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1. In Situ Maturation and Tissue Adaptation of Type 2 Innate Lymphoid Cell Progenitors

Author

Zeis, Patrice, Lian, Mi, Fan, Xiying, Herman, Josip S, Hernandez, Daniela C, Gentek, Rebecca, Elias, Shlomo, Symowski, Cornelia, Knöpper, Konrad, Peltokangas, Nina, Friedrich, Christin, Doucet-Ladeveze, Remi, Kabat, Agnieszka M, Locksley, Richard M, Voehringer, David, Bajenoff, Marc, Rudensky, Alexander Y, Romagnani, Chiara, Grün, Dominic, and Gasteiger, Georg

Subjects
Biomedical and Clinical Sciences, Immunology, Stem Cell Research, Genetics, Animals, Cell Differentiation, Cells, Cultured, Female, Humans, Immunity, Innate, Interleukin-18 Receptor alpha Subunit, Lung, Lymphocytes, Lymphoid Progenitor Cells, Mice, Mice, Inbred C57BL, Promyelocytic Leukemia Zinc Finger Protein, Signal Transduction, Single-Cell Analysis, T Cell Transcription Factor 1, Transcription Factors, ILC2, ILCP, Innate lymphoid cells, Nippostrongylus Brasiliensis, bone marrow, immune system development, progenitors, single cell atlas, single-cell RNA-seq, tissue immunity
Abstract

Innate lymphoid cells (ILCs) are generated early during ontogeny and persist predominantly as tissue-resident cells. Here, we examined how ILCs are maintained and renewed within tissues. We generated a single cell atlas of lung ILC2s and found that Il18r1+ ILCs comprise circulating and tissue-resident ILC progenitors (ILCP) and effector-cells with heterogeneous expression of the transcription factors Tcf7 and Zbtb16, and CD103. Our analyses revealed a continuous differentiation trajectory from Il18r1+ ST2- ILCPs to Il18r- ST2+ ILC2s, which was experimentally validated. Upon helminth infection, recruited and BM-derived cells generated the entire spectrum of ILC2s in parabiotic and shield chimeric mice, consistent with their potential role in the renewal of tissue ILC2s. Our findings identify local ILCPs and reveal ILCP in situ differentiation and tissue adaptation as a mechanism of ILC maintenance and phenotypic diversification. Local niches, rather than progenitor origin, or the developmental window during ontogeny, may dominantly imprint ILC phenotypes in adult tissues.

Published
2020

3. Convergent evolution of monocyte differentiation in adult skin instructs Langerhans cell identity.

Author

Appios, Anna, Davies, James, Sirvent, Sofia, Henderson, Stephen, Trzebanski, Sébastien, Schroth, Johannes, Law, Morven L., Carvalho, Inês Boal, Pinto, Marlene Magalhaes, Carvalho, Cyril, Kan, Howard Yuan-Hao, Lovlekar, Shreya, Major, Christina, Vallejo, Andres, Hall, Nigel J., Ardern-Jones, Michael, Liu, Zhaoyuan, Ginhoux, Florent, Henson, Sian M., and Gentek, Rebecca

Subjects
LANGERHANS cells, HAIR follicles, DENDRITIC cells, SKIN innervation, PHAGOCYTES
Abstract

Langerhans cells (LCs) are distinct among phagocytes, functioning both as embryo-derived, tissue-resident macrophages in skin innervation and repair and as migrating professional antigen-presenting cells, a function classically assigned to dendritic cells (DCs). Here, we demonstrate that both intrinsic and extrinsic factors imprint this dual identity. Using ablation of embryo-derived LCs in the murine adult skin and tracking differentiation of incoming monocyte-derived replacements, we found intrinsic intraepidermal heterogeneity. We observed that ontogenically distinct monocytes give rise to LCs. Within the epidermis, Jagged-dependent activation of Notch signaling, likely within the hair follicle niche, provided an initial site of LC commitment before metabolic adaptation and survival of monocyte-derived LCs. In the human skin, embryo-derived LCs in newborns retained transcriptional evidence of their macrophage origin, but this was superseded by DC-like immune modules after postnatal expansion. Thus, adaptation to adult skin niches replicates conditioning of LC at birth, permitting repair of the embryo-derived LC network. Editor's summary: Langerhans cells (LCs) are specialized skin-resident antigen-presenting cells that not only share developmental origins with tissue-resident macrophages but also acquire the dendritic cell–like ability to migrate to draining lymph nodes. How this dual LC identity is imprinted and maintained is not completely understood. Using a mouse model of adult LC repopulation, Appios et al. found that both the developmental origin of repopulating monocytes and epidermal niche signaling imprint LC identity. A subset of infiltrating monocytes underwent stepwise differentiation involving loss of Zeb2-regulated macrophage identity, Jagged/Notch-dependent imprinting of LC fate, and survival signals in the epidermis. Similar developmental programs were detected among human embryo–derived LCs in postnatal skin. Together, these findings identify intrinsic and extrinsic factors guiding LC specification in the skin. —Claire Olingy [ABSTRACT FROM AUTHOR]

Published
2024
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5. Correction: Landscape of mast cell populations across organs in mice and humans

Author

Tauber, Marie, primary, Basso, Lilian, additional, Martin, Jeremy, additional, Bostan, Luciana, additional, Pinto, Marlene Magalhaes, additional, Thierry, Guilhem R., additional, Houmadi, Raïssa, additional, Serhan, Nadine, additional, Loste, Alexia, additional, Blériot, Camille, additional, Kamphuis, Jasper B.J., additional, Grujic, Mirjana, additional, Kjellén, Lena, additional, Pejler, Gunnar, additional, Paul, Carle, additional, Dong, Xinzhong, additional, Galli, Stephen J., additional, Reber, Laurent L., additional, Ginhoux, Florent, additional, Bajenoff, Marc, additional, Gentek, Rebecca, additional, and Gaudenzio, Nicolas, additional

Published
2024
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7. Landscape of mast cell populations across organs in mice and humans

Author

Tauber, Marie, primary, Basso, Lilian, additional, Martin, Jeremy, additional, Bostan, Luciana, additional, Pinto, Marlene Magalhaes, additional, Thierry, Guilhem R., additional, Houmadi, Raïssa, additional, Serhan, Nadine, additional, Loste, Alexia, additional, Blériot, Camille, additional, Kamphuis, Jasper B.J., additional, Grujic, Mirjana, additional, Kjellén, Lena, additional, Pejler, Gunnar, additional, Paul, Carle, additional, Dong, Xinzhong, additional, Galli, Stephen J., additional, Reber, Laurent L., additional, Ginhoux, Florent, additional, Bajenoff, Marc, additional, Gentek, Rebecca, additional, and Gaudenzio, Nicolas, additional

Published
2023
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9. Landscape of mast cell populations across organs in mice and humans

Author

Tauber, Marie, Basso, Lilian, Martin, Jeremy, Bostan, Luciana, Pinto, Marlene Magalhaes, Thierry, Guilhem R., Houmadi, Raissa, Serhan, Nadine, Loste, Alexia, Bleriot, Camille, Kamphuis, Jasper, Grujic, Mirjana, Kjellén, Lena, Pejler, Gunnar, Paul, Carle, Dong, Xinzhong, Galli, Stephen J., Reber, Laurent L., Ginhoux, Florent, Bajenoff, Marc, Gentek, Rebecca, Gaudenzio, Nicolas, Tauber, Marie, Basso, Lilian, Martin, Jeremy, Bostan, Luciana, Pinto, Marlene Magalhaes, Thierry, Guilhem R., Houmadi, Raissa, Serhan, Nadine, Loste, Alexia, Bleriot, Camille, Kamphuis, Jasper, Grujic, Mirjana, Kjellén, Lena, Pejler, Gunnar, Paul, Carle, Dong, Xinzhong, Galli, Stephen J., Reber, Laurent L., Ginhoux, Florent, Bajenoff, Marc, Gentek, Rebecca, and Gaudenzio, Nicolas

Abstract

Mast cells (MCs) are tissue-resident immune cells that exhibit homeostatic and neuron-associated functions. Here, we combined whole-tissue imaging and single-cell RNA sequencing datasets to generate a pan-organ analysis of MCs in mice and humans at steady state. In mice, we identify two mutually exclusive MC populations, MrgprB2(+) connective tissue-type MCs and MrgprB2(neg) mucosal-type MCs, with specific transcriptomic core signatures. While MrgprB2(+) MCs develop in utero independently of the bone marrow, MrgprB2(neg) MCs develop after birth and are renewed by bone marrow progenitors. In humans, we unbiasedly identify seven MC subsets (MC1-7) distributed across 12 organs with different transcriptomic core signatures. MC1 are preferentially enriched in the bladder, MC2 in the lungs, and MC4, MC6, and MC7 in the skin. Conversely, MC3 and MC5 are shared by most organs but not skin. This comprehensive analysis offers valuable insights into the natural diversity of MC subtypes in both mice and humans. Combining whole-tissue imaging and single-cell RNA sequencing datasets, Tauber et al. present a pan-organ analysis of mast cells in mice and humans at steady state, revealing an unexpected heterogeneity of mast cell populations across tissues and species.

Published
2023
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11. CSF1R-dependent macrophages in the salivary gland are essential for epithelial regeneration after radiation-induced injury.

Author

McKendrick, John G., Jones, Gareth-Rhys, Elder, Sonia S., Watson, Erin, T'Jonck, Wouter, Mercer, Ella, Magalhaes, Marlene S., Rocchi, Cecilia, Hegarty, Lizi M., Johnson, Amanda L., Schneider, Christoph, Becher, Burkhard, Pridans, Clare, Mabbott, Neil, Liu, Zhaoyuan, Ginhoux, Florent, Bajenoff, Marc, Gentek, Rebecca, Bain, Calum C., and Emmerson, Elaine

Subjects
SALIVARY glands, MACROPHAGES, REGENERATION (Biology), ONTOGENY, HEAD & neck cancer, EPITHELIAL cells, DOSE-response relationship (Radiation)
Abstract

The salivary glands often become damaged in individuals receiving radiotherapy for head and neck cancer, resulting in chronic dry mouth. This leads to detrimental effects on their health and quality of life, for which there is no regenerative therapy. Macrophages are the predominant immune cell in the salivary glands and are attractive therapeutic targets due to their unrivaled capacity to drive tissue repair. Yet, the nature and role of macrophages in salivary gland homeostasis and how they may contribute to tissue repair after injury are not well understood. Here, we show that at least two phenotypically and transcriptionally distinct CX3CR1+ macrophage populations are present in the adult salivary gland, which occupy anatomically distinct niches. CD11c+CD206CD163 macrophages typically associate with gland epithelium, whereas CD11cCD206+CD163+ macrophages associate with blood vessels and nerves. Using a suite of complementary fate mapping systems, we show that there are highly dynamic changes in the ontogeny and composition of salivary gland macrophages with age. Using an in vivo model of radiation-induced salivary gland injury combined with genetic or antibody-mediated depletion of macrophages, we demonstrate an essential role for macrophages in clearance of cells with DNA damage. Furthermore, we show that epithelial-associated macrophages are indispensable for effective tissue repair and gland function after radiation-induced injury, with their depletion resulting in reduced saliva production. Our data, therefore, provide a strong case for exploring the therapeutic potential of manipulating macrophages to promote tissue repair and thus minimize salivary gland dysfunction after radiotherapy. Editor's summary: Radiation therapy is an effective treatment for head and neck cancer but comes with a wide range of side effects, including chronic dry mouth. McKendrick et al. investigated the role of macrophages in salivary glands to better understand their response to radiation and how they can be targeted to restore function. They identified two transcriptionally distinct CX3CR1+ macrophage subsets in salivary glands of adult mice. The gland epithelium was enriched for CD11c+CD206CD163 macrophages, whereas CD11cCD206+CD163+ macrophages localized to blood vessels and nerves. A mouse model of radiation-induced salivary gland injury confirmed that this treatment changes the composition and longevity of macrophage subsets at this site, but epithelium-associated CD11c+CD206CD163 macrophages specifically are required for epithelial cell regeneration after injury. These findings provide insights into salivary gland responses to irradiation and can guide future therapies. —Christiana Fogg [ABSTRACT FROM AUTHOR]

Published
2023
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14. SIRT1 regulates macrophage self‐renewal

Author

Imperatore, Francesco, Maurizio, Julien, Vargas Aguilar, Stephanie, Busch, Clara J, Favret, Jérémy, Kowenz‐Leutz, Elisabeth, Cathou, Wilfried, Gentek, Rebecca, Perrin, Pierre, Leutz, Achim, Berruyer, Carole, and Sieweke, Michael H

Published
2017
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15. Single-cell analysis of mast cell populations across organs reveals insights into cell origins, anatomical niches and neuron-associated functions.

Author

Gaudenzio, Nicolas, primary, Tauber, Marie, additional, Basso, Lilian, additional, Wemelle, Eve, additional, Martin, Jeremy, additional, Bostan, Luciana, additional, Pinto, Marlene Magalhaes, additional, Thierry, Guilhem, additional, Houmadi, Raissa, additional, Serhan, Nadine, additional, Loste, Alexia, additional, Bleriot, Camille, additional, Samrout, Celine El, additional, Lasrado, Reena, additional, Kamphuis, Jasper, additional, Pachnis, Vassilis, additional, Grujic, Mirjana, additional, Kjellén, Lena, additional, Pejler, Gunnar, additional, Paul, Carle, additional, Dong, Xinzhong, additional, Galli, Stephen, additional, Reber, Laurent, additional, Ginhoux, Florent, additional, Bajenoff, Marc, additional, Gentek, Rebecca, additional, and Knauff, Claude, additional

Published
2022
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16. CSF1R-dependent macrophages in the salivary gland are essential for epithelial regeneration following radiation-induced injury

Author

McKendrick, John G, primary, Jones, Gareth-Rhys, additional, Elder, Sonia S, additional, Mercer, Ella, additional, Magalhaes, Marlene S, additional, Rocchi, Cecilia, additional, Hegarty, Lizi M, additional, Johnson, Amanda L, additional, Schneider, Christoph, additional, Becher, Burkhard, additional, Pridans, Clare, additional, Mabbott, Neil A, additional, Liu, Zhaoyuan, additional, Ginhoux, Florent, additional, Bajenoff, Marc, additional, Gentek, Rebecca, additional, Bain, Calum C, additional, and Emmerson, Elaine, additional

Published
2022
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17. Developmental programming of macrophages by early life adversity

Author

Magalhaes, Marlene S., Potter, Harry, Ahlback, Anna, Gentek, Rebecca, Magalhaes, Marlene S., Potter, Harry, Ahlback, Anna, and Gentek, Rebecca

Abstract

Macrophages are central elements of all organs, where they have a multitude of physiological and pathological functions. The first macrophages are produced during fetal development, and most adult organs retain populations of fetal-derived macrophages that self-maintain without major input of hematopoietic stem cell-derived monocytes. Their developmental origins make macrophages highly susceptible to environmental perturbations experienced in early life, in particular the fetal period. It is now well recognized that such adverse developmental conditions contribute to a wide range of diseases later in life. This chapter explores the notion that macrophages are key targets of environmental adversities during development, and mediators of their long-term impact on health and disease. We first briefly summarize our current understanding of macrophage ontogeny and their biology in tissues and consider potential mechanisms by which environmental stressors may mediate fetal programming. We then review evidence for programming of macrophages by adversities ranging from maternal immune activation and diet to environmental pollutants and toxins, which have disease relevance for different organ systems. Throughout this chapter, we contemplate appropriate experimental strategies to study macrophage programming. We conclude by discussing how our current knowledge of macrophage programming could be conceptualized, and finally highlight open questions in the field and approaches to address them.

Published
2022

18. Mast cell ontogeny: From fetal development to life-long health and disease.

Author

Shin Li Chia, Kapoor, Simran, Carvalho, Cyril, Bajénoff, Marc, and Gentek, Rebecca

Subjects
MAST cells, MAST cell disease, FETAL development, CYTOLOGY, MYELOID cells, FETAL tissues, ONTOGENY
Abstract

Mast cells (MCs) are evolutionarily ancient innate immune cells with important roles in protective immunity against bacteria, parasites, and venomous animals. They can be found in most organs of the body, where they also contribute to normal tissue functioning, for example by engaging in crosstalk with nerves. Despite this, they are most widely known for their detrimental roles in allergy, anaphylaxis, and atopic disease. Just like macrophages, mast cells were conventionally thought to originate from the bone marrow. However, they are already present in fetal tissues before the onset of bone marrow hematopoiesis, questioning this dogma. In recent years, our view of myeloid cell ontogeny has been revised. We now know that the first mast cells originate from progenitors made in the extra-embryonic yolk sac, and later get supplemented with mast cells produced from subsequent waves of hematopoiesis. In most connective tissues, sizeable populations of fetal-derived mast cells persist into adulthood, where they self-maintain largely independently from the bone marrow. These developmental origins are highly reminiscent of macrophages, which are known to have critical functions in development. Mast cells too may thus support healthy development. Their fetal origins and longevity also make mast cells susceptible to genetic and environmental perturbations, which may render them pathological. Here, we review our current understanding of mast cell biology from a developmental perspective. We first summarize how mast cell populations are established from distinct hematopoietic progenitor waves, and how they are subsequently maintained throughout life. We then discuss what functions mast cells may normally have at early life stages, and how they may be co-opted to cause, worsen, or increase susceptibility to disease. [ABSTRACT FROM AUTHOR]

Published
2023
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24. Comment on “Tumor-initiating cells establish an IL-33–TGF-β niche signaling loop to promote cancer progression”

Author

Kamphuis, Jasper B. J., primary, Worrall, William P. M., additional, Stackowicz, Julien, additional, Mougel, Aurélie, additional, Mauré, Emilie, additional, Conde, Eva, additional, Bruhns, Pierre, additional, Guilleminault, Laurent, additional, Gaudenzio, Nicolas, additional, Chen, Jinmiao, additional, Gentek, Rebecca, additional, and Reber, Laurent L., additional

Published
2021
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28. Distinct Waves from the Hemogenic Endothelium Give Rise to Layered Lymphoid Tissue Inducer Cell Ontogeny

Author

Simic, Milesa, primary, Manosalva, Iris, additional, Spinelli, Lionel, additional, Gentek, Rebecca, additional, Shayan, Raheleh R., additional, Siret, Carole, additional, Girard-Madoux, Mathilde, additional, Wang, Shuaiwei, additional, de Fabritus, Lauriane, additional, Verschoor, Janneke, additional, Kerdiles, Yann M., additional, Bajenoff, Marc, additional, Stumm, Ralf, additional, Golub, Rachel, additional, and van de Pavert, Serge A., additional

Published
2020
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30. Remodeling of reactive lymph nodes: Dynamics of stromal cells and underlying chemokine signaling

Author

Thierry, Guilhem R., Gentek, Rebecca, Bajenoff, Marc, Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), and ANR-17-CE15-0015,StroMAC,Cross-talk des macrophages et du stroma au sein du ganglion lymphatique(2017)

Subjects
0301 basic medicine, Chemokine, Stromal cell, Lymphocyte, Immunology, Inflammation, [SDV.IMM.II]Life Sciences [q-bio]/Immunology/Innate immunity, 03 medical and health sciences, 0302 clinical medicine, Immune system, Stroma, Antigen, Cell Movement, medicine, Animals, Homeostasis, Humans, Immunology and Allergy, Lymphocytes, ComputingMilieux_MISCELLANEOUS, Immunity, Cellular, biology, Cell biology, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Lymph Nodes, Lymph, Chemokines, Stromal Cells, medicine.symptom, Signal Transduction, 030215 immunology
Abstract

Lymph nodes (LNs) are secondary immune organs dispersed throughout the body. They are primarily composed of lymphocytes, "transient passengers" that are only present for a few hours. During this time, they extensively interact with a meshwork of stromal cells. Although these cells constitute less than 5% of all LN cells, they are integral to LN function: Stromal cells create a three-dimensional network that provides a rigid backbone for the transport of lymph and generates "roads" for lymphocyte migration. Beyond structural support, the LN stroma also produces survival signals for lymphocytes and provides nutrients, soluble factors, antigens, and immune cells collectively required for immune surveillance and the generation of adaptive immune responses. A unique feature of LNs is their ability to considerably and rapidly change size: the volume and cellularity of inflamed LNs can increase up to 20-fold before returning to homeostatic levels. This cycle will be repeated many times during life and is accommodated by stromal cells. The dynamics underlying this dramatic remodeling are subject of this review. We will first introduce the main types of LN stromal cells and explain their known functions. We will then discuss how these cells enable LN growth during immune responses, with a particular focus on underlying cellular mechanisms and molecular cues. Similarly, we will elaborate on stromal dynamics mediating the return to LN homeostasis, a process that is mechanistically much less understood than LN expansion.

Published
2019
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31. Epidermal gamma delta T cells originate from yolk sac hematopoiesis and clonally self-renew in the adult

Author

Gentek, Rebecca, Ghigo, Clement, Hoeffel, Guillaume, Jorquera, Audrey, Msallam, Rasha, Wienert, Stephan, Klauschen, Frederick, Ginhoux, Florent, Bajenoff, Marc, Centre d'Immunologie de Marseille - Luminy (CIML), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU), and Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)

Subjects
integumentary system, [SDV.IMM]Life Sciences [q-bio]/Immunology
Abstract

The murine epidermis harbors two immune cell lineages, Langerhans cells (LCs) and gamma delta T cells known as dendritic epidermal T cells (DETCs). LCs develop from both early yolk sac (YS) progenitors and fetal liver monocytes before locally self-renewing in the adult. For DETCs, the mechanisms of homeostatic maintenance and their hematopoietic origin are largely unknown. Here, we exploited multicolor fate mapping systems to reveal that DETCs slowly turn over at steady state. Like for LCs, homeostatic maintenance of DETCs is achieved by clonal expansion of tissue-resident cells assembled in proliferative units. The same mechanism, albeit accelerated, facilitates DETC replenishment upon injury. Hematopoietic lineage tracing uncovered that DETCs are established independently of definitive hematopoietic stem cells and instead originate from YS hematopoiesis, again reminiscent of LCs. DETCs thus resemble LCs concerning their maintenance, replenishment mechanisms, and hematopoietic development, suggesting that the epidermal microenvironment exerts a lineage-independent influence on the initial seeding and homeostatic maintenance of its resident immune cells.

Published
2018

32. Origin and microenvironment contribute to the sexually dimorphic phenotype and function of peritoneal macrophages

Author

Bain, Calum C., primary, Gibson, Douglas A., additional, Steers, Nicholas, additional, Boufea, Katarina, additional, Louwe, Pieter A., additional, Docherty, Catherine, additional, Huici, Victor, additional, Gentek, Rebecca, additional, Magalhaes-Pinto, Marlene, additional, Bajenoff, Marc, additional, Benezech, Cecile, additional, Dockrell, David, additional, Saunders, Philippa TK, additional, Batada, Nizar, additional, and Jenkins, Stephen J, additional

Published
2019
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34. Two distinct interstitial macrophage populations coexist across tissues in specific subtissular niches

Author

Chakarov, Svetoslav, primary, Lim, Hwee Ying, additional, Tan, Leonard, additional, Lim, Sheau Yng, additional, See, Peter, additional, Lum, Josephine, additional, Zhang, Xiao-Meng, additional, Foo, Shihui, additional, Nakamizo, Satoshi, additional, Duan, Kaibo, additional, Kong, Wan Ting, additional, Gentek, Rebecca, additional, Balachander, Akhila, additional, Carbajo, Daniel, additional, Bleriot, Camille, additional, Malleret, Benoit, additional, Tam, John Kit Chung, additional, Baig, Sonia, additional, Shabeer, Muhammad, additional, Toh, Sue-Anne Ee Shiow, additional, Schlitzer, Andreas, additional, Larbi, Anis, additional, Marichal, Thomas, additional, Malissen, Bernard, additional, Chen, Jinmiao, additional, Poidinger, Michael, additional, Kabashima, Kenji, additional, Bajenoff, Marc, additional, Ng, Lai Guan, additional, Angeli, Veronique, additional, and Ginhoux, Florent, additional

Published
2019
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35. Developmental origin and maintenance of distinct testicular macrophage populations

Author

Mossadegh-Keller, Noushin, Gentek, Rebecca, Gimenez, Gregory, Bigot, Sylvain, Mailfert, Sebastien, Sieweke, Michael H., Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Max Delbrück Centrum für Molekulare Medizin (MDC), ANR-10-INBS-0004,France-BioImaging,Développment d'une infrastructure française distribuée coordonnée(2010), ANR-11-BSV3-0026,ReNEW,Mecanismes d'autorenouvellement des macrophages differencies(2011), European Project: 695093,MacAge, Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU), and Max-Delbrück-Centrum für Molekulare Medizin in der Helmholtzgemeinschaft, 13125 Berlin, Germany

Subjects
Male, Cancer Research, Testicular macrophage populations, Cell Proliferation/physiology, Real-Time Polymerase Chain Reaction, Mice, Testis, Animals, Immunity, Cellular/physiology, Spermatogenesis, Testis/cytology, Research Articles, Cell Proliferation, Immunity, Cellular, Gene Expression Profiling, Macrophages, Stem Cells, Immune cells, Brief Definitive Report, Macrophages/cytology, Flow Cytometry, Testicular macrophages (tM phi), Stem Cells/physiology, Mice, Inbred C57BL, [SDV.IMM]Life Sciences [q-bio]/Immunology, Spermatogenesis/physiology
Abstract

Mossadegh-Keller et al. show distinct origin of two different testicular macrophage populations during the postnatal development. Embryonic precursors give rise exclusively to the interstitial macrophage population, whereas peritubular macrophages derive from bone marrow progenitors only postnatally. Surprisingly, both macrophage populations display a remarkable long life span., Testicular macrophages (tMφ) are the principal immune cells of the mammalian testis. Beyond classical immune functions, they have been shown to be important for organogenesis, spermatogenesis, and male hormone production. In the adult testis, two different macrophage populations have been identified based on their distinct tissue localization and morphology, but their developmental origin and mode of homeostatic maintenance are unknown. In this study, we use genetic lineage–tracing models and adoptive transfer protocols to address this question. We show that embryonic progenitors give rise to the interstitial macrophage population, whereas peritubular macrophages are exclusively seeded postnatally in the prepuberty period from bone marrow (BM)–derived progenitors. As the proliferative capacity of interstitial macrophages declines, BM progenitors also contribute to this population. Once established, both the peritubular and interstitial macrophage populations exhibit a long life span and a low turnover in the steady state. Our observations identify distinct developmental pathways for two different tMφ populations that have important implications for the further dissection of their distinct roles in organ homeostasis and testicular function.

Published
2017

41. A central role for Notch in effector CD8+ T cell differentiation

Author

Backer, Ronald A, primary, Helbig, Christina, additional, Gentek, Rebecca, additional, Kent, Andrew, additional, Laidlaw, Brian J, additional, Dominguez, Claudia X, additional, de Souza, Yevan S, additional, van Trierum, Stella E, additional, van Beek, Ruud, additional, Rimmelzwaan, Guus F, additional, ten Brinke, Anja, additional, Willemsen, A Marcel, additional, van Kampen, Antoine H C, additional, Kaech, Susan M, additional, Blander, J Magarian, additional, van Gisbergen, Klaas, additional, and Amsen, Derk, additional

Published
2014
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43. A central role for Notch in effector CD8+ T cell differentiation.

Author

Backer, Ronald A, Helbig, Christina, Gentek, Rebecca, Kent, Andrew, Laidlaw, Brian J, Dominguez, Claudia X, de Souza, Yevan S, van Trierum, Stella E, van Beek, Ruud, Rimmelzwaan, Guus F, ten Brinke, Anja, Willemsen, A Marcel, van Kampen, Antoine H C, Kaech, Susan M, Blander, J Magarian, van Gisbergen, Klaas, and Amsen, Derk

Subjects
T cell differentiation, NOTCH proteins, CELLULAR signal transduction, INFLUENZA viruses, GENE expression, PROGENITOR cells, INTERLEUKIN-2, INFLAMMATORY mediators
Abstract

Activated CD8+ T cells choose between terminal effector cell (TEC) or memory precursor cell (MPC) fates. We found that the signaling receptor Notch controls this 'choice'. Notch promoted the differentiation of immediately protective TECs and was correspondingly required for the clearance of acute infection with influenza virus. Notch activated a major portion of the TEC-specific gene-expression program and suppressed the MPC-specific program. Expression of Notch was induced on naive CD8+ T cells by inflammatory mediators and interleukin 2 (IL-2) via pathways dependent on the metabolic checkpoint kinase mTOR and the transcription factor T-bet. These pathways were subsequently amplified downstream of Notch, creating a positive feedback loop. Notch thus functions as a central hub where information from different sources converges to match effector T cell differentiation to the demands of an infection. [ABSTRACT FROM AUTHOR]

Published
2014
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44. TECHNICAL COMMENT ABSTRACTS.

Author

Kamphuis, Jasper B. J., Worrall, William P. M., Stackowicz, Julien, Mougel, Aurélie, Mauré, Emilie, Conde, Eva, Bruhns, Pierre, Guilleminault, Laurent, Gaudenzio, Nicolas, Chen, Jinmiao, Gentek, Rebecca, Reber, Laurent L., Taniguchi, Sachiko, Elhance, Ajit, Duzer, Avery Van, Kumar, Sushil, Leitenberger, Justin, and Oshimori, Naoki

Published
2021

45. Fate-Mapping Macrophages: From Ontogeny to Functions.

Author

Ahlback A and Gentek R

Subjects
Monocytes cytology, Hematopoietic Stem Cells cytology, Animals, Mice, Cell Differentiation, Macrophages cytology, Cell Lineage, Genetic Markers
Abstract

Macrophages are vital to the physiological function of most tissues, but also contribute to disease through a multitude of pathological roles. They are thus highly plastic and heterogeneous. It is now well recognized that macrophages develop from several distinct progenitors from embryogenesis onwards and extending throughout life. Tissue-resident macrophages largely originate from embryonic sources and in many cases self-maintain independently without monocyte input. However, in certain tissues, monocyte-derived macrophages replace these over time or as a result of tissue injury and inflammation. This additional layer of heterogeneity has introduced many questions regarding the influence of origin on fate and function of macrophages in health and disease. To comprehensively address these questions, appropriate methods of tracing macrophage ontogeny are required. This chapter explores why ontogeny is of vital importance in macrophage biology and how to delineate macrophage populations by origin through genetic fate mapping. First, we summarize the current view of macrophage ontogeny and briefly discuss how origin may influence macrophage function in homeostasis and pathology. We go on to make the case for genetic fate mapping as the gold standard and briefly review different fate-mapping models. We then put forward our recommendations for fate-mapping strategies best suited to answer specific research questions and finally discuss the strengths and limitations of currently available models., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published
2024
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46. Developmental programming of macrophages by early life adversity.

Author

Magalhaes MS, Potter HG, Ahlback A, and Gentek R

Subjects
Hematopoietic Stem Cells, Humans, Animals, Adverse Childhood Experiences, Macrophages
Abstract

Macrophages are central elements of all organs, where they have a multitude of physiological and pathological functions. The first macrophages are produced during fetal development, and most adult organs retain populations of fetal-derived macrophages that self-maintain without major input of hematopoietic stem cell-derived monocytes. Their developmental origins make macrophages highly susceptible to environmental perturbations experienced in early life, in particular the fetal period. It is now well recognized that such adverse developmental conditions contribute to a wide range of diseases later in life. This chapter explores the notion that macrophages are key targets of environmental adversities during development, and mediators of their long-term impact on health and disease. We first briefly summarize our current understanding of macrophage ontogeny and their biology in tissues and consider potential mechanisms by which environmental stressors may mediate fetal programming. We then review evidence for programming of macrophages by adversities ranging from maternal immune activation and diet to environmental pollutants and toxins, which have disease relevance for different organ systems. Throughout this chapter, we contemplate appropriate experimental strategies to study macrophage programming. We conclude by discussing how our current knowledge of macrophage programming could be conceptualized, and finally highlight open questions in the field and approaches to address them., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published
2022
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47. Imaging the Lymph Node Stroma.

Author

Ghigo C, Gentek R, and Bajénoff M

Subjects
Humans, Lymph Nodes ultrastructure, Microscopy, Confocal methods, Molecular Imaging methods, Stromal Cells ultrastructure
Abstract

Lymph node (LN) stromal cells are being recognized as key organizers of the immune system. They assemble in complex 3D networks and hence, need to be studied in situ to fully understand their exact functions. Here, we describe two distinct but complementary procedures that allow analyzing LN stromal cells at high resolution by confocal imaging.

Published
2018
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48. Developmental origin and maintenance of distinct testicular macrophage populations.

Author

Mossadegh-Keller N, Gentek R, Gimenez G, Bigot S, Mailfert S, and Sieweke MH

Subjects
Animals, Cell Proliferation physiology, Flow Cytometry, Gene Expression Profiling, Immunity, Cellular physiology, Macrophages cytology, Macrophages metabolism, Male, Mice, Mice, Inbred C57BL, Real-Time Polymerase Chain Reaction, Spermatogenesis physiology, Stem Cells physiology, Testis immunology, Testis metabolism, Macrophages physiology, Testis cytology
Abstract

Testicular macrophages (tMφ) are the principal immune cells of the mammalian testis. Beyond classical immune functions, they have been shown to be important for organogenesis, spermatogenesis, and male hormone production. In the adult testis, two different macrophage populations have been identified based on their distinct tissue localization and morphology, but their developmental origin and mode of homeostatic maintenance are unknown. In this study, we use genetic lineage-tracing models and adoptive transfer protocols to address this question. We show that embryonic progenitors give rise to the interstitial macrophage population, whereas peritubular macrophages are exclusively seeded postnatally in the prepuberty period from bone marrow (BM)-derived progenitors. As the proliferative capacity of interstitial macrophages declines, BM progenitors also contribute to this population. Once established, both the peritubular and interstitial macrophage populations exhibit a long life span and a low turnover in the steady state. Our observations identify distinct developmental pathways for two different tMφ populations that have important implications for the further dissection of their distinct roles in organ homeostasis and testicular function., (© 2017 Mossadegh-Keller et al.)

Published
2017
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