The chemotactic receptor EBI2 regulates the homeostasis, localization and immunological function of splenic dendritic cells

Gatto, Dominique; Wood, Katherine C.; Caminschi, Irina; Murphy-Durland, Danielle; Schofield, Peter R.; Christ, Daniel; Karupiah, Gunasegaran; Brink, Robert

doi:10.1038/ni.2555

Cited by 165 publications

(206 citation statements)

References 47 publications

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“…þ DCs in the bridging channels of the spleen and the subsequent immune response to particulate antigens (Gatto et al 2013). Finally, although sphingosine-1-phosphate receptor 1 (S1PR1) blockade has no effect on DC localization in the LN, it does lead to the redistribution of immature CD4…”

Section: The Chemokine System In Innate Immunitymentioning

confidence: 99%

The Chemokine System in Innate Immunity

Sokol

Luster

2015

Cold Spring Harb Perspect Biol

615

468

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Section: The Chemokine System In Innate Immunitymentioning

confidence: 99%

The Chemokine System in Innate Immunity

Sokol

Luster

2015

Cold Spring Harb Perspect Biol

615

468

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“…A second possibility is that the location of the targeted DC may be critical. CD4 + CD11b + DCs targeted by DCIR-2 predominantly localize in marginal zone (MZ) bridging channels, allowing efficient capture of particulate Ag (31,52). It has been shown that CD4 + CD11b + DCs that capture "SRBCs," a classical type of particulate Ag, move from the MZ bridging channels to the T/B border (52), where responses eventually lead to GC formation.…”

Section: Cd8mentioning

confidence: 99%

“…It has been shown that CD4 + CD11b + DCs that capture "SRBCs," a classical type of particulate Ag, move from the MZ bridging channels to the T/B border (52), where responses eventually lead to GC formation. Because targeting Ag via DCIR-2 did not induce such movement of DCs, but left them within the MZ bridging channels (30,31), their capacity to induce GC formation may have been compromised. Interestingly, location within the bridging channels is where CD11c low blood "DCs" were reported to support T cell-independent B cell responses by providing survival signals such as BAFF and APRIL (53).…”

Section: Cd8mentioning

confidence: 99%

Targeting Antigen to Clec9A Primes Follicular Th Cell Memory Responses Capable of Robust Recall

Kato

Zaid

Davey

et al. 2015

The Journal of Immunology

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Targeting Ags to dendritic cell (DC) surface receptors can induce a variety of responses depending on the DC type targeted, the receptor targeted, and the adjuvant used. Clec9A (DNGR-1), which is expressed by CD8+ DCs, has been shown to bind F-actin exposed on damaged cells. Targeting Ag to this receptor in mice and nonhuman primates induces strong humoral immunity even in the absence of adjuvant, a process seen for a few select DC receptors. In contrast with other receptors, however, targeting Clec9A induces long-lived, affinity-matured Ab responses that are associated with efficient CD4+ T cell responses shown to possess properties of follicular Th cells (TFH). In this article, we provide definitive evidence that Clec9A targeting promotes the development of TFH by showing that responding CD4 T cells express CXCR5, PD1, the TFH transcription factor Bcl6, and the cytokine IL-21, and that these cells localize to germinal centers. Furthermore, we extend studies from the model Ag OVA to the viral Ag glycoprotein D of HSV-1 and examine the capacity of primed TFH to form functional memory. We show that targeting glycoprotein D to Clec9A even in the absence of adjuvant induced long-lived memory CXCR5+ PD1hi CD4+ T cells that proliferated extensively upon secondary challenge and rapidly developed into effector TFH. This was associated with enhanced germinal center B cell responses and accelerated Ab production. Our study indicates that targeting Ags to Clec9A in the absence of adjuvant routinely generates TFH responses that form long-lived memory capable of robust secondary TFH responses.

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“…EBI2 is a chemoattractant receptor of the GPCR family with no known roles other than controlling cell migration and/or positioning. Specifically, EBI2 promotes the positioning of dendritic cells and activated B lymphocytes to specialized outer and interfollicular niches in secondary lymphoid organs and plays important roles in primary antibody responses (Gatto et al, 2009(Gatto et al, , 2013Pereira et al, 2009bPereira et al, , 2010aYi et al, 2012;Yi and Cyster, 2013). Thus, the phenotypic similarity between EBI2-and CH25H-deficient mice favor a model in which oxysterols sensed by EBI2 expressed in OCPs regulate bone mass homeostasis predominantly by promoting OCP cell movement and positioning, which facilitates cell fusion and enhances the development of large OCs.…”

Section: Ebi2 Signaling Controls Ocp-directed Migration Toward Bone Smentioning

confidence: 99%

“…However, systemic RANKL administration has been shown to increase OCP homing back to BM and to promote local OC differentiation (Kotani et al, 2013). These studies suggest that OCP movement in and out of BM tissue is highly regulated and that balanced responsiveness to B lymphocyte migration in secondary lymphoid organs (Gatto et al, 2009(Gatto et al, , 2013Pereira et al, 2009b;Hannedouche et al, 2011;Kelly et al, 2011;Liu et al, 2011;Yi and Cyster, 2013), in controlling monocyte and OCP movement and positioning within BM. We show that EBI2 is highly expressed in OCPs and mature OCs and promotes OCP motility in vitro and in various chemoattractants regulates OCP movement and differentiation.…”

mentioning

confidence: 99%

Oxysterols and EBI2 promote osteoclast precursor migration to bone surfaces and regulate bone mass homeostasis

Nevius¹,

Pinho²,

Dhodapkar³

et al. 2015

J Cell Biol

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Bone surfaces attract hematopoietic and nonhematopoietic cells, such as osteoclasts (OCs) and osteoblasts (OBs), and are targeted by bone metastatic cancers. However, the mechanisms guiding cells toward bone surfaces are essentially unknown. Here, we show that the Gi protein-coupled receptor (GPCR) EBI2 is expressed in mouse monocyte/OC precursors (OCPs) and its oxysterol ligand 7,25-dihydroxycholesterol (7,25-OHC) is secreted abundantly by OBs. Using in vitro time-lapse microscopy and intravital two-photon microscopy, we show that EBI2 enhances the development of large OCs by promoting OCP motility, thus facilitating cell-cell interactions and fusion in vitro and in vivo. EBI2 is also necessary and sufficient for guiding OCPs toward bone surfaces. Interestingly, OCPs also secrete 7,25-OHC, which promotes autocrine EBI2 signaling and reduces OCP migration toward bone surfaces in vivo. Defective EBI2 signaling led to increased bone mass in male mice and protected female mice from age-and estrogen deficiency-induced osteoporosis. This study identifies a novel pathway involved in OCP homing to the bone surface that may have significant therapeutic potential.

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The chemotactic receptor EBI2 regulates the homeostasis, localization and immunological function of splenic dendritic cells

Cited by 165 publications

References 47 publications

The Chemokine System in Innate Immunity

The Chemokine System in Innate Immunity

Targeting Antigen to Clec9A Primes Follicular Th Cell Memory Responses Capable of Robust Recall

Oxysterols and EBI2 promote osteoclast precursor migration to bone surfaces and regulate bone mass homeostasis

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