mTOR intersects antibody-inducing signals from TACI in marginal zone B cells

Sintes, Jordi; Gentile, Maurizio; Zhang, Shuling; García-Carmona, Yolanda; Magri, Giuliana; Cassis, Linda; Segura-Garzón, Daniel; Ciociola, Alessandra; Grasset, E.; Bascones, Sabrina; Comerma, Laura; Pybus, Marc; Lligé, David; Puga, Irene; Gutzeit, Cindy; He, Bing; Dubois, Wendy; Crespo, Marta; Pascual, Julio; Mensa, Anna; Aróstegui, Juan I.; Juan, Manel; Yagüe, Jordi; Serrano, Sergi; Lloreta, Josep; Meffre, Eric; Hahne, Michael; Cunningham‐Rundles, Charlotte; Mock, Beverly A.; Cerutti, Andrea

doi:10.1038/s41467-017-01602-4

Cited by 56 publications

(59 citation statements)

References 61 publications

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“…Functionally, BAFF upregulates Toll-like receptor (TLR) expression in B cells, and cooperates with dual BCR/TLR signals to drive T-independent B cell differentiation. [51][52][53][54] In addition, whereas combined BCR/TLR9 signaling induces B cell proliferation followed by apoptotic cell death, the provision of excess BAFF allows these cells to differentiate into short-lived plasma cells with pathogenic potential. 49,50 As described below, humoral autoimmunity in BAFF transgenic (BAFF-Tg) mice is T cell independent but requires signals through the TLR adapter molecule MyD88 and TACI, confirming the relevance of this crosstalk in driving breaks in B cell tolerance.…”

Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

“…[51][52][53][54] In addition, whereas combined BCR/TLR9 signaling induces B cell proliferation followed by apoptotic cell death, the provision of excess BAFF allows these cells to differentiate into short-lived plasma cells with pathogenic potential. 52 These interactions have important implications for autoimmunity because cross talk between type 1 IFN, TLR, BCR, and BAFF signaling preferentially supports the survival, class-switch recombination, and plasma cell 57 An additional function of BAFF may be to preferentially enhance the generation of IL10-producing regulatory cells, [58][59][60] however this effect appears to be lost in the setting of inflammation ( Figure 3). By enhancing the production of the short TACI isoform, TLR9 signals amplify this response.…”

Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

“…54 Importantly, whereas TACI expression is critical for BAFF-driven autoimmunity, BAFF-R signals exerted complementary roles in facilitating breaks in B cells tolerance. Alternatively, BAFF-R and TACI ligation could enhance B cell TLR mediated signals 52 and thereby facilitate class-switched autoantibody production. 75 Although the mechanisms whereby BAFF-R and TACI signals integrate to break B cell tolerance have not been completely defined, we hypothesize that BAFF-R signals both facilitate the survival of low-affinity autoreactive transitional B cells and promote the expansion of autoreactive clones that have engaged self-antigen.…”

Section: Baff-r and Taci Signals Integrate To Promote Autoimmunity mentioning

confidence: 99%

“…49,50 As described below, humoral autoimmunity in BAFF transgenic (BAFF-Tg) mice is T cell independent but requires signals through the TLR adapter molecule MyD88 and TACI, confirming the relevance of this crosstalk in driving breaks in B cell tolerance. [51][52][53][54] In addition, whereas combined BCR/TLR9 signaling induces B cell proliferation followed by apoptotic cell death, the provision of excess BAFF allows these cells to differentiate into short-lived plasma cells with pathogenic potential. 55 Finally, TACI, in particular the short human isoform, can enter endosomal compartments where it associates with the TLR adapter molecule MyD88 through a domain separate from the TLR TIR domain to mediate enhanced NFκB signals that drive plasma cell differentiation.…”

Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

“…46 Marginal zone B cells express high levels of TACI and in these cells TLR9 and TACI recruit both MyD88 and mTOR to facilitate T-independent class switching and plasma cell differentiation. 52 These interactions have important implications for autoimmunity because cross talk between type 1 IFN, TLR, BCR, and BAFF signaling preferentially supports the survival, class- 57 An additional function of BAFF may be to preferentially enhance the generation of IL10-producing regulatory cells, [58][59][60] however this effect appears to be lost in the setting of inflammation ( Figure 3). 61 In addition to regulating B cell survival, serum BAFF levels modulate the relative autoreactivity of the naive B cell repertoire.…”

Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

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BAFF inhibition in SLE—Is tolerance restored?

Jackson

Davidson

2019

Immunological Reviews

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The B cell activating factor (BAFF) inhibitor, belimumab, is the first biologic drug approved for the treatment of SLE, and exhibits modest, but durable, efficacy in decreasing disease flares and organ damage. BAFF and its homolog APRIL are TNF‐like cytokines that support the survival and differentiation of B cells at distinct developmental stages. BAFF is a crucial survival factor for transitional and mature B cells that acts as rheostat for the maturation of low‐affinity autoreactive cells. In addition, BAFF augments innate B cell responses via complex interactions with the B cell receptor (BCR) and Toll like receptor (TLR) pathways. In this manner, BAFF impacts autoreactive B cell activation via extrafollicular pathways and fine tunes affinity selection within germinal centers (GC). Finally, BAFF and APRIL support plasma cell survival, with differential impacts on IgM‐ and IgG‐producing populations. Therapeutically, BAFF and combined BAFF/APRIL inhibition delays disease onset in diverse murine lupus strains, although responsiveness to BAFF inhibition is model dependent, in keeping with heterogeneity in clinical responses to belimumab treatment in humans. In this review, we discuss the mechanisms whereby BAFF/APRIL signals promote autoreactive B cell activation, discuss whether altered selection accounts for therapeutic benefits of BAFF inhibition, and address whether new insights into BAFF/APRIL family complexity can be exploited to improve human lupus treatments.

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Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

Section: Baff-r and Taci Signals Integrate To Promote Autoimmunity mentioning

confidence: 99%

Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

Section: Interactions Between Baff/april and Tlr Signaling Pathwaysmentioning

confidence: 99%

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BAFF inhibition in SLE—Is tolerance restored?

Jackson

Davidson

2019

Immunological Reviews

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Dexamethasone improves thymoma-associated myasthenia gravis via the AKT-mTOR pathway

Liu¹,

Chen²,

Wang³

et al. 2023

Naunyn-Schmiedeberg's Arch Pharmacol

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Clinically, thymoma patients are often complicated with myasthenia gravis (MG). Dexamethasone, a glucocorticoid with anti-inflammatory effects, could be used as an immunosuppressant for thymoma-associated MG, but the mechanism of action remains to be explored. In this study, Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis, weighted gene co-expression network analysis (WGCNA) of potential targets was performed by screening the intersection targets of dexamethasone and thymoma-associated MG from the database. Furthermore, the key targets and core active components were identified by topological analysis of the protein–protein interaction (PPI) network. Molecular docking technology was applied to screen the complexes with stable binding of dexamethasone and core targets. Patients with thymoma were divided into two groups according to whether they received dexamethasone before operation, and immunohistochemistry and western blot were used to verify the selected target of dexamethasone in treating thymoma-associated MG. The results showed that the action pathway of dexamethasone on the disease was closely enriched to phosphatidylinositol 3-kinase (PI3K)-protein kinase B (PKB/AKT), mammalian target of rapamycin (mTOR) signaling pathways. The expressions of AKT1 and its downstream molecule mTOR in the thymoma microenvironment of thymoma-associated MG patients who did not receive dexamethasone before operation were higher than those in the group receiving dexamethasone before operation. This study demonstrates that dexamethasone can promote apoptosis through the AKT-mTOR pathway for the treatment of thymoma-associated MG, as validated by network pharmacology predictions and clinical specimen experiments, and can be verified by large-scale clinical trials in the future. This study also provides theoretical support and new research perspectives for this disease.

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Silencing TLR4/MyD88/NF-κB Signaling Pathway Alleviated Inflammation of Corneal Epithelial Cells Infected by ISE

et al. 2020

Inflammation

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mTOR intersects antibody-inducing signals from TACI in marginal zone B cells

Cited by 56 publications

References 61 publications

BAFF inhibition in SLE—Is tolerance restored?

BAFF inhibition in SLE—Is tolerance restored?

Dexamethasone improves thymoma-associated myasthenia gravis via the AKT-mTOR pathway

Silencing TLR4/MyD88/NF-κB Signaling Pathway Alleviated Inflammation of Corneal Epithelial Cells Infected by ISE

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