufik, Noirel, Josselin, Tamouza, Ryad, Limou, Sophie, Delaneau, Olivier, Fellay, Jacques, Bensussan, Armand, Le Clerc, Sigrid, McLaren, Paul J., and Zagury, Jean-François

Subjects
SINGLE nucleotide polymorphisms, GENE expression, ALLELES, HIV, GENOME-wide association studies
Abstract

Introduction: We have reanalyzed the genomic data of the International Collaboration for the Genomics of HIV (ICGH), centering on HIV-1 Elite Controllers. Methods: We performed a genome-wide Association Study comparing 543 HIV Elite Controllers with 3,272 uninfected controls of European descent. Using the latest database for imputation, we analyzed 35,552 Single Nucleotide Polymorphisms (SNPs) within the Major Histocompatibility Complex (MHC) region. Results: Our analysis identified 2,626 SNPs significantly associated (p<5. 10-8) with elite control of HIV-1 infection, including well-established MHC signals such as the rs2395029-G allele which tags HLA-B*57:01. A thorough investigation of SNPs in linkage disequilibrium with rs2395029 revealed an extensive haploblock spanning 1.9 megabases in the MHC region tagging HLA-B*57:01, comprising 379 SNP alleles impacting 72 genes. This haploblock contains damaging variations in proteins like NOTCH4 and DXO and is also associated with a strong differential pattern of expression of multiple MHC genes such as HLA-B, MICB, and ZBTB12. The study was expanded to include two cohorts of seropositive African-American individuals, where a haploblock tagging the HLA-B*57:03 allele was similarly associated with control of viral load. The mRNA expression profile of this haploblock in African Americans closely mirrored that in the European cohort. Discussion: These findings suggest that additional molecular mechanisms beyond the conventional antigen-presenting role of class I HLA molecules may contribute to the observed influence of HLA-B*57:01/B*57:03 alleles on HIV-1 elite control. Overall, this study has uncovered a large haploblock associated with HLA-B*57 alleles, providing novel insights into their massive effect on HIV-1 elite control. [ABSTRACT FROM AUTHOR]

Published
2023
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5. Fc receptors act as innate immune receptors during infection?

Author

Laassili, Chaimaa, El Hend, Fatiha Ben, Benzidane, Riad, Oumeslakht, Loubna, Aziz, Abdel-Ilah, El Fatimy, Rachid, Bensussan, Armand, and Mkaddem, Sanae Ben

Subjects
FC receptors, COMPLEMENT activation, NATURAL immunity, BACTERIAL diseases, PHAGOCYTOSIS
Abstract

Innate immunity constitutes the first nonspecific immunological line of defense against infection. In this response, a variety of mechanisms are activated: the complement system, phagocytosis, and the inflammatory response. Then, adaptive immunity is activated. Major opsonization mediators during infections are immunoglobulins (Igs), the function of which is mediated through Fc receptors (FcRs). However, in addition to their role in adaptive immunity, FcRs have been shown to play a role in innate immunity by interacting directly with bacteria in the absence of their natural ligands (Igs). Additionally, it has been hypothesized that during the early phase of bacterial infection, FcRs play a protective role via innate immune functions mediated through direct recognition of bacteria, and as the infection progresses to later phases, FcRs exhibit their established function as receptors in adaptive immunity. This review provides detailed insight into the potential role of FcRs as innate immune mediators of the host defense against bacterial infection independent of opsonins. [ABSTRACT FROM AUTHOR]

Published
2023
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6. Derivation and Preclinical Characterization of CYT-303, a Novel NKp46-NK Cell Engager Targeting GPC3.

Author

Arulanandam, Antonio, Lin, Liang, Chang, Hao-Ming, Cerutti, Martine, Choblet, Sylvie, Gao, Peng, Rath, Armin, Bensussan, Armand, Kadouche, Jean, Teper, Daniel, Mandelboim, Ofer, and Li, Wei

Subjects
KILLER cells, CARCINOEMBRYONIC antigen, SERIAL murders, KRA, INTRAVENOUS therapy
Abstract

Glypican-3 (GPC3) is an oncofetal antigen that is highly expressed in multiple solid tumors, including hepatocellular carcinoma, and is barely expressed in adult normal tissues except the placenta. NKp46 activation receptor is expressed in all-natural killer (NK) cells, including tumor-infiltrating NK cells. FLEX-NKTM is a platform for the production of tetravalent multifunctional antibody NK cell engagers (NKE). CYT-303 was designed using the FLEX-NK scaffold, incorporating a novel humanized NKp46 binder that does not induce NKp46 internalization and a humanized GPC3 binder that targets the membrane-proximal lobe to mediate NK cell-redirected killing of HCC tumors. CYT-303 shows sub-nanomolar binding affinities to both GPC3 and NKp46. CYT-303 was highly potent and effective in mediating NK cell-redirected cytotoxicity against multiple HCC tumor cell lines and tumor spheroids. More interestingly, it can reverse the dysfunction induced in NK cells following repeated rounds of serial killing of tumors. It also mediated antibody-dependent cellular phagocytosis (ADCP) and complement-dependent cytotoxicity against GPC3-expressing HCC tumors. In vivo, CYT-303 showed no toxicity or cytokine release in cynomolgus monkeys up to the highest dose (60 mg/kg), administered weekly by intravenous infusion for 28 days. These results demonstrate the potential of CYT-303 to be a safe and effective therapy against HCC. [ABSTRACT FROM AUTHOR]

Published
2023
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8. CD160 receptor in CLL: Current state and future avenues.

Author

Oumeslakht, Loubna, Aziz, Abdel-ilah, Bensussan, Armand, and Ben Mkaddem, Sanae

Subjects
CHRONIC leukemia, CHRONIC lymphocytic leukemia, MEMBRANE glycoproteins, B cells, PROGNOSIS, DISEASE relapse
Abstract

CD160 is a glycosylphosphatidylinositol (GPI)-anchored cell surface glycoprotein expressed on cytotoxic natural killer (NK) cells and T-cell subsets. It plays a crucial role in the activation of NK-cell cytotoxicity and cytokine production. It also modulates the immune system and is involved in some pathologies, such as cancer. CD160 is abnormally expressed in B-cell chronic lymphocytic leukemia (CLL) but not expressed in normal B lymphocytes. Its expression in CLL enhances tumor cell proliferation and resistance to apoptosis. CD160 is also a potential prognostic marker for the detection of minimal residual disease (MRD) in CLL, which is important for the clinical management of CLL, the prevention of disease relapse, and the achievement of complete remission. In this review, we present an overview of CD160 and its involvement in the pathophysiology of CLL. We also discuss its use as a prognostic marker for the assessment of MRD in CLL. [ABSTRACT FROM AUTHOR]

Published
2022
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9. The soluble form of CD160 acts as a tumor mediator of immune escape in melanoma.

Author

Gauci, Marie-Léa, Giustiniani, Jérôme, Lepelletier, Clémence, Garbar, Christian, Thonnart, Nicolas, Dumaz, Nicolas, Foussat, Arnaud, Lebbé, Céleste, Bensussan, Armand, and Marie-Cardine, Anne

Subjects
MELANOMA, KILLER cells, CANCER invasiveness, TUMOR microenvironment, TUMORS, UVEA cancer, GRANZYMES, SKIN cancer
Abstract

Melanoma is responsible for 90% of skin cancer-related deaths. Major therapeutic advances have led to a considerable improvement in the prognosis of patients, with the development of targeted therapies (BRAF or MEK inhibitors) and immunotherapy (anti-CTLA-4 or -PD-1 antibodies). However, the tumor constitutes an immunosuppressive microenvironment that prevents the therapeutic efficacy and/or promotes the development of secondary resistances. CD160 is an activating NK-cell receptor initially described as delineating the NK and CD8+T-cell cytotoxic populations. Three forms of CD160 have been described: (1) the GPI isoform, constitutively expressed and involved in the initiation of NK-cells' cytotoxic activity, (2) the transmembrane isoform, neo-synthesized upon cell activation, allowing the amplification of NK cells' cytotoxic functions and (3) the soluble form, generated after cleavage of the GPI isoform, which presents an immuno-suppressive activity. By performing immunohistochemistry analyses, we observed a strong expression of CD160 at the primary cutaneous tumor site of melanoma patients. We further demonstrated that melanoma cells express CD160-GPI isoform and constitutively release the soluble form (sCD160) into the tumor environment. sCD160 was shown to inhibit the cytotoxic activity of NK-cells towards their target cells. In addition, it was found in the serum of melanoma patients and associated with increased tumor dissemination. Altogether these results support a role for sCD160 in the mechanisms leading to the inhibition of anti-tumor response and immune surveillance in melanoma. [ABSTRACT FROM AUTHOR]

Published
2022
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10. Validation of AAC-11-Derived Peptide Anti-Tumor Activity in a Single Graft Sézary Patient-Derived Xenograft Mouse Model.

Author

Habault, Justine, Thonnart, Nicolas, Ram-Wolff, Caroline, Bagot, Martine, Bensussan, Armand, Poyet, Jean-Luc, and Marie-Cardine, Anne

Subjects
PEPTIDES, ANTINEOPLASTIC agents, LABORATORY mice, SEZARY syndrome, T cells
Abstract

Sézary syndrome (SS) is an aggressive cutaneous T cell lymphoma with poor prognosis mainly characterized by the expansion of a tumor CD4+ T cell clone in both skin and blood. So far, the development of new therapeutic strategies has been hindered by a lack of reproducible in vivo models closely reflecting patients' clinical features. We developed an SS murine model consisting of the intravenous injection of Sézary patients' PBMC, together with a mixture of interleukins, in NOD-SCID-gamma mice. Thirty-four to fifty days after injection, mice showed skin disorders similar to that observed in patients, with the detection of epidermis thickening and dermal tumor T cell infiltrates. Although experimental variability was observed, Sézary cells could be tracked in the blood stream, confirming that our model could efficiently exhibit both skin and blood involvement. Using this model, we evaluated the therapeutic potential of RT39, a cell-penetrating peptide derived from the survival protein anti-apoptosis clone 11 (AAC-11), that we previously characterized as specifically inducing apoptosis of Sézary patients' malignant clone ex vivo. Systemic administration of RT39 led to cutaneous tumor T cells depletion, demonstrating efficient malignant cells' targeting and a favorable safety profile. These preclinical data confirmed that RT39 might be an innovative therapeutic tool for Sézary syndrome. [ABSTRACT FROM AUTHOR]

Published
2022
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11. The NFAT3/RERG Complex in Luminal Breast Cancers Is Required to Inhibit Cell Invasion and May Be Correlated With an Absence of Axillary Lymph Nodes Colonization.

Author

Coillard, Lucie, Guaddachi, Frédéric, Ralu, Maëlle, Brabencova, Eva, Garbar, Christian, Bensussan, Armand, Le Bras, Morgane, Lehmann-Che, Jacqueline, and Jauliac, Sébastien

Subjects
TRIPLE-negative breast cancer, LYMPH nodes, BREAST cancer, CANCER relapse, RAS proteins, TUMOR markers, ESTROGEN
Abstract

Luminal breast cancers represent 70% of newly diagnosed breast cancers per annum and have a relatively good prognosis compared with triple-negative breast cancers. Luminal tumors that are responsive to hormonal therapy are particularly associated with a favorable prognosis. Nonetheless, the absolute number of metastatic relapses in luminal cancers is larger than in triple-negative breast cancers. A better understanding of the biology of luminal cancers, control of metastases formation, and identification of predictive markers of their evolution are therefore still necessary. In this context, we previously disclosed the key role of NFAT3 in regulating luminal breast cancer invasion. We have now identified a specific inhibitory region, in the C-terminal part of NFAT3, required for the inhibition of invasion of the human luminal breast cancer cell line T-47D. Indeed, we showed that this 85 amino acid C-terminal region acts as a dominant negative form of NFAT3 and that its overexpression in the T-47D cell line led to increased cell invasion. Mechanistically, we have revealed that this region of NFAT3 interacts with the small Ras GTPase RERG (RAS like estrogen regulated growth inhibitor) and shown that RERG expression is required for NFAT3 to impede T-47D cell invasion. We have validated the association of NFAT3 with RERG in human luminal breast cancer tissues. We have shown an increase of the quantity of the NFAT3/RERG complexes in patients without axillary lymph node colonization and therefore proposed that the detection of this complex may be a non-invasive marker of axillary lymph node colonization. [ABSTRACT FROM AUTHOR]

Published
2022
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12. The NFAT3/RERG Complex in Luminal Breast Cancers Is Required to Inhibit Cell Invasion and May Be Correlated With an Absence of Axillary Lymph Nodes Colonization.

Author

Coillard, Lucie, Guaddachi, Frédéric, Ralu, Maëlle, Brabencova, Eva, Garbar, Christian, Bensussan, Armand, Le Bras, Morgane, Lehmann-Che, Jacqueline, and Jauliac, Sébastien

Subjects
TRIPLE-negative breast cancer, LYMPH nodes, BREAST cancer, CANCER relapse, RAS proteins, TUMOR markers, ESTROGEN
Abstract

Luminal breast cancers represent 70% of newly diagnosed breast cancers per annum and have a relatively good prognosis compared with triple-negative breast cancers. Luminal tumors that are responsive to hormonal therapy are particularly associated with a favorable prognosis. Nonetheless, the absolute number of metastatic relapses in luminal cancers is larger than in triple-negative breast cancers. A better understanding of the biology of luminal cancers, control of metastases formation, and identification of predictive markers of their evolution are therefore still necessary. In this context, we previously disclosed the key role of NFAT3 in regulating luminal breast cancer invasion. We have now identified a specific inhibitory region, in the C-terminal part of NFAT3, required for the inhibition of invasion of the human luminal breast cancer cell line T-47D. Indeed, we showed that this 85 amino acid C-terminal region acts as a dominant negative form of NFAT3 and that its overexpression in the T-47D cell line led to increased cell invasion. Mechanistically, we have revealed that this region of NFAT3 interacts with the small Ras GTPase RERG (RAS like estrogen regulated growth inhibitor) and shown that RERG expression is required for NFAT3 to impede T-47D cell invasion. We have validated the association of NFAT3 with RERG in human luminal breast cancer tissues. We have shown an increase of the quantity of the NFAT3/REG complexes in patients without axillary lymph node colonization and therefore proposed that the detection of this complex may be a non-invasive marker of axillary lymph node colonization. [ABSTRACT FROM AUTHOR]

Published
2022
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13. Cutaneous Wound Healing: A Review about Innate Immune Response and Current Therapeutic Applications.

Author

Adib, Yara, Bensussan, Armand, and Michel, Laurence

Subjects
WOUND healing, SKIN injuries, IMMUNE response, CELL populations, IMMUNE system
Abstract

Skin wounds and compromised wound healing are major concerns for the public. Although skin wound healing has been studied for decades, the molecular and cellular mechanisms behind the process are still not completely clear. The systemic responses to trauma involve the body's inflammatory and immunomodulatory cellular and humoral networks. Studies over the years provided essential insights into a complex and dynamic immunity during the cutaneous wound healing process. This review will focus on innate cell populations involved in the initial phase of this orchestrated process, including innate cells from both the skin and the immune system. [ABSTRACT FROM AUTHOR]

Published
2022
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15. Persistent deficiency of mucosal-associated invariant T cells during dermatomyositis.

Author

Cassius, Charles, Branchtein, Mylene, Battistella, Maxime, Amode, Reyhan, Lepelletier, Clémence, Jachiet, Marie, Masson, Adèle de, Frumholtz, Laure, Chasset, François, Amoura, Zahir, Mathian, Alexis, Samri, Assia, Monfort, Jean-Benoit, Bachmeyer, Claude, Bengoufa, Djaouida, Cordoliani, Florence, Bagot, Martine, Bensussan, Armand, Bouaziz, Jean-David, and Buanec, Hélène Le

Subjects
ATOPIC dermatitis, COMPARATIVE studies, DERMATOMYOSITIS, FLOW cytometry, IMMUNITY, PSORIASIS, T cells, PHENOTYPES, CYTOTOXINS
Abstract

Objectives Mucosal-associated invariant T (MAIT) cells are innate-like lymphocytes that are important for antibacterial immunity and may have regulatory roles. MAIT cells are decreased during SLE. However, their frequencies and phenotype have not been investigated in DM. We studied MAIT cell frequencies and phenotype in DM patients with active and inactive disease (after treatment). Methods Peripheral blood flow cytometry analysis of MAIT cells was compared between DM (n  = 22), SLE (n  = 10), psoriasis (n  = 7) and atopic dermatitis (n  = 5) patients, and healthy controls (n  = 19). Results A dramatic decrease of circulating MAIT cell frequency was observed in active DM and SLE patients compared with healthy controls and other inflammatory skin diseases [active DM: median = 0.25% (interquartile range 0.19–0.6%), P  < 0.0001; active SLE: median = 0.61 (0.55–0.77), P  < 0.0001 vs healthy controls: 2.32% (1.18–4.45%)]. MAIT cells from active DM patients had an abnormal phenotype including increased expression of CD25 and cytotoxic T-lymphocyte-associated protein 4 that correlated with their low frequency in the blood. Conclusion In DM, peripheral blood MAIT cells are dramatically reduced and have an activated/exhausted phenotype that may be linked to increased activation-induced cell death. [ABSTRACT FROM AUTHOR]

Published
2020
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16. In vivo anti-MUC1+ tumor activity and sequences of high-affinity anti-MUC1-SEA antibodies.

Author

Pichinuk, Edward, Chalik, Michael, Benhar, Itai, Ginat-Koton, Ravit, Ziv, Ravit, Smorodinsky, Nechama I., Haran, Gabi, Garbar, Christian, Bensussan, Armand, Meeker, Alan, Guillaume, Thierry, Rubinstein, Daniel B., and Wreschner, Daniel H.

Subjects
IMMUNOGLOBULINS, MONOCLONAL antibodies, IMMUNOSTAINING, CANCER cells, PROSTATE cancer, LOBULAR carcinoma, PANCREATIC cancer
Abstract

Cleavage of the MUC1 glycoprotein yields two subunits, an extracellular alpha-subunit bound to a smaller transmembrane beta-subunit. Monoclonal antibodies (mAbs) directed against the MUC1 alpha–beta junction comprising the SEA domain, a stable cell-surface moiety, were generated. Sequencing of all seven anti-SEA domain mAbs showed that they clustered into four groups and sequences of all groups are presented here. mAb DMB5F3 with picomolar affinity for the MUC1 SEA target was selected for further evaluation. Immunohistochemical staining of a series of malignancies with DMB5F3 including lung, prostate, breast, colon, and pancreatic carcinomas revealed qualitative and qualitative differences between MUC1 expression on normal versus malignant cells: DMB5F3 strongly stained malignant cells in a near-circumferential pattern, whereas MUC1 in normal pancreatic and breast tissue showed only weak apical positivity of ductal/acinar cells. Humanized chimeric DMB5F3 linked to ZZ-PE38 (ZZ IgG-binding protein fused to Pseudomonas exotoxin) induced vigorous cytotoxicity of MUC1+ malignant cells in vitro. The intensity of cell killing correlated with the level of MUC1 expression by the target cell, suggesting a MUC1 expression threshold for cell killing. MUC1+ Colo357 pancreatic cancer cells xenotransplanted into nude and SCID mice models were treated with the chDMB5F3:ZZ-PE38 immunocomplex. In both transplant models, chDMB5F3:ZZ-PE38 exhibited significant in vivo anti-tumor activity, suppressing up to 90% of tumor volume in the SCID model compared with concomitant controls. The efficacy of chDMB5F3:ZZ-PE38 immunotoxin in mediating tumor killing both in vitro and in vivo strongly suggests a clinical role for anti-MUC1 SEA antibody in the treatment of MUC1-expressing malignancies. [ABSTRACT FROM AUTHOR]

Published
2020
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19. Microenvironment tailors nTreg structure and function.

Author

Schiavon, Valérie, Duchez, Sophie, Branchtein, Mylène, How-Kit, Alexandre, Cassius, Charles, Daunay, Antoine, Shen, Yimin, Dubanchet, Sylvie, Colisson, Renaud, Vanneaux, Valérie, Pruvost, Alain, Roucairol, Camille, Setterblad, Niclas, Bouaziz, Jean-David, Boissier, Marie-Christophe, Semerano, Luca, Graux, Carlos, Bensussan, Armand, Burny, Arsène, and Gallo, Robert

Subjects
T cells, CELLULAR control mechanisms, CELL physiology, CLINICAL trials, GRAFT versus host disease
Abstract

Natural regulatory T cells (nTregs) ensure the control of self-tolerance and are currently used in clinical trials to alleviate autoimmune diseases and graft-versus-host disease after hematopoietic stem cell transfer. Based on CD39/CD26 markers, blood nTreg analysis revealed the presence of five different cell subsets, each representing a distinct stage of maturation. Ex vivo added microenvironmental factors, including IL-2, TGFβ, and PGE2, direct the conversion from naive precursor to immature memory and finally from immature to mature memory cells, the latest being a no-return stage. Phenotypic and genetic characteristics of the subsets illustrate the structural parental maturation between subsets, which further correlates with the expression of regulatory factors. Regarding nTreg functional plasticity, both maturation stage and microenvironmental cytokines condition nTreg activities, which include blockade of autoreactive immune cells by cell-cell contact, Th17 and IL-10 Tr1-like activities, or activation of TCR-stimulating dendritic cell tolerization. Importantly, blood nTreg CD39/CD26 profile remained constant over a 2-y period in healthy persons but varied from person to person. Preliminary data on patients with autoimmune diseases or acute myelogenous leukemia illustrate the potential use of the nTreg CD39/CD26 profile as a blood biomarker to monitor chronic inflammatory diseases. Finally, we confirmed that naive conventional CD4 T cells, TCR-stimulated under a tolerogenic conditioned medium, could be ex vivo reprogrammed to FOXP3 lineage Tregs, and further found that these cells were exclusively committed to suppressive function under all microenvironmental contexts. [ABSTRACT FROM AUTHOR]

Published
2019
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23. Human Cardiac-Derived Stem/Progenitor Cells Fine-Tune Monocyte-Derived Descendants Activities toward Cardiac Repair.

Author

Dam, Noémie, Hocine, Hocine Rachid, Palacios, Itziar, DelaRosa, Olga, Menta, Ramón, Charron, Dominique, Bensussan, Armand, El Costa, Hicham, Jabrane-Ferrat, Nabila, Dalemans, Wilfried, Lombardo, Eleuterio, and Al-Daccak, Reem

Subjects
HEART diseases, THERAPEUTICS, IMMUNE response, HOMEOSTASIS
Abstract

Cardiac repair following MI relies on a finely regulated immune response involving sequential recruitment of monocytes to the injured tissue. Monocyte-derived cells are also critical for tissue homeostasis and healing process. Our previous findings demonstrated the interaction of T and natural killer cells with allogeneic human cardiac-derived stem/progenitor cells (hCPC) and suggested their beneficial effect in the context of cardiac repair. Therefore, we investigated here whether monocytes and their descendants could be also modulated by allogeneic hCPC toward a repair/anti-inflammatory phenotype. Through experimental in vitro assays, we assessed the impact of allogeneic hCPC on the recruitment, functions and differentiation of monocytes. We found that allogeneic hCPC at steady state or under inflammatory conditions can incite CCL-2/CCR2-dependent recruitment of circulating CD14+CD16- monocytes and fine-tune their activation toward an anti-inflammatory profile. Allogeneic hCPC also promoted CD14+CD16- monocyte polarization into anti-inflammatory/immune-regulatory macrophages with high phagocytic capacity and IL10 secretion. Moreover, hCPC bended the differentiation of CD14+CD16- monocytes to dendritic cells (DCs) toward anti-inflammatory macrophage-like features and impaired their antigen-presenting function in favor of immune-modulation. Collectively, our results demonstrate that allogeneic hCPC could reshape monocytes, macrophages as well as DCs responses by favoring their anti-inflammatory/tolerogenic activation/polarization. Thereby, therapeutic allogeneic hCPC might also contribute to post-infarct myocardial healing by modeling the activities of monocytes and their derived descendants. [ABSTRACT FROM AUTHOR]

Published
2017
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24. Therapeutic Antibodies to KIR3DL2 and Other Target Antigens on Cutaneous T-Cell Lymphomas.

Author

Schmitt, Christian, Marie-Cardine, Anne, and Bensussan, Armand

Subjects
SEZARY syndrome, MYCOSIS fungoides, CUTANEOUS T-cell lymphoma
Abstract

KIR3DL2 is a member of the killer cell immunoglobulin-like receptor (KIR) family that was initially identified at the surface of natural killer (NK) cells. KIR3DL2, also known as CD158k, is expressed as a disulfide-linked homodimer. Each chain is composed of three immunoglobulin-like domains and a long cytoplasmic tail containing two immunoreceptor tyrosine-based inhibitory motifs. Beside its expression on NK cells, it is also found on rare circulating T lymphocytes, mainly CD8+. Although the KIR gene number varies between haplotype, KIR3DL2 is a framework gene present in all individuals. Together with the presence of genomic regulatory sequences unique to KIR3DL2, this suggests some particular functions for the derived protein in comparison with other KIR family members. Several ligands have been identified for KIR3DL2. As for other KIRs, binding to HLA class I molecules is essential for NK development by promoting phenomena such as licensing and driving NK cell maturation. For KIR3DL2, this includes binding to HLA-A3 and -A11 and to the free heavy chain form of HLA-B27. In addition, KIR3DL2 binds to CpG oligonucleotides (ODN) and ensures their transport to endosomal toll-like receptor 9 that promotes cell activation. These characteristics have implicated KIR3DL2 in several pathologies: ankylosing spondylitis and cutaneous T-cell lymphomas such as Sézary syndrome, CD30+ cutaneous lymphoma, and transformed mycosis fungoides. Consequently, a new generation of humanized monoclonal antibodies (mAbs) directed against KIR3DL2 has been helpful in the diagnosis, follow-up, and treatment of these diseases. In addition, preliminary clinical studies of a novel targeted immunotherapy for cutaneous T-cell lymphomas using the anti-KIR3DL2 mAb IPH4102 are now underway. In this review, we discuss the various aspects of KIR3DL2 on the functions of CD4+ T cells and how targeting this receptor helps to develop innovative therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published
2017
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25. Dermatopulmonary Syndrome Associated With Anti-MDA5 Antibodies After Allogeneic Hematopoietic Stem Cell Transplantation.

Author

Lepelletier, Clémence, Bengoufa, Djaouida, Lyes, Zeltni, de Masson, Adèle, Chasset, François, Jachiet, Marie, Michonneau, David, Robin, Marie, Peffault de Latour, Régis, Sicre de Fontbrune, Flore, Tandjaoui-Lambiotte, Yacine, Bensussan, Armand, Rybojad, Michel, Tazi, Abdellatif, Bagot, Martine, Socié, Gérard, Bergeron, Anne, and Bouaziz, Jean-David

Published
2017
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26. Increased expression of PD1 and CD39 on CD3+CD4+ skin T cells in the elderly.

Author

Zuelgaray, Elina, Boccara, David, Ly Ka So, Sophie, Boismal, Françoise, Mimoun, Maurice, Bagot, Martine, Bensussan, Armand, Bouaziz, Jean‐David, and Michel, Laurence

Subjects
SKIN, HUMAN phenotype, DISEASE susceptibility, INNATE lymphoid cells, COMMUNICABLE diseases
Abstract

Normal ageing is associated with an impaired systemic immune response contributing to an increased susceptibility to infectious diseases. The aim of this study was to compare the lymphocyte phenotype in human skin from old and young healthy subjects. Skin samples from donors were used for explant cultures before flow cytometric analysis. Our results depicted a higher proportion of CD4+ and a lower proportion of CD8+ among CD3+ T cells, a decreased proportion of CD45RA+ naive T cells (3.5 ± 1.9% vs 22.9 ± 11.1%, P ≤ 0.007) and an upregulation of the expression of CD39 and PD1 on CD3+CD4+ T cells (25.1 ± 8.5% vs 12.5 ± 8.5%, P ≤ 0.003, 68.8 ± 11.6% vs 50.0 ± 11.3%, P ≤ 0.01, respectively) in the skin of old subjects. These findings could explain a reduced generation of long‐lived memory T cells and an impaired antitumoral response in the skin of the elderly. [ABSTRACT FROM AUTHOR]

Published
2019
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27. Intrinsically aged dermal fibroblasts fail to differentiate into adipogenic lineage.

Author

Brun, Cécilia, Ly Ka So, Sophie, Maginiot, François, Bensussan, Armand, Michel, Laurence, Larghero, Jérôme, Wong, Hélène, Oddos, Thierry, and Cras, Audrey

Subjects
CONNECTIVE tissue cells, FIBROBLASTS, ADIPOSE tissues
Abstract

A letter to the editor is presented discussing adipose tissues and the regeneration of adult tissues as well as their self-renewal and differentiation potential.

Published
2016
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28. MUC1-ARF—A Novel MUC1 Protein That Resides in the Nucleus and Is Expressed by Alternate Reading Frame Translation of MUC1 mRNA.

Author

Chalick, Michael, Jacobi, Oded, Pichinuk, Edward, Garbar, Christian, Bensussan, Armand, Meeker, Alan, Ziv, Ravit, Zehavi, Tania, Smorodinsky, Nechama I., Hilkens, John, Hanisch, Franz-Georg, Rubinstein, Daniel B., and Wreschner, Daniel H.

Subjects
MUCINS, PROTEIN expression, MESSENGER RNA, GENETIC code, MEMBRANE proteins
Abstract

Translation of mRNA in alternate reading frames (ARF) is a naturally occurring process heretofore underappreciated as a generator of protein diversity. The MUC1 gene encodes MUC1-TM, a signal-transducing trans-membrane protein highly expressed in human malignancies. Here we show that an AUG codon downstream to the MUC1-TM initiation codon initiates an alternate reading frame thereby generating a novel protein, MUC1-ARF. MUC1-ARF, like its MUC1-TM 'parent’ protein, contains a tandem repeat (VNTR) domain. However, the amino acid sequence of the MUC1-ARF tandem repeat as well as N- and C- sequences flanking it differ entirely from those of MUC1-TM. In vitro protein synthesis assays and extensive immunohistochemical as well as western blot analyses with MUC1-ARF specific monoclonal antibodies confirmed MUC1-ARF expression. Rather than being expressed at the cell membrane like MUC1-TM, immunostaining showed that MUC1-ARF protein localizes mainly in the nucleus: Immunohistochemical analyses of MUC1-expressing tissues demonstrated MUC1-ARF expression in the nuclei of secretory luminal epithelial cells. MUC1-ARF expression varies in different malignancies. While the malignant epithelial cells of pancreatic cancer show limited expression, in breast cancer tissue MUC1-ARF demonstrates strong nuclear expression. Proinflammatory cytokines upregulate expression of MUC1-ARF protein and co-immunoprecipitation analyses demonstrate association of MUC1-ARF with SH3 domain-containing proteins. Mass spectrometry performed on proteins coprecipitating with MUC1-ARF demonstrated Glucose-6-phosphate 1-dehydrogenase (G6PD) and Dynamin 2 (DNM2). These studies not only reveal that the MUC1 gene generates a previously unidentified MUC1-ARF protein, they also show that just like its ‘parent’ MUC1-TM protein, MUC1-ARF is apparently linked to signaling and malignancy, yet a definitive link to these processes and the roles it plays awaits a precise identification of its molecular functions. Comprising at least 524 amino acids, MUC1-ARF is, furthermore, the longest ARF protein heretofore described. [ABSTRACT FROM AUTHOR]

Published
2016
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29. Targeting the Tumor Microenvironment: The Protumor Effects of IL-17 Related to Cancer Type.

Author

Fabre, Joseph, Giustiniani, Jerome, Garbar, Christian, Antonicelli, Frank, Merrouche, Yacine, Bensussan, Armand, Bagot, Martine, and al-Dacak, Reem

Subjects
TUMOR microenvironment, INTERLEUKIN-17, CANCER immunotherapy, EXTRACELLULAR matrix, CARCINOGENESIS, HETERODIMERS
Abstract

The inflammatory process contributes to immune tolerance as well as to tumor progression and metastasis. By releasing extracellular signals, cancerous cells constantly shape their surrounding microenvironment through their interactions with infiltrating immune cells, stromal cells and components of extracellular matrix. Recently, the pro-inflammatory interleukin 17 (IL-17)-producing T helper lymphocytes, the Th17 cells, and the IL-17/IL-17 receptor (IL-17R) axis gained special attention. The IL-17 family comprises at least six members, IL-17A, IL-17B, IL-17C, IL-17D, IL-17E (also called IL-25), and IL-17F. Secreted as disulfide-linked homo- or heterodimers, the IL-17 bind to the IL-17R, a type I cell surface receptor, of which there are five variants, IL-17RA to IL-17RE. This review focuses on the current advances identifying the promoting role of IL-17 in carcinogenesis, tumor metastasis and resistance to chemotherapy of diverse solid cancers. While underscoring the IL-17/IL-17R axis as promising immunotherapeutic target in the context of cancer managing, this knowledge calls upon further in vitro and in vivo studies that would allow the development and implementation of novel strategies to combat tumors. [ABSTRACT FROM AUTHOR]

Published
2016
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30. The Uterine Immune Profile May Help Women With Repeated Unexplained Embryo Implantation Failure After In Vitro Fertilization.

Author

Petitbarat, Marie, Chevrier, Lucie, Vezmar, Katia, Lédée, Nathalie, Rahmati, Mona, Dubanchet, Sylvie, Gahéry, Hanne, Bensussan, Armand, Chaouat, Gerard, and Vitoux, Dominique

Subjects
BIRTH rate, ENDOMETRIUM physiology, IMMUNOLOGY, FERTILIZATION in vitro, UTERINE diseases
Abstract

Labeled problem Embryo implantation remains the main limiting factor in assisted reproductive medicine (20% success rate). Methods of study An endometrial immune profiling was performed among 394 women with the previous history of repeated embryo implantation failures (RIF). The endometrial immune profile documented the ratio of IL-15/Fn-14 mRNA as a biomarker of uNK cell activation/maturation (together with the uNK cell count) and the IL-18/TWEAK mRNA ratio as a biomarker of both angiogenesis and the Th1/Th2 balance. According to their profile, we recommended personalized care to counteract the documented dysregulation and assessed its effects by the live birth rate (LBR) for the next embryo transfer. Results Endometrial immune profiles appeared to be dysregulated in 81.7% of the RIF patients compared to control. Overactivation was diagnosed in 56.6% and low activation in 25%. The LBR among these dysregulated/treated patients at the first subsequent embryo transfer was 39.8%. Conclusion Endometrial immune profiling may improve our understanding of RIF and subsequent LBR if treated. [ABSTRACT FROM AUTHOR]

Published
2016
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32. PARKIN Inactivation Links Parkinson's Disease to Melanoma.

Author

Hui-Han Hu, Kannengiesser, Caroline, Lesage, Suzanne, André, Jocelyne, Mourah, Samia, Michel, Laurence, Descamps, Vincent, Basset-Seguin, Nicole, Bagot, Martine, Bensussan, Armand, Lebbé, Céleste, Deschamps, Lydia, Saiag, Philippe, Leccia, Marie-Thérèse, Bressac-de-Paillerets, Brigitte, Tsalamlal, Amel, Kumar, Rajiv, Klebe, Stephan, Grandchamp, Bernard, and Andrieu-Abadie, Nathalie

Subjects
PROTEIN metabolism, DNA analysis, ENZYME metabolism, CELL lines, CELL physiology, ENZYMES, EPITHELIAL cells, GENES, GENETICS, MELANOMA, GENETIC mutation, PARKINSON'S disease, PROTEINS, SKIN tumors, WESTERN immunoblotting, RELATIVE medical risk, CASE-control method, SEQUENCE analysis, ODDS ratio, GENOTYPES
Abstract

Background: Melanoma incidence is higher in patients affected by Parkinson's disease (PD) and vice versa, but the genetic link shared by both diseases is unknown. As PARK2 is both a tumor suppressor gene and frequently mutated in young onset PD, we evaluated the role of PARK2 in melanoma predisposition and progression.Methods: An in-depth PARK2 gene dosage analysis and sequencing was performed on 512 French case patients and 562 healthy control patients, as well as sporadic tumors and melanoma cell lines. The frequency of genetic alterations was compared between case patients and control patients using two-sided Fisher's exact tests and odds ratio (OR) calculations. We used western blotting to determine PARKIN expression in melanocytes and melanoma cell lines and transfection followed by clonogenic assays to evaluate the effect of PARKIN expression on cellular proliferation. All statistical tests were two-sided.Results: Germline PARK2 mutations (including copy number variations, splicing, and putative deleterious missense mutations) were present in 25 case patients but only four control patients (OR = 3.95, 95% confidence interval = 1.34 to 15.75). Copy number variations (CNVs) and loss of heterozygosity were present in 60% and 74%, respectively, of primary tumors. PARKIN protein was expressed in melanocytes but not in most melanoma cell lines, and its expression decreased following melanocyte transformation by oncogenic NRAS. Re-expression of PARKIN in melanoma cell lines resulted in a drastic reduction of cell proliferation and inhibition of PARKIN in melanocytes stimulated their proliferation.Conclusion: Our results show an important role for PARK2 as a tumor suppressor both in melanoma predisposition and progression, which could explain the epidemiological association of these diseases. [ABSTRACT FROM AUTHOR]

Published
2016
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33. Phenotypic and functional changes in dermal primary fibroblasts isolated from intrinsically aged human skin.

Author

Brun, Cécilia, Jean‐Louis, Francette, Oddos, Thierry, Bagot, Martine, Bensussan, Armand, and Michel, Laurence

Subjects
FIBROBLASTS, DESMOID tumors, ARTIFICIAL skin, PELAGE, TOUCH
Abstract

Dermal fibroblasts play a key role in maintaining skin homoeostasis by synthesizing and degrading extracellular matrix components. During ageing, they are subjected to changes, such as the loss of type I collagen expression and an increased synthesis of metalloproteinase I, leading to fragmentation of collagen fibrils with consequent reduction of the mechanical tension and defects of skin wound healing. Most information about fibroblast ageing was obtained from experiments performed on replicative-senescent dermal fibroblasts in vitro. However, the senescence status of fibroblasts isolated from intrinsically aged skins and its consequences on functionality need to be deeper investigated. Herein, we studied age-related phenotypic and functional alteration of fibroblasts from 'young' (<35 years) and 'old' (>50 years) donors. Our results brought evidence of the senescent status of 'old' fibroblasts by senescence associated β-galactosidase ( SA- βgal) positive staining and p16 expression. A PCR array focusing on senescence highlighted a subset of downregulated genes including cell cycle progression and ECM genes in 'old' fibroblasts as well as a subset of upregulated genes involved in senescence features. In 'old' fibroblasts, we measured a downregulation of proliferative and contractile capacities of migratory potential under PDGF stimulation and activation into myofibroblasts under TGF β. Old fibroblasts were also more sensitive to oxidative stress than 'young' ones. Of interest, downregulation of p16 expression partially reversed the senescent phenotype of 'old' fibroblasts but failed to restore their functional properties. In conclusion, our data brought evidence of phenotypic and functional differences between fibroblasts from young and intrinsically aged skin that may contribute to the alterations observed with ageing. [ABSTRACT FROM AUTHOR]

Published
2016
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34. Genes involved in the WNT and vesicular trafficking pathways are associated with melanoma predisposition.

Author

Ibarrola‐Villava, Maider, Kumar, Rajiv, Nagore, Eduardo, Benfodda, Meriem, Guedj, Mickael, Gazal, Steven, Hu, Hui‐Han, Guan, Jian, Rachkonda, P. Sivaramakishna, Descamps, Vincent, Basset‐Seguin, Nicole, Bensussan, Armand, Bagot, Martine, Saiag, Philippe, Schadendorf, Dirk, Martin‐Gonzalez, Manuel, Mayor, Matias, Grandchamp, Bernard, Ribas, Gloria, and Nadem, Soufir

Abstract

Multifactorial predisposition to melanoma includes genes involved in pigmentation, immunity and DNA repair. Nonetheless, missing heritability in melanoma is still important. We studied the role of 335 candidate SNPs in melanoma susceptibility by using a dedicated chip and investigating 110 genes involved in different pathways. A discovery set was comprised of 1069 melanoma patients and 925 controls from France. Data were replicated using validation phases II (1085 cases and 801 controls from Spain) and III (1808 cases and 1894 controls from Germany and a second set of Spanish samples). In addition, an exome sequencing study was performed in three high-risk French melanoma families. Nineteen SNPs in 17 genes were initially associated with melanoma in the French population. Six SNPs were replicated in phase II, including two new SNPs in the WNT3 (rs199524) and VPS41 (rs11773094) genes. The role of VPS41 and WNT3 was confirmed in a meta-analysis (3940 melanoma cases and 3620 controls) with two-side p values of 0.002, (OR = 0.86) and 4.07 × 10−10 (OR = 0.80), respectively. Exome sequencing revealed a non-synonymous VPS41 variant in one family that was shown to be strongly associated with familial melanoma (OR = 4.46, p = 0.001) in an independent sample of 178 melanoma families. WNT3 belongs to WNT pathway known to play a crucial role in melanoma, whereas VPS41 regulates vesicular trafficking and is thought to play a role in pigmentation. Our work identified two new pathways involved in melanoma predisposition. These results may be useful in the future for identifying individuals highly predisposed to melanoma. [ABSTRACT FROM AUTHOR]

Published
2015
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35. Prognostic Factors in Operable Breast Cancer Treated with Neoadjuvant Chemotherapy: Towards a Quantification of Residual Disease.

Author

Mombelli, Sarah, Kwiatkowski, Fabrice, Abrial, Catherine, Wang-Lopez, Qian, de Boissieu, Paul, Garbar, Christian, Bensussan, Armand, and Curé, Hervé

Subjects
ANTINEOPLASTIC agents, DISEASE relapse, BREAST cancer prognosis, ACADEMIC medical centers, CHI-squared test, COMBINED modality therapy, LONGITUDINAL method, MULTIVARIATE analysis, RADIOTHERAPY, STATISTICS, T-test (Statistics), TUMOR classification, DATA analysis, PROPORTIONAL hazards models, RETROSPECTIVE studies, DESCRIPTIVE statistics, KAPLAN-Meier estimator, DIAGNOSIS, HISTORY
Abstract

Objective: Neoadjuvant chemotherapy (NACT) allows for a more frequent use of breast-conservative surgery; it is also an in vivo model of individual tumor sensitivity which permits to determine new prognostic factors to personalize the therapeutic approach. Methods: Between 2000 and 2012, 318 patients with primary invasive breast cancer were treated with a median of 6 cycles of NACT; they received either an anthracycline-based FEC 100 protocol (31.1%), or anthracyclines + taxanes (53.5%), with trastuzumab if indicated (15.4%). Results: After a median follow-up of 44.2 months, the pathological complete response rate according to the classification of Chevallier et al. [Am J Clin Oncol 1993;16:223-228] was 19.3%, and overall (OS) and disease-free survival (DFS) at 10 years were 60.2 and 69.6%, respectively. Univariate analyses demonstrated that the Residual Disease in Breast and Nodes (RDBN) index was the most significant prognostic factor for OS (p = 0.0082) and DFS (p = 0.0022), and multivariate analyses mainly revealed that the residual tumor size, residual involved node number and post-chemotherapy Scarff-Bloom-Richardson (SBR) grading were the most significant prognostic factors. Conclusions: In a cohort of patients who were all homogeneously treated with some of the most common drugs for breast cancer, we demonstrate that NACT may provide additional prognostic factors and confirm the RDBN index. As this index allows for the prediction of survival with different breast cancer subtypes, we suggest that it should be calculated routinely to help clinicians to select patients who need adjuvant treatments. © 2015 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published
2015
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36. Membrane expression of NK receptors CD160 and CD158k contributes to delineate a unique CD4+ T-lymphocyte subset in normal and mycosis fungoides skin.

Author

Sako, Nouhoum, Schiavon, Valérie, Bounfour, Touda, Dessirier, Valérie, Ortonne, Nicolas, Olive, Daniel, Ram‐Wolff, Caroline, Michel, Laurence, Sicard, Hélène, Marie‐Cardine, Anne, Bagot, Martine, Bensussan, Armand, and Schmitt, Christian

Abstract

CD160 is a GPI-anchored Ig-like receptor identified by the BY55 mAb on human circulating CD56dim+ NK cells and TCRγδ lymphocytes. In addition, while most intestinal T lymphocytes express it, only a minor circulating CD4+ or CD8+ T lymphocyte subset is CD160+. Here we describe a population of CD4+CD160+ human blood T lymphocytes of circulating cutaneous T cells. These rare T lymphocytes represent 2.1 ± 1.9% of the circulating CD3+CD4+ T cells, coexpress CD8αα, CD244, and perforin but lack CD28 expression, a phenotype corresponding to effector memory cytotoxic T-lymphocytes. Functional studies further confirmed their cytotoxic potential. These cells lack αEβ7 integrin and CCR7 expression but do express skin-addressing molecules CLA, and CCR4. In normal human skin, CD4+CD160+ cells represent 34.6 ± 14.7% of the CD4+ T lymphocytes extracted by collagenase treatment. These T cells coexpress CLA (81 ± 13.6%), CCR4 (62.3 ± 15.9%), and some CD8αα (19.6 ± 13%) or CCR7 (24.4 ± 11.7%) expression. Cutaneous T-cell lymphoma cells express the natural killer receptor KIR3DL2 (CD158k) used as a tumor marker. Not only we confirmed the expression of this marker in the blood and/or skin of mycosis fungoides patients but we also show for the first time CD158k expression (often associated with CD160) on cutaneous CD4+ T cells from healthy individuals (25.3 ± 15%). Therefore, CD4+CD160+ T cells expressing CD158k might represent specialized cutaneous lymphocytes devoted to immune surveillance, from which could originate cutaneous T-cell lymphomas such as mycosis fungoides. © 2014 International Society for Advancement of Cytometry [ABSTRACT FROM AUTHOR]

Published
2014
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37. Granulocyte-Colony Stimulating Factor Related Pathways Tested on an Endometrial Ex-Vivo Model.

Author

Rahmati, Mona, Petitbarat, Marie, Dubanchet, Sylvie, Bensussan, Armand, Chaouat, Gerard, and Ledee, Nathalie

Subjects
GRANULOCYTE-colony stimulating factor, ENDOMETRIAL diseases, REPRODUCTIVE health, MOLECULAR interactions, MISCARRIAGE, ENDOMETRIUM
Abstract

Introduction: Recombinant human Granulocyte-Colony Stimulating Factor (rhG-CSF) supplementation seems to be a promising innovative therapy in reproductive medicine, used in case of recurrent miscarriage, embryo implantation failure or thin endometrium, although its mechanisms of action remain unknown. Our aim was to identify possible endometrial pathways influenced by rhG-CSF. Materials and Methods: Hypothetical molecular interactions regulated by G-CSF were designed through a previous large scale endometrial microarray study. The variation of endometrial expression of selected target genes was confirmed in control and infertile patients. G-CSF supplementation influence on these targets was tested on an endometrial ex-vivo culture. Middle luteal phase endometrial biopsies were cultured on collagen sponge with or without rhG-CSF supplementation during 3 consecutive days. Variations of endometrial mRNA expression for the selected targets were studied by RT-PCR. Results: At the highest dose of rhG-CSF stimulation, the mRNA expression of these selected target genes was significantly increased if compared with their expression without addition of rhG-CSF. The selected targets were G-CSF Receptor (G-CSFR), Integrin alpha-V/beta-3 (ITGB3) implicated in cell migration and embryo implantation, Plasminogen Activator Urokinase Receptor (PLAUR) described as interacting with integrins and implicated in cell migration, Thymidine Phosphorylase (TYMP) implicated in local angiogenesis, CD40 and its ligand CD40L involved in cell proliferation control. Conclusion: RhG-CSF seems able to influence endometrial expressions crucial for implantation process involving endometrial vascular remodelling, local immune modulation and cellular adhesion pathways. These variations observed in an ex-vivo model should be tested in-vivo. The strict indications or counter indication of rhG-CSF supplementation in reproductive field are not yet established, while the safety of its administration in early pregnancy on early embryogenesis still needs to be demonstrated. Nevertheless, rhG-CSF appears as a promising therapy in some difficult and unsolved cases of reproductive failure. Indications of pre-conceptual rhG-CSF supplementation may derive from a diagnosed lack of endometrial expression of some target genes. [ABSTRACT FROM AUTHOR]

Published
2014
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38. T-Plastin Expression Downstream to the Calcineurin/NFAT Pathway Is Involved in Keratinocyte Migration.

Author

Brun, Cécilia, Demeaux, Agathe, Guaddachi, Frédéric, Jean-Louis, Francette, Oddos, Thierry, Bagot, Martine, Bensussan, Armand, Jauliac, Sébastien, and Michel, Laurence

Subjects
KERATINOCYTES, FIMBRIN, GENE expression, CALCINEURIN, NUCLEAR factor of activated T-cells, CELL migration, CELL proliferation
Abstract

Cutaneous wound healing requires keratinocyte proliferation, migration and differentiation to restore the barrier function of the skin. The calcineurin/nuclear factor of activated-T-cell (NFAT) signaling pathway has been recently shown to be involved in keratinocyte growth, differentiation and migration. It is induced by an increased intracellular calcium rate and its inhibition results in decreased capacities of keratinocytes to migrate. Nevertheless, the link between calcineurin activation and keratinocyte migration remains unknown. Recently, Orai1, a pore subunit of a store-operated calcium channel that favors calcium influx, was shown to play a critical role to control proliferation and migration of basal keratinocytes. Of interest, the actin-bundling T-plastin is crucial in cell motility through cross-linking to actin filament and its synthesis was shown to be induced by calcium influx and regulated by the calcineurin/NFAT pathway in tumor Sezary cells. We investigated herein the role of the calcineurin/NFAT pathway-dependent T-plastin in keratinocyte migration, by quantifying T-plastin expression in keratinocytes and by analyzing their migration under calcineurin inhibition or knockdown of NFAT2 or T-plastin. We did confirm the role of the calcineurin/NFAT pathway in keratinocyte migration as shown by their decreased capacities to migrate after FK506 treatment or siNFAT2 transfection in both scratching and Boyden assays. The expression of NFAT2 and T-plastin in keratinocytes was decreased under FK506 treatment, suggesting that T-plastin plays a role in keratinocyte migration downstream to the calcineurin/NFAT pathway. Accordingly, siRNA knockdown of T-plastin expression also decreased their migration capacities. Actin lamellipodia formation as well as FAK and β6-integrin expression were also significantly decreased after treatment with FK506 or siRNA, reinforcing that NFAT2-dependent T-plastin expression plays a role in keratinocyte migration. These results indicate that T-plastin might be considered as a major actor in the mechanisms underlying calcineurin/NFAT-dependent keratinocyte migration and may explain wound-healing defects observed in patients under calcineurin inhibitor long-term treatment. [ABSTRACT FROM AUTHOR]

Published
2014
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39. Regulatory T-cells in pregnancy: historical perspective, state of the art, and burning questions.

Author

Ruocco, Maria Grazia, Chaouat, Gérard, Florez, Laura, Bensussan, Armand, and Klatzmann, David

Subjects
SUPPRESSOR cells, T cells, PREGNANCY, DENDRITIC cells, KILLER cells
Abstract

In this review, we first revisit the original concept of "suppressor T-cells" in pregnancy, put it in a historical perspective, and then highlight the main data that licensed its resurrection and revision into the concept of "regulatory T-cells" (Tregs) in pregnancy. We review the evidence for a major role of Tregs in murine and human pregnancy and discuss Treg interactions with dendritic and uterine natural killer cells, other players of maternal-fetal tolerance. Finally, we highlight what we consider as the most important questions in the field. [ABSTRACT FROM AUTHOR]

Published
2014
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41. Regulatory T cells in pregnancy: historical perspective, state of the art and burning questions.

Author

Ruocco, Maria Grazia, Chaouat, Gérard, Florez, Laura, Bensussan, Armand, and Klatzmann, David

Subjects
T cells, PREGNANCY, DENDRITIC cells, KILLER cells, UTERUS
Abstract

In this review, we first revisit the original concept of "suppressor T cells" in pregnancy, put it in a historical perspective and then highlight the main data that licensed its resurrection and revision into the concept of "regulatory T cells" (Tregs) in pregnancy. We review the evidence for a major role of Tregs in murine and human pregnancy and discuss Treg interactions with dendritic and uterine natural killer cells, other players of maternal-fetal tolerance. Finally, we highlight what we consider as the most important questions in the field. [ABSTRACT FROM AUTHOR]

Published
2014
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42. Contribution of CD39 to the immunosuppressive microenvironment of acute myeloid leukaemia at diagnosis.

Author

Dulphy, Nicolas, Henry, Guylaine, Hemon, Patrice, Khaznadar, Zena, Dombret, Hervé, Boissel, Nicolas, Bensussan, Armand, and Toubert, Antoine

Subjects
T cells, IMMUNOSUPPRESSION, ACUTE myeloid leukemia, CELL receptors, TUMOR genetics
Abstract

The article presents the result of a study which examined the role of regulatory T cells (Tregs) subpopulations in the development of an immunosuppressive environment in acute myeloid leukemia (AML). The researchers suggest that these Tregs have the capacity to move into tissues based on the detection of CCR4, CCRS CCR7 and CD49d expressions of homing receptors specific for skin, intestine, lymph nodes and inflamed tissues. They also suggested that Tregs would prevent anti-tumor response.

Published
2014
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43. A Large French Case-Control Study Emphasizes the Role of Rare Mc1R Variants in Melanoma Risk.

Author

Hui-Han Hu, Benfodda, Mériem, Dumaz, Nicolas, Gazal, Steven, Descamps, Vincent, Bourillon, Agnès, Basset-Seguin, Nicole, Riffault, Angélique, Ezzedine, Khaled, Bagot, Martine, Bensussan, Armand, Saiag, Philippe, Grandchamp, Bernard, and Soufir, Nadem

Abstract

Background. The MC1R gene implicated in melanogenesis and skin pigmentation is highly polymorphic. Several alleles are associated with red hair and fair skin phenotypes and contribute to melanoma risk. Objective. This work aims to assess the effect of different classes of MC1R variants, notably rare variants, on melanoma risk. Methods. MC1R coding region was sequenced in 1131 melanoma patients and 869 healthy controls. MC1R variants were classified as RHC (R) and non-RHC (r). Rare variants (frequency < 1%) were subdivided into two subgroups, predicted to be damaging (D) or not (nD). Results. Both R and r alleles were associated with melanoma (OR = 2.66 [2.20-3.23] and 1.51 [1.32-1.73]) and had similar population attributable risks (15.8% and 16.6%).We also identified 69 rare variants, of which 25 were novel. D variants were strongly associated with melanoma (OR = 2.38 [1.38-4.15]) and clustered in the same MC1R domains as R alleles (intracellular 2, transmembrane 2 and 7). Conclusion. This work confirms the role of R and r alleles in melanoma risk in the French population and proposes a novel class of rare D variants as important melanoma risk factors. These findings may improve the definition of high-risk subjects that could be targeted for melanoma prevention and screening. [ABSTRACT FROM AUTHOR]

Published
2014
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44. IL-17A is produced by breast cancer TILs and promotes chemoresistance and proliferation through ERK1/2.

Author

Cochaud, Stéphanie, Giustiniani, Jérôme, Thomas, Clémence, Laprevotte, Emilie, Garbar, Christian, Savoye, Aude-Marie, Curé, Hervé, Mascaux, Corinne, Alberici, Gilles, Bonnefoy, Nathalie, Eliaou, Jean-François, Bensussan, Armand, and Bastid, Jeremy

Subjects
INTERLEUKIN-17, BREAST cancer treatment, CANCER cell proliferation, CYTOKINES, DRUG resistance in cancer cells, LYMPHOCYTES, DOCETAXEL
Abstract

The proinflammatory cytokine Interleukin 17A (hereafter named IL-17A) or IL-17A producing cells are elevated in breast tumors environment and correlate with poor prognosis. Increased IL-17A is associated with ER(-) or triple negative tumors and reduced Disease Free Survival. However, the pathophysiological role of IL-17A in breast cancer remains unclear although several studies suggested its involvement in cancer cell dissemination. Here we demonstrated that a subset of breast tumors is infiltrated with IL-17A-producing cells. Increased IL-17A seems mainly associated to ER(-) and triple negative/basal-like tumors. Isolation of tumor infiltrating T lymphocytes (TILs) from breast cancer biopsies revealed that these cells secreted significant amounts of IL-17A. We further established that recombinant IL-17A recruits the MAPK pathway by upregulating phosphorylated ERK1/2 in human breast cancer cell lines thereby promoting proliferation and resistance to conventional chemotherapeutic agents such as docetaxel. We also confirmed here that recombinant IL-17A stimulates migration and invasion of breast cancer cells as previously reported. Importantly, TILs also induced tumor cell proliferation, chemoresistance and migration and treatment with IL-17A-neutralizing antibodies abrogated these effects. Altogether these results demonstrated the pathophysiological role of IL-17A-producing cell infiltrate in a subset of breast cancers. Therefore, IL-17A appears as potential therapeutic target for breast cancer. [ABSTRACT FROM AUTHOR]

Published
2013
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46. MUC1/CD227 IMMUNOHISTOCHEMISTRY IN ROUTINE PRACTICE IS A USEFUL BIOMARKER IN BREAST CANCERS.

Author

Garbar, Christian, Mascaux, Corinne, Curé, Hervé, and Bensussan, Armand

Subjects
BREAST cancer, CANCER prognosis, CANCER treatment, MUCIN genetics, IMMUNOHISTOCHEMISTRY, BIOMARKERS, HORMONE receptors
Abstract

Over-expression of MUC1/CD227 is observed in 90% of breast tumors. Classical morphologic description and semi-quantitative digital measurement of MUC1 were performed from immunohistochemical stained slides of 123 routine histological samples. Measures of MUC1 expression showed statistical differences between non tumoral (NT) breast tissue and Ductal Carcinoma In Situ (DCIS) or infiltrating carcinoma (IC), p < 0.0001. Loss of MUC1 was correlated with high Ki67 index (p = 0.001) and loss of hormonal receptors (p = 0.03), whereas no correlations were found with HER2 expression. High-grade DCIS or IC showed increasing loss of apical polarised and cytoplasmic expression of MUC1. [ABSTRACT FROM AUTHOR]

Published
2013
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47. Genetic variation at KIT locus may predispose to melanoma.

Author

Bourillon, Agnes, Hu, Hui‐Han, Hetet, Gilles, Lacapere, Jean‐Jacques, André, Jocelyne, Descamps, Vincent, Basset‐Seguin, Nicole, Ogbah, Zighereda, Puig, Susana, Saiag, Philippe, Bagot, Martine, Bensussan, Armand, Grandchamp, Bernard, Dumaz, Nicolas, and Soufir, Nadem

Subjects
MELANOMA, HUMAN genetic variation, DISEASE progression, SINGLE nucleotide polymorphisms, CANCER risk factors, MELANOCYTES, CELLULAR signal transduction
Abstract

As loss of KIT frequently occurs in melanoma progression, we hypothesized that KIT is implicated in predisposition to melanoma ( MM). Thus, we sequenced the KIT coding region in 112 familial MM cases and 143 matched controls and genotyped tag single-nucleotide polymorphisms ( SNPs) in two cohorts of melanoma patients and matched controls. Five rare KIT substitutions, all predicted possibly or probably deleterious, were identified in five patients, but none in controls [ RR = 2.26 (1.26-2.26)]. Expressed in melanocyte lines, three substitutions inhibited KIT signaling. Comparison with exomes database (7020 alleles) confirmed a significant excess of rare deleterious KIT substitutions in patients. Additionally, a common SNP, rs2237028, was associated with MM risk, and 6 KIT variants were associated with nevus count. Our data strongly suggest that rare KIT substitutions predispose to melanoma and that common variants at KIT locus may also impact nevus count and melanoma risk. [ABSTRACT FROM AUTHOR]

Published
2013
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48. Active Chronic Sarcoidosis is Characterized by Increased Transitional Blood B Cells, Increased IL-10-Producing Regulatory B Cells and High BAFF Levels.

Author

Saussine, Anne, Tazi, Abdellatif, Feuillet, Séverine, Rybojad, Michel, Juillard, Caroline, Bergeron, Anne, Dessirier, Valérie, Bouhidel, Fatiha, Janin, Anne, Bensussan, Armand, Bagot, Martine, Bouaziz, Jean-David, and Hoshino, Yoshihiko

Subjects
SARCOIDOSIS, IMMUNE response, HYPERGAMMAGLOBULINEMIA, B cells, ORGAN donors, HOMEOSTASIS
Abstract

Background: Sarcoidosis is a multisystemic disease of unknown etiology characterized by a disproportionate Th1 granulomatous immune response in the organs involved. Plasmatic hypergammaglobulinemia and B cell accumulation in granulomatous lesions suggest the possible role of humoral immune responses in the pathogenesis of sarcoidosis. The purpose of this study is to describe B cell peripheral compartment in sarcoidosis. Methodology/Principal Findings: We analyzed blood B cell subsets and BAFF levels in 33 patients with chronic sarcoidosis (active sarcoidosis n = 18; inactive sarcoidosis n = 15) and 18 healthy donors. Active chronic sarcoidosis patients had significantly less circulating memory B cells (p<0.01), more transitional (p<0.01) and increased numbers of IL-10-producing regulatory B cells (p<0.05) compared with healthy donors and patients with inactive sarcoidosis. BAFF serum levels were significantly higher in patients with active sarcoidosis (p<0.01 versus healthy donors and inactive sarcoidosis patients) and strongly correlated with serum hypergammaglobulinemia (r = 0.53, p<0.01) and angiotensin converting enzyme levels (r = 0.61, p =<0.01). Conclusions/Significance: These data show that there is an altered B cell homeostasis in active sarcoidosis and suggest BAFF antagonist drugs as potential new treatments of this disease. [ABSTRACT FROM AUTHOR]

Published
2012
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49. TWEAK Affects Keratinocyte G2/M Growth Arrest and Induces Apoptosis through the Translocation of the AIF Protein to the Nucleus.

Author

Alaoui, Sanaa Sabour, Dessirier, Valérie, De Araujo, Elisabeth, Alexaki, Vassilia-Ismini, Pelekanou, Vassiliki, Lkhider, Mustapha, Stathopoulos, Efstathios N., Castanas, Elias, Bagot, Martine, Bensussan, Armand, and Tsapis, Andreas

Subjects
APOPTOSIS, FIBROBLAST growth factors, IMMUNOMODULATORS, CELL proliferation, NEOVASCULARIZATION, CANCER cells
Abstract

The soluble TNF-like weak inducer of apoptosis (TWEAK, TNFSF12) binds to the fibroblast growth factor-inducible 14 receptor (FN14, TNFRSF12A) on the cell membrane and induces multiple biological responses, such as proliferation, migration, differentiation, angiogenesis and apoptosis. Previous reports show that TWEAK, which does not contain a death domain in its cytoplasmic tail, induces the apoptosis of tumor cell lines through the induction of TNFα secretion. TWEAK induces apoptosis in human keratinocytes. Our experiments clearly demonstrate that TWEAK does not induce the secretion of TNFα or TRAIL proteins. The use of specific inhibitors and the absence of procaspase-3 cleavage suggest that the apoptosis of keratinocytes follows a caspase- and cathepsin B-independent pathway. Further investigation showed that TWEAK induces a decrease in the mitochondrial membrane potential of keratinocytes. Confocal microscopy showed that TWEAK induces the cleavage and the translocation of apoptosis inducing factor (AIF) from the mitochondria to the nucleus, thus initiating caspase-independent apoptosis. Moreover, TWEAK induces FOXO3 and GADD45 expression, cdc2 phosphorylation and cdc2 and cyclinB1 degradation, resulting in the arrest of cell growth at the G2/M phase. Finally, we report that TWEAK and FN14 are normally expressed in the basal layer of the physiological epidermis and are greatly enhanced in benign (psoriasis) and malignant (squamous cell carcinoma) skin pathologies that are characterized by an inflammatory component. TWEAK might play an essential role in skin homeostasis and pathology. [ABSTRACT FROM AUTHOR]

Published
2012
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50. IFN-α and CD46 stimulation are associated with active lupus and skew natural T regulatory cell differentiation to type 1 regulatory T (Tr1) cells.

Author

Buanec, Hélène Le, Gougeon, Marie-Lise, Mathian, Alexis, Lebon, Pierre, Dupont, Jean-Michel, Peltre, Gabriel, Hemon, Patrice, Schmid, Michel, Bizzini, Bernard, Künding, Thomas, Burny, Arsène, Bensussan, Armand, Amoura, Zahir, Gallo, Robert C., and Zagury, Daniel

Subjects
T cells, IMMUNOPATHOLOGY, AIDS, ANTI-inflammatory agents, IMMUNOLOGY of inflammation, LUPUS erythematosus, IMMUNOTHERAPY, PATIENTS
Abstract

Immune suppressive activities exerted by regulatory T-cell subsets have several specific functions, including self-tolerance and regulation of adaptive immune reactions, and their dysfunction can lead to autoimmune diseases and contribute to AIDS and cancer. Two functionally distinct regulatory T-cell subsets are currently identified in peripheral tissues: thymus-developed natural T regulatory cells (nTregs) controlling self-tolerance and antiinflammatory IL-10-secreting type 1 regulatory T cells (Tr1) derived from Ag-stimulated T cells, which regulate inflammation-dependent adaptive immunity and minimize immunopathology. We establish herein that cell contact-mediated nTreg regulatory function is inhibited by inflammation, especially in the presence of the complement C3b receptor (CD46). Instead, as with other T-cell subsets, the latter inflammatory conditions of stimulation skew nTreg differentiation to Tr1 cells secreting IL-10, an effect potentiated by IFN-a. The clinical relevance of these findings was verified in a study of 152 lupus patients, in which we showed that lupus nTreg dysfunction is not due to intrinsic defects but is rather induced by C3b stimulation of CD46 and IFN-a and that these immune components of inflammation are directly associated with active lupus. These results provide a rationale for using anti-IFN-α Ab immunotherapy in lupus patients. [ABSTRACT FROM AUTHOR]

Published
2011
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