The Ly49E Receptor Inhibits the Immune Control of Acute Trypanosoma cruzi Infection

Filtjens, Jessica; Coltel, Nicolas; Cencig, Sabrina; Taveirne, Sylvie; Ammel, Els Van; Acker, Aline Van; Kerre, Tessa; Matthys, Patrick; Taghon, Tom; Vandekerckhove, Bart; Carlier, Yves; Truyens, Carine; Leclercq, Georges

doi:10.3389/fimmu.2016.00472

Cited by 5 publications

(4 citation statements)

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“…Studies have shown that Ly49E is not involved in several pathophysiological situations, including malaria infection ( Filtjens et al, 2014 ), chemically induced colitis ( Van Acker et al, 2016 ), and different tumors ( Filtjens et al, 2016b ). However, young Ly49E-KO mice could control the parasite infection better ( Filtjens et al, 2016a ). Although Ly49E activation by uPA, a non-MHC class I ligand ( Van Den Broeck et al, 2008 ), could inhibit the effector functions of NK cell lines or fetal thymic NK cells, freshly isolated liver group 1 ILCs from Ly49E-deficient and WT mice did not differ in cytotoxic capacity in the presence of uPA ( Filtjens et al, 2013 ).…”

Section: Discussionmentioning

confidence: 99%

Ly49E separates liver ILC1s into embryo-derived and postnatal subsets with different functions

Chen

Wang

Hao

et al. 2022

Journal of Experimental Medicine

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Type 1 innate lymphoid cells (ILC1s) represent the predominant population of liver ILCs and function as important effectors and regulators of immune responses, but the cellular heterogeneity of ILC1s is not fully understood. Here, single-cell RNA sequencing and flow cytometric analysis demonstrated that liver ILC1s could be dissected into Ly49E+ and Ly49E− populations with unique transcriptional and phenotypic features. Genetic fate-mapping analysis revealed that liver Ly49E+ ILC1s with strong cytotoxicity originated from embryonic non–bone marrow hematopoietic progenitor cells (HPCs), persisted locally during postnatal life, and mediated protective immunity against cytomegalovirus infection in newborn mice. However, Ly49E− ILC1s developed from BM and extramedullary HPCs after birth, gradually replaced Ly49E+ ILC1s in the livers with age, and contained the memory subset in recall response to hapten challenge. Thus, our study shows that Ly49E dissects liver ILC1s into two unique subpopulations, with distinct origins and a bias toward neonatal innate or adult immune memory responses.

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Section: Discussionmentioning

confidence: 99%

Ly49E separates liver ILC1s into embryo-derived and postnatal subsets with different functions

Chen

Wang

Hao

et al. 2022

Journal of Experimental Medicine

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“…Liver trNK cells in mice are also functionally unique as they exhibit a higher level of baseline activation relative to splenic or liver cNK cells ( 56 ). They are larger and more granular, and express Ly49E, which mediates responses to liver-specific infections such as T. cruzi ( 173 ). Cytokine release is more efficient from these cells, TNFα, GM-CSF and IL-2 are all increased, and their high expression of TRAIL and FasL makes them better at inducing target cell apoptosis by alternative killing.…”

Section: Integrins As Markers For Residencymentioning

confidence: 99%

Natural Killer Cell Integrins and Their Functions in Tissue Residency

Shannon

Mace

2021

Front. Immunol.

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Integrins are transmembrane receptors associated with adhesion and migration and are often highly differentially expressed receptors amongst natural killer cell subsets in microenvironments. Tissue resident natural killer cells are frequently defined by their differential integrin expression compared to other NK cell subsets, and integrins can further localize tissue resident NK cells to tissue microenvironments. As such, integrins play important roles in both the phenotypic and functional identity of NK cell subsets. Here we review the expression of integrin subtypes on NK cells and NK cell subsets with the goal of better understanding how integrin selection can dictate tissue residency and mediate function from the nanoscale to the tissue environment.

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“…At 6–7 weeks post-injection, the mice were sacrificed by cervical dislocation and perfused with PBS. Single-cell suspensions of liver, spleen, bone marrow, and intestinal LPL were generated as previously described ( Van Acker et al, 2017 ; Filtjens et al, 2016 ; Filtjens et al, 2013 ). Lungs were cut in pieces and digested in RPMI1640 (Life Technologies) supplemented with 2% FCS, collagenase D (2 mg/mL, Roche), and Dnase I (0.2 mg/mL, Roche).…”

Section: Methodsmentioning

confidence: 99%

The transcription factor RUNX2 drives the generation of human NK cells and promotes tissue residency

Wahlen

Matthijssens

Loocke

et al. 2022

eLife

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Natural killer (NK) cells are innate lymphocytes that eliminate virus-infected and cancer cells by cytotoxicity and cytokine secretion. In addition to circulating NK cells, distinct tissue-resident NK subsets have been identified in various organs. Although transcription factors regulating NK cell development and function have been extensively studied in mice, the role of RUNX2 in these processes has not been investigated, neither in mice nor in human. Here, by manipulating RUNX2 expression with either knockdown or overexpression in human haematopoietic stem cell-based NK cell differentiation cultures, combined with transcriptomic and ChIP-sequencing analyses, we established that RUNX2 drives the generation of NK cells, possibly through induction of IL-2Rβ expression in NK progenitor cells. Importantly, RUNX2 promotes tissue residency in human NK cells. Our findings have the potential to improve existing NK cell-based cancer therapies and can impact research fields beyond NK cell biology, since tissue-resident subsets have also been described in other lymphocyte subpopulations.

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The Ly49E Receptor Inhibits the Immune Control of Acute Trypanosoma cruzi Infection

Cited by 5 publications

References 50 publications

Ly49E separates liver ILC1s into embryo-derived and postnatal subsets with different functions

Ly49E separates liver ILC1s into embryo-derived and postnatal subsets with different functions

Natural Killer Cell Integrins and Their Functions in Tissue Residency

The transcription factor RUNX2 drives the generation of human NK cells and promotes tissue residency

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