CD45RA
            <sup>+</sup>
            CD62L
            <sup>−</sup>
            ILCs in human tissues represent a quiescent local reservoir for the generation of differentiated ILCs

Kokkinou, Efthymia; Pandey, Ram Vinay; Mazzurana, Luca; Gutiérrez-Pérez, Irene; Tibbitt, Christopher A.; Weigel, Whitney; Soini, Tea; Carrasco, Anna; Rao, Anna; Nagasawa, Maho; Bal, Suzanne M.; Jangard, Mattias; Friberg, Danielle; Lindforss, Ulrik; Nordenvall, Caroline; Ljunggren, Malin; Haapaniemi, Staffan; Keita, Åsa V.; Söderholm, Johan D.; Hedin, Charlotte; Spits, Hergen; Bryceson, Yenan T.; Mjösberg, Jenny

doi:10.1126/sciimmunol.abj8301

Cited by 19 publications

(13 citation statements)

References 73 publications

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“…Moreover, the authors demonstrated an accumulation of a CD62Lsubpopulation of CD45RA + ILCp in the inflamed mucosa of patients with both UC and CD. The expansion of CD26L -ILCp was found to be inversely proportional to the frequency of NKp44 + ILC3s, suggesting that disruptions to ILCp compartments may act to promote the disequilibrium of ILCs observed in IBD (67).…”

Section: Ilc1 In Intestinal Inflammationmentioning

confidence: 94%

“…While a question remains as to what extent this may impact IBD pathogenesis (65), it is notable that such a switch was additionally observed in the population of ILC precursors (ILCp); an increase in NKp44 + and CD56 + ILCp was detected in CD patients, coupled to a decrease in their corresponding naïve CD45RA + ILCp (64). However, while circulating human ILCp has been shown to contribute to the pool of ILCs in tissues (66), the extent to which perturbations in peripheral ILCp in IBD patents may impact the ILC compartment within the intestinal mucosae remains to be determined-for example, recent research has shown that CD45RA + ILCp exhibits tissue-specific differentiation potential (67). Moreover, the authors demonstrated an accumulation of a CD62Lsubpopulation of CD45RA + ILCp in the inflamed mucosa of patients with both UC and CD.…”

Section: Ilc1 In Intestinal Inflammationmentioning

confidence: 99%

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Helper-Like Type-1 Innate Lymphoid Cells in Inflammatory Bowel Disease

et al. 2022

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Inflammatory bowel disease (IBD) is an idiopathic condition characterized by chronic relapsing inflammation in the intestine. While the precise etiology of IBD remains unknown, genetics, the gut microbiome, environmental factors, and the immune system have all been shown to contribute to the disease pathophysiology. In recent years, attention has shifted towards the role that innate lymphoid cells (ILCs) may play in the dysregulation of intestinal immunity observed in IBD. ILCs are a group of heterogenous immune cells which can be found at mucosal barriers. They act as critical mediators of the regulation of intestinal homeostasis and the orchestration of its inflammatory response. Despite helper-like type 1 ILCs (ILC1s) constituting a particularly rare ILC population in the intestine, recent work has suggested that an accumulation of intestinal ILC1s in individuals with IBD may act to exacerbate its pathology. In this review, we summarize existing knowledge on helper-like ILC1 plasticity and their classification in murine and human settings. Moreover, we discuss what is currently understood about the roles that ILC1s may play in the progression of IBD pathogenesis.

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Section: Ilc1 In Intestinal Inflammationmentioning

confidence: 94%

Section: Ilc1 In Intestinal Inflammationmentioning

confidence: 99%

Helper-Like Type-1 Innate Lymphoid Cells in Inflammatory Bowel Disease

et al. 2022

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“…It is suggested that the blood-circulating ILCPs could provide “on-demand” replenishment of ILC subsets in the inflamed sites as their niche to differentiate and propagate, which makes a clear contrast to naïve T cells in the lymph node (LN). However, ILCPs harbor differentiation potential into ILC subsets (e.g., ILC1/2/3 with T-bet/Gata-3/RORγt expression functionally reminiscent of Th1/2/17) and a quiescent state with reduced glycolysis and mitochondrial activity, without effector cytokine production or extensive proliferation, which all associate with the characteristics of naïve T cells ( 59 ). This tempts us to speculate that the biological significance of the blood-circulating ILCPs may be an innate counterpart of naïve T cells, which differentiate into helper and cytotoxic T cells of the acquired immune system.…”

Section: Variation Of the Ontogeny Of Ilcsmentioning

confidence: 99%

Waves of layered immunity over innate lymphoid cells

et al. 2022

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Innate lymphoid cells (ILCs) harbor tissue-resident properties in border zones, such as the mucosal membranes and the skin. ILCs exert a wide range of biological functions, including inflammatory response, maintenance of tissue homeostasis, and metabolism. Since its discovery, tremendous effort has been made to clarify the nature of ILCs, and scientific progress revealed that progenitor cells of ILC can produce ILC subsets that are functionally reminiscent of T-cell subsets such as Th1, Th2, and Th17. Thus, now it comes to the notion that ILC progenitors are considered an innate version of naïve T cells. Another important discovery was that ILC progenitors in the different tissues undergo different modes of differentiation pathways. Furthermore, during the embryonic phase, progenitor cells in different developmental chronologies give rise to the unique spectra of immune cells and cause a wave to replenish the immune cells in tissues. This observation leads to the concept of layered immunity, which explains the ontology of some cell populations, such as B-1a cells, γδ T cells, and tissue-resident macrophages. Thus, recent reports in ILC biology posed a possibility that the concept of layered immunity might disentangle the complexity of ILC heterogeneity. In this review, we compare ILC ontogeny in the bone marrow with those of embryonic tissues, such as the fetal liver and embryonic thymus, to disentangle ILC heterogeneity in light of layered immunity.

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“…Claudin-2 transcriptional regulation analyses showed a significant role of interleukin 22 (IL-22) (10). IL-22 is usually produced at the site of inflammation by Th22, Th17, or innate lymphoid cell type 3 (11)(12)(13)(14)(15). It is a cytokine with double activity: 1) activates the immune system and 2) contributes to the enhanced production of extracellular matrix components.…”

Section: Introductionmentioning

confidence: 99%

IL-22 regulates endometrial regeneration by enhancing tight junctions and orchestrating extracellular matrix

Ganieva

Schneiderman

et al. 2022

Front. Immunol.

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The uterine endometrium uniquely regenerates after menses, postpartum, or after breaks in the uterine layer integrity throughout women’s lives. Direct cell–cell contacts ensured by tight and adherens junctions play an important role in endometrial integrity. Any changes in these junctions can alter the endometrial permeability of the uterus and have an impact on the regeneration of uterine layers. Interleukin 22 (IL-22) is a cytokine that is recognized for its role in epithelial regeneration. Moreover, it is crucial in controlling the inflammatory response in mucosal tissues. Here, we studied the role of IL-22 in endometrial recovery after inflammation-triggered abortion. Fecundity of mice was studied in consecutive matings of the same animals after lipopolysaccharide (LPS) (10 µg per mouse)-triggered abortion. The fecundity rate after the second mating was substantially different between IL-22 knockout (IL-22−/−) (9.1%) and wild-type (WT) (71.4%) mice (p < 0.05), while there was no difference between the groups in the initial mating, suggesting that IL-22 deficiency might be associated with secondary infertility. A considerable difference was observed between IL-22−/− and WT mice in the uterine clearance following LPS-triggered abortion. Gross examination of the uteri of IL-22−/− mice revealed non-viable fetuses retained inside the horns (delayed clearance). In contrast, all WT mice had completed abortion with total clearance after LPS exposure. We also discovered that IL-22 deficiency is associated with a decreased expression of tight junctions (claudin-2 and claudin-10) and cell surface pathogen protectors (mucin-1). Moreover, IL-22 has a role in the remodeling of the uterine tissue in the inflammatory environment by regulating epithelial–mesenchymal transition markers called E- and N-cadherin. Therefore, IL-22 contributes to the proper regeneration of endometrial layers after inflammation-triggered abortion. Thus, it might have a practical significance to be utilized as a treatment option postpartum (enhanced regeneration function) and in secondary infertility caused by inflammation (enhanced barrier/protector function).

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CD45RA ⁺ CD62L ⁻ ILCs in human tissues represent a quiescent local reservoir for the generation of differentiated ILCs

Cited by 19 publications

References 73 publications

Helper-Like Type-1 Innate Lymphoid Cells in Inflammatory Bowel Disease

Helper-Like Type-1 Innate Lymphoid Cells in Inflammatory Bowel Disease

Waves of layered immunity over innate lymphoid cells

IL-22 regulates endometrial regeneration by enhancing tight junctions and orchestrating extracellular matrix

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CD45RA + CD62L − ILCs in human tissues represent a quiescent local reservoir for the generation of differentiated ILCs

Cited by 19 publications

References 73 publications

Helper-Like Type-1 Innate Lymphoid Cells in Inflammatory Bowel Disease

Helper-Like Type-1 Innate Lymphoid Cells in Inflammatory Bowel Disease

Waves of layered immunity over innate lymphoid cells

IL-22 regulates endometrial regeneration by enhancing tight junctions and orchestrating extracellular matrix

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Product

Resources

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CD45RA ⁺ CD62L ⁻ ILCs in human tissues represent a quiescent local reservoir for the generation of differentiated ILCs