Your search keyword '"Lopez-Lastra, Silvia"' showing total 12 results

1. Accelerated thymopoiesis and improved T‐cell responses in HLA‐A2/‐DR2 transgenic BRGS‐based human immune system mice.

Author

Masse‐Ranson, Guillemette, Dusséaux, Mathilde, Fiquet, Oriane, Darche, Sylvie, Boussand, Maud, Li, Yan, Lopez‐Lastra, Silvia, Legrand, Nicolas, Corcuff, Erwan, Toubert, Antoine, Centlivre, Mireille, Bruel, Timothée, Spits, Hergen, Schwartz, Olivier, Lévy, Yves, Strick‐Marchand, Hélène, and Di Santo, James P.

Subjects

T cells, IMMUNE system, TRANSGENES, IMMUNIZATION, LYMPHOCYTES

Abstract

Human immune system (HIS) mouse models provide a robust in vivo platform to study human immunity. Nevertheless, the signals that guide human lymphocyte differentiation in HIS mice remain poorly understood. Here, we have developed a novel Balb/c Rag2−/−Il2rg−/−SirpaNOD (BRGS) HIS mouse model expressing human HLA‐A2 and ‐DR2 transgenes (BRGSA2DR2). When comparing BRGS and BRGSA2DR2 HIS mice engrafted with human CD34+ stem cells, a more rapid emergence of T cells in the circulation of hosts bearing human HLA was shown, which may reflect a more efficient human T‐cell development in the mouse thymus. Development of CD4+ and CD8+ T cells was accelerated in BRGSA2DR2 HIS mice and generated more balanced B and T‐cell compartments in peripheral lymphoid organs. Both B‐ and T‐cell function appeared enhanced in the presence of human HLA transgenes with higher levels of class switched Ig, increased percentages of polyfunctional T cells and clear evidence for antigen‐specific T‐cell responses following immunization. Taken together, the presence of human HLA class I and II molecules can improve multiple aspects of human B‐ and T‐cell homeostasis and function in the BRGS‐based HIS mouse model. [ABSTRACT FROM AUTHOR]

Published

2019

2. Human thymopoiesis is influenced by a common genetic variant within the TCRA-TCRD locus.

Author

Clave, Emmanuel, Araujo, Itauá Leston, Alanio, Cécile, Patin, Etienne, Bergstedt, Jacob, Urrutia, Alejandra, Lopez-Lastra, Silvia, Li, Yan, Charbit, Bruno, MacPherson, Cameron Ross, Hasan, Milena, Melo-Lima, Breno Luiz, Douay, Corinne, Saut, Noémie, Germain, Marine, Trégouët, David-Alexandre, Morange, Pierre-Emmanuel, Fontes, Magnus, Duffy, Darragh, and Di Santo, James P.

Subjects

HUMAN genetic variation, T cell receptors, LABORATORY mice, HUMAN gene mapping, HUMAN genome

Abstract

Aging, sex, and genetics substantially affect human thymic function. Mining the Milieu Intérieur: Personalized medicine partly depends on understanding what causes variance even outside the context of overt disease. The Milieu Intérieur Consortium enrolled 1000 healthy adults to study how genetics and the environment influence the immune system. Clave et al. leveraged samples from this cohort to see how thymic output, known to decrease over time, is affected by other factors. In addition to seeing sex-dependent differences, a genome-wide association study revealed variants that were associated with thymic output, which was confirmed in an independent cohort and mouse models. The authors have also developed a Web application for other investigators to examine the Milieu Intérieur data. The thymus is the primary lymphoid organ where naïve T cells are generated; however, with the exception of age, the parameters that govern its function in healthy humans remain unknown. We characterized the variability of thymic function among 1000 age- and sex-stratified healthy adults of the Milieu Intérieur cohort, using quantification of T cell receptor excision circles (TRECs) in peripheral blood T cells as a surrogate marker of thymopoiesis. Age and sex were the only nonheritable factors identified that affect thymic function. TREC amounts decreased with age and were higher in women compared to men. In addition, a genome-wide association study revealed a common variant (rs2204985) within the T cell receptor TCRA-TCRD locus, between the DD2 and DD3 gene segments, which associated with TREC amounts. Strikingly, transplantation of human hematopoietic stem cells with the rs2204985 GG genotype into immunodeficient mice led to thymopoiesis with higher TRECs, increased thymocyte counts, and a higher TCR repertoire diversity. Our population immunology approach revealed a genetic locus that influences thymopoiesis in healthy adults, with potentially broad implications in precision medicine. [ABSTRACT FROM AUTHOR]

Published

2018

3. MOSAIC: Multi-Omic Spatial Atlas in Cancer, effect on precision oncology.

Author

Lehar, Joseph, Madissoon, Elo, Chevallier, Jerome, Schiratti, Jean Baptiste, Kamburov, Atanas, Barnes, Rodrigo, Haignere, Carla, Joy, Anna, Dodacki, Agnès, Hoffmann, Caroline, Lopez Lastra, Silvia, Espin Perez, Almudena, Bayard, Quentin, von Loga, Katharina, Chaperon, Hubert, Vert, Jean-Philippe, Durand, Eric, Soumelis, Vassili, Wainrib, Gilles, and Clozel, Thomas

Published

2023

4. Modeling Natural Killer Cell Targeted Immunotherapies.

Author

Lopez-Lastra, Silvia and Di Santo, James P.

Subjects

KILLER cells, IMMUNOTHERAPY, IMMUNOLOGY

Abstract

Animal models have extensively contributed to our understanding of human immunobiology and to uncover the underlying pathological mechanisms occurring in the development of diseases. However, mouse models do not reproduce the genetic and molecular complexity inherent in human disease conditions. Human immune system (HIS) mouse models that are susceptible to human pathogens and can recapitulate human hematopoiesis and tumor immunobiology provide one means to bridge the interspecies gap. Natural killer cells are the founding member of the innate lymphoid cell family. They exert a rapid and strong immune response against tumor and pathogen-infected cells. Their antitumor features have long been exploited for therapeutic purposes in the context of cancer. In this review, we detail the development of highly immunodeficient mouse strains and the models currently used in cancer research. We summarize the latest improvements in adoptive natural killer (NK) cell therapies and the development of novel NK cell sources. Finally, we discuss the advantages of HIS mice to study the interactions between human NK cells and human cancers and to develop new therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2017

5. In Vivo Efficacy of Umbilical Cord Blood Stem Cell-Derived NK Cells in the Treatment of Metastatic Colorectal Cancer.

Author

Veluchamy, John P., Lopez-Lastra, Silvia, Spanholtz, Jan, Bohme, Fenna, Nina Kok, Heideman, Daniëlle A. M., Verheul, Henk M. W., Di Santo, James P., de Gruijl, Tanja D., and van der Vliet, Hans J.

Subjects

MONOCLONAL antibodies, EPIDERMAL growth factor receptors, COLON cancer treatment

Abstract

Therapeutic monoclonal antibodies against the epidermal growth factor receptor (EGFR) act by inhibiting EGFR downstream signaling and by eliciting a natural killer (NK) cell-mediated antitumor response. The IgG1 mAb cetuximab has been used for treatment of RASwt metastatic colorectal cancer (mCRC) patients, showing limited efficacy. In the present study, we address the potential of adoptive NK cell therapy to overcome these limitations investigating two allogeneic NK cell products, i.e., allogeneic activated peripheral blood NK cells (A-PBNK) and umbilical cord blood stem cell-derived NK cells (UCB-NK). While cetuximab monotherapy was not effective against EGFR- RASwt, EGFR+ RASmut, and EGFR+ BRAFmut cells, A-PBNK were able to initiate lysis of EGFR+ colon cancer cells irrespective of RAS or BRAF status. Cytotoxic effects of A-PBNK (but not UCB-NK) were further potentiated significantly by coating EGFR+ colon cancer cells with cetuximab. Of note, a significantly higher cytotoxicity was induced by UCB-NK in EGFR-RASwt (42 ± 8 versus 67 ± 7%), EGFR+ RASmut (20 ± 2 versus 37 ± 6%), and EGFR+ BRAFmut (23 ± 3 versus 43 ± 7%) colon cancer cells compared to A-PBNK and equaled the cytotoxic efficacy of the combination of A-PBNK and cetuximab. The antitumor efficacy of UCB-NK cells against cetuximab-resistant human EGFR+ RASmut colon cancer cells was further confirmed in an in vivo preclinical mouse model where UCB-NK showed enhanced antitumor cytotoxicity against colon cancer independent of EGFR and RAS status. As UCB-NK have been proven safe in a recently conducted phase I clinical trial in acute myeloid leukemia, a fast translation into clinical proof of concept for mCRC could be considered. [ABSTRACT FROM AUTHOR]

Published

2017

6. NFIL3 Orchestrates the Emergence of Common Helper Innate Lymphoid Cell Precursors.

Author

Xu, Wei, Domingues, Rita G., Fonseca-Pereira, Diogo, Ferreira, Manuela, Ribeiro, Hélder, Lopez-Lastra, Silvia, Motomura, Yasutaka, Moreira-Santos, Lara, Bihl, Franck, Braud, Véronique, Kee, Barbara, Brady, Hugh, Coles, Mark C., Vosshenrich, Christian, Kubo, Masato, Di Santo, James P., and Veiga-Fernandes, Henrique

Abstract

Summary Innate lymphoid cells (ILCs) are a family of effectors that originate from a common innate lymphoid cell progenitor. However, the transcriptional program that sets the identity of the ILC lineage remains elusive. Here, we show that NFIL3 is a critical regulator of the common helper-like innate lymphoid cell progenitor (CHILP). Cell-intrinsic Nfil3 ablation led to variably impaired development of fetal and adult ILC subsets. Conditional gene targeting demonstrated that NFIL3 exerted its function prior to ILC subset commitment. Accordingly, NFIL3 ablation resulted in loss of ID2 + CHILP and PLZF + ILC progenitors. Nfil3 expression in lymphoid progenitors was under the control of the mesenchyme-derived hematopoietin IL-7, and NFIL3 exerted its function via direct Id2 regulation in the CHILP. Moreover, ectopic Id2 expression in Nfil3 -null precursors rescued defective ILC lineage development in vivo. Our data establish NFIL3 as a key regulator of common helper-like ILC progenitors as they emerge during early lymphopoiesis. [ABSTRACT FROM AUTHOR]

Published

2015

7. A bispecific nanobody approach to leverage the potent and widely applicable tumor cytolytic capacity of Vγ9Vδ2-T cells.

Author

de Bruin, Renée C. G., Veluchamy, John P., Lougheed, Sinéad M., Schneiders, Famke L., Lopez-Lastra, Silvia, Lameris, Roeland, Stam, Anita G., Sebestyen, Zsolt, Kuball, Jürgen, Molthoff, Carla F. M., Hooijberg, Erik, Roovers, Rob C., Santo, James P. Di, van Bergen en Henegouwen, Paul M. P., Verheul, Henk M. W., de Gruijl, Tanja D., and van der Vliet, Hans J.

Subjects

CANCER immunotherapy, T cells, CANCER treatment, THERAPEUTICS

Abstract

Though Vγ9Vδ2-T cells constitute only a small fraction of the total T cell population in human peripheral blood, they play a vital role in tumor defense and are therefore of major interest to explore for cancer immunotherapy. Vγ9Vδ2-T cell-based cancer immunotherapeutic approaches developed so far have been generally well tolerated and were able to induce significant clinical responses. However, overall results were inconsistent, possibly due to the fact that these strategies induced systemic activation of Vγ9Vδ2-T cells without preferential accumulation and targeted activation in the tumor. Here we show that a novel bispecific nanobody-based construct targeting both Vγ9Vδ2-T cells and EGFR induced potent Vγ9Vδ2-T cell activation and subsequent tumor cell lysis bothin vitroand in anin vivomouse xenograft model. Tumor cell lysis was independent ofKRASandBRAFtumor mutation status and common Vγ9Vδ2-T cell receptor sequence variations. In combination with the conserved monomorphic nature of the Vγ9Vδ2-TCR and the facile replacement of the tumor-specific nanobody, this immunotherapeutic approach can be applied to a large group of cancer patients. [ABSTRACT FROM PUBLISHER]

Published

2018

8. Systemic Human ILC Precursors Provide a Substrate for Tissue ILC Differentiation.

Author

Lim, Ai Ing, Li, Yan, Lopez-Lastra, Silvia, Stadhouders, Ralph, Paul, Franziska, Casrouge, Armanda, Serafini, Nicolas, Puel, Anne, Bustamante, Jacinta, Surace, Laura, Masse-Ranson, Guillemette, David, Eyal, Strick-Marchand, Helene, Le Bourhis, Lionel, Cocchi, Roberto, Topazio, Davide, Graziano, Paolo, Muscarella, Lucia Anna, Rogge, Lars, and Norel, Xavier

Subjects

*INNATE lymphoid cells, *CELL differentiation, *CYTOTOXIC T cells, *T helper cells, *TRANSCRIPTION factors, *RETINOIC acid receptors

Abstract

Summary Innate lymphoid cells (ILCs) represent innate versions of T helper and cytotoxic T cells that differentiate from committed ILC precursors (ILCPs). How ILCPs give rise to mature tissue-resident ILCs remains unclear. Here, we identify circulating and tissue ILCPs in humans that fail to express the transcription factors and cytokine outputs of mature ILCs but have these signature loci in an epigenetically poised configuration. Human ILCPs robustly generate all ILC subsets in vitro and in vivo. While human ILCPs express low levels of retinoic acid receptor (RAR)-related orphan receptor C (RORC) transcripts, these cells are found in RORC-deficient patients and retain potential for EOMES + natural killer (NK) cells, interferon gamma-positive (IFN-γ + ) ILC1s, interleukin (IL)-13 + ILC2s, and for IL-22 + , but not for IL-17A + ILC3s. Our results support a model of tissue ILC differentiation (“ILC-poiesis”), whereby diverse ILC subsets are generated in situ from systemically distributed ILCPs in response to local environmental signals. [ABSTRACT FROM AUTHOR]

Published

2017

9. Interleukin-15-Dependent T-Cell-like Innate Intraepithelial Lymphocytes Develop in the Intestine and Transform into Lymphomas in Celiac Disease.

Author

Ettersperger, Julien, Montcuquet, Nicolas, Malamut, Georgia, Guegan, Nicolas, Lopez-Lastra, Silvia, Gayraud, Ségolène, Reimann, Christian, Vidal, Elodie, Cagnard, Nicolas, Villarese, Patrick, Andre-Schmutz, Isabelle, Gomes Domingues, Rita, Godinho-Silva, Cristina, Veiga-Fernandes, Henrique, Lhermitte, Ludovic, Asnafi, Vahid, Macintyre, Elizabeth, Cellier, Christophe, Beldjord, Kheira, and Di Santo, James P.

Subjects

*INTERLEUKIN-15, *CELIAC disease, *T cells, *LYMPHOMAS, *LYMPHOCYTES, *EPITHELIAL cells, *PATIENTS

Abstract

Summary The nature of gut intraepithelial lymphocytes (IELs) lacking antigen receptors remains controversial. Herein we showed that, in humans and in mice, innate intestinal IELs expressing intracellular CD3 (iCD3 + ) differentiate along an Id2 transcription factor (TF)-independent pathway in response to TF NOTCH1, interleukin-15 (IL-15), and Granzyme B signals. In NOTCH1-activated human hematopoietic precursors, IL-15 induced Granzyme B, which cleaved NOTCH1 into a peptide lacking transcriptional activity. As a result, NOTCH1 target genes indispensable for T cell differentiation were silenced and precursors were reprogrammed into innate cells with T cell marks including intracellular CD3 and T cell rearrangements. In the intraepithelial lymphoma complicating celiac disease, iCD3 + innate IELs acquired gain-of-function mutations in Janus kinase 1 or Signal transducer and activator of transcription 3, which enhanced their response to IL-15. Overall we characterized gut T cell-like innate IELs, deciphered their pathway of differentiation and showed their malignant transformation in celiac disease. [ABSTRACT FROM AUTHOR]

Published

2016

10. Lipid-Associated Macrophages Are Induced by Cancer-Associated Fibroblasts and Mediate Immune Suppression in Breast Cancer.

Author

Timperi E, Gueguen P, Molgora M, Magagna I, Kieffer Y, Lopez-Lastra S, Sirven P, Baudrin LG, Baulande S, Nicolas A, Champenois G, Meseure D, Vincent-Salomon A, Tardivon A, Laas E, Soumelis V, Colonna M, Mechta-Grigoriou F, Amigorena S, and Romano E

Subjects

Animals, Cell Adhesion Molecules, Neuronal, Cell Line, Tumor, Fibroblasts pathology, Humans, Immune Checkpoint Inhibitors, Lipids, Macrophages, Mice, Tumor Microenvironment genetics, Cancer-Associated Fibroblasts pathology, Triple Negative Breast Neoplasms pathology

Abstract

Tumor-associated macrophages (TAM) play a detrimental role in triple-negative breast cancer (TNBC). In-depth analysis of TAM characteristics and interactions with stromal cells, such as cancer-associated fibroblast (CAF), could provide important biological and therapeutic insights. Here we identify at the single-cell level a monocyte-derived STAB1+TREM2high lipid-associated macrophage (LAM) subpopulation with immune suppressive capacities that is expanded in patients resistant to immune checkpoint blockade (ICB). Genetic depletion of this LAM subset in mice suppressed TNBC tumor growth. Flow cytometry and bulk RNA sequencing data demonstrated that coculture with TNBC-derived CAFs led to reprogramming of blood monocytes towards immune suppressive STAB1+TREM2high LAMs, which inhibit T-cell activation and proliferation. Cell-to-cell interaction modeling and assays in vitro demonstrated the role of the inflammatory CXCL12-CXCR4 axis in CAF-myeloid cell cross-talk and recruitment of monocytes in tumor sites. Altogether, these data suggest an inflammation model whereby monocytes recruited to the tumor via the CAF-driven CXCL12-CXCR4 axis acquire protumorigenic LAM capacities to support an immunosuppressive microenvironment., Significance: This work identifies a novel lipid-associated macrophage subpopulation with immune suppressive functions, offering new leads for therapeutic interventions in triple-negative breast cancer., (©2022 American Association for Cancer Research.)

Published

2022

11. A bispecific nanobody approach to leverage the potent and widely applicable tumor cytolytic capacity of Vγ9Vδ2-T cells.

Author

de Bruin RCG, Veluchamy JP, Lougheed SM, Schneiders FL, Lopez-Lastra S, Lameris R, Stam AG, Sebestyen Z, Kuball J, Molthoff CFM, Hooijberg E, Roovers RC, Santo JPD, van Bergen En Henegouwen PMP, Verheul HMW, de Gruijl TD, and van der Vliet HJ

Abstract

Though Vγ9Vδ2-T cells constitute only a small fraction of the total T cell population in human peripheral blood, they play a vital role in tumor defense and are therefore of major interest to explore for cancer immunotherapy. Vγ9Vδ2-T cell-based cancer immunotherapeutic approaches developed so far have been generally well tolerated and were able to induce significant clinical responses. However, overall results were inconsistent, possibly due to the fact that these strategies induced systemic activation of Vγ9Vδ2-T cells without preferential accumulation and targeted activation in the tumor. Here we show that a novel bispecific nanobody-based construct targeting both Vγ9Vδ2-T cells and EGFR induced potent Vγ9Vδ2-T cell activation and subsequent tumor cell lysis both in vitro and in an in vivo mouse xenograft model. Tumor cell lysis was independent of KRAS and BRAF tumor mutation status and common Vγ9Vδ2-T cell receptor sequence variations. In combination with the conserved monomorphic nature of the Vγ9Vδ2-TCR and the facile replacement of the tumor-specific nanobody, this immunotherapeutic approach can be applied to a large group of cancer patients.

Published

2017

12. A functional DC cross talk promotes human ILC homeostasis in humanized mice.

Author

Lopez-Lastra S, Masse-Ranson G, Fiquet O, Darche S, Serafini N, Li Y, Dusséaux M, Strick-Marchand H, and Di Santo JP

Abstract

Humanized mice harboring human hematopoietic systems offer a valuable small-animal model to assess human immune responses to infection, inflammation, and cancer. Human immune system (HIS) mice develop a broad repertoire of antigen receptor bearing B and T cells that can participate in adaptive immune responses after immunization. In contrast, analysis of innate immune components, including innate lymphoid cells (ILCs) and natural killer (NK) cells, is limited in current HIS mouse models, partly because of the poor development of these rare lymphoid subsets. Here we show that novel dendritic cell (DC)-boosted BALB/c Rag2 -/- Il2rg -/- Sirpa NOD Flk2 -/- (BRGSF) HIS mice harbor abundant NK cells and tissue-resident ILC subsets in lymphoid and nonlymphoid mucosal sites. We find that human NK cells and ILCs are phenotypically and functionally mature and provide evidence that human DC activation in BRGSF-based HIS mice can "cross talk" to human NK cells and ILCs. This novel HIS mouse model should provide the opportunity to study the immunobiology of human NK cell and ILC subsets in vivo in response to various environmental challenges., Competing Interests: Conflict-of-interest disclosure: J.P.D. is a stakeholder in AXENIS (founder, member of the executive board). The remaining authors declare no conflict of interest.

Published

2017