Differential Lyn-dependence of the SHIP1-deficient mast cell phenotype

Miranda, Susana M. Nunes de; Wilhelm, Thomas; Huber, Michael; Zorn, Carolin N.

doi:10.1186/s12964-016-0135-0

Cited by 13 publications

(30 citation statements)

References 48 publications

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“…This indicated that effects on degranulation and Ca 2+ mobilisation were quantitatively uncoupled in DKO BMMCs. Such uncoupling has also been reported, amongst others, in Lyn -deficient as well as in Ship1/Lyn double-deficient BMMCs 27 , 28 . The exact mechanism has not been elucidated yet.…”

Section: Resultssupporting

confidence: 66%

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Stimulus strength determines the BTK-dependence of the SHIP1-deficient phenotype in IgE/antigen-triggered mast cells

Zorn

Simonowski

Huber

2018

Sci Rep

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Antigen (Ag)-mediated crosslinking of IgE-loaded high-affinity receptors for IgE (FcεRI) on mast cells (MCs) triggers activation of proinflammatory effector functions relevant for IgE-associated allergic disorders. The cytosolic tyrosine kinase BTK and the SH2-containing inositol-5′-phosphatase SHIP1 are central positive and negative regulators of Ag-triggered MC activation, respectively, contrarily controlling Ca2+ mobilisation, degranulation, and cytokine production. Using genetic and pharmacological techniques, we examined whether BTK activation in Ship1−/− MCs is mandatory for the manifestation of the well-known hyperactive phenotype of Ship1−/− MCs. We demonstrate the prominence of BTK for the Ship1−/− phenotype in a manner strictly dependent on the strength of the initial Ag stimulus; particular importance for BTK was identified in Ship1−/− bone marrow-derived MCs in response to stimulation with suboptimal Ag concentrations. With respect to MAPK activation, BTK showed particular importance at suboptimal Ag concentrations, allowing for an analogous-to-digital switch resulting in full activation of ERK1/2 already at low Ag concentrations. Our data allow for a more precise definition of the role of BTK in FcεRI-mediated signal transduction and effector function in MCs. Moreover, they suggest that reduced activation or curtate expression of SHIP1 can be compensated by pharmacological inhibition of BTK and vice versa.

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Section: Resultssupporting

confidence: 66%

“…1b , Y-P of PLCγ1 and PLCγ2 was reduced in Btk −/− BMMCs compared to WT cells; moreover, Y-P of PLCγ1 and PLCγ2 in Ship1 −/− BMMCs was drastically augmented (Fig. 2e ) 28 . This enhancement was reduced in DKO BMMCs to Y-P levels found in WT cells (Fig.…”

Section: Resultsmentioning

confidence: 86%

Stimulus strength determines the BTK-dependence of the SHIP1-deficient phenotype in IgE/antigen-triggered mast cells

Zorn

Simonowski

Huber

2018

Sci Rep

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“…The cytosolic phosphatase SHIP-1, SH2-containing inositol-5′-phosphatase, has critical roles in microphages, including generation of alternatively activated macrophages, 39 regulation of LPS-induced macrophage inflammatory responses 40 and modulation of myeloproliferation. 11 Diverse cellular functions have been previously investigated in association of Lyn and SHIP-1, 41 , 42 but whether Lyn is involved in SHIP-1 expression or membrane translation 43 remains unclear. To investigate it, we measured SHIP-1 expression in Lyn-silenced and control MH-S cells at 0, 30 and 60 min post infection of PAO1.…”

Section: Resultsmentioning

confidence: 99%

“…Diverse cellular functions have been previously investigated in association with both Lyn and SHIP-1. 41 , 42 SHIP-1 and Lyn are involved in regulation of integrin alpha IIb-β3 signaling in platelets, 41 and in respect to Ag-triggered degranulation in mast cells. 42 In macrophages, Lyn and SHIP-1 negatively regulate macrophage colony-stimulating factor-induced Akt activity.…”

Section: Discussionmentioning

confidence: 99%

“… 41 , 42 SHIP-1 and Lyn are involved in regulation of integrin alpha IIb-β3 signaling in platelets, 41 and in respect to Ag-triggered degranulation in mast cells. 42 In macrophages, Lyn and SHIP-1 negatively regulate macrophage colony-stimulating factor-induced Akt activity. 24 A previous study demonstrated that activation of macrophages by the stimulation of LPS is negatively regulated by a Lyn/PI3K axis and promoted by SHIP-1.…”

Section: Discussionmentioning

confidence: 99%

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Lyn prevents aberrant inflammatory responses to Pseudomonas infection in mammalian systems by repressing a SHIP-1-associated signaling cluster

Fang

et al. 2016

Sig Transduct Target Ther

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The pleiotropic Src kinase Lyn has critical roles in host defense in alveolar macrophages against bacterial infection, but the underlying mechanism for Lyn-mediated inflammatory response remains largely elusive. Using mouse Pseudomonas aeruginosa infection models, we observed that Lyn−/− mice manifest severe lung injury and enhanced inflammatory responses, compared with wild-type littermates. We demonstrate that Lyn exerts this immune function through interaction with IL-6 receptor and cytoskeletal protein Ezrin via its SH2 and SH3 domains. Depletion of Lyn results in excessive STAT3 activation, and enhanced the Src homology 2-containing inositol-5-phopsphatase 1 (SHIP-1) expression. Deletion of SHIP-1 in Lyn−/− mice (double knockout) promotes mouse survival and reduces inflammatory responses during P. aeruginosa infection, revealing the rescue of the deadly infectious phenotype in Lyn deficiency. Mechanistically, loss of SHIP-1 reduces NF-κB-dependent cytokine production and dampens MAP kinase activation through a TLR4-independent PI3K/Akt pathway. These findings reveal Lyn as a regulator for host immune response against P. aeruginosa infection through SHIP-1 and IL-6/STAT3 signaling pathway in alveolar macrophages.

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Src Family Protein Kinase Controls the Fate of B Cells in Autoimmune Diseases

et al. 2020

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There are more than 80 kinds of autoimmune diseases known at present, including rheumatoid arthritis (RA), systemic lupus erythematosus (SLE), systemic sclerosis (SSc), inflammatory bowel disease (IBD), as well as other disorders. Autoimmune diseases have a characteristic of immune responses directly attacking own tissues, leading to systematic inflammation and subsequent tissue damage. B cells play a vital role in the development of autoimmune diseases and differentiate into plasma cells or memory B cells to secrete highaffinity antibody or provide long-lasting function. Drugs targeting B cells show good therapeutic effects for the treatment of autoimmune diseases, such as rituximab (anti-CD20 antibody). Src family protein kinases (SFKs) are believed to play important roles in a variety of cellular functions such as growth, proliferation, and differentiation of B cell via B cell antigen receptor (BCR). Lck/Yes-related novel protein tyrosine kinase (LYN), BLK (B lymphocyte kinase), and Fyn are three different kinds of SFKs mainly expressed in B cells. LYN has a dual role in the BCR signal. On the one hand, positive signals are beneficial to the development and maturation of B cells. On the other hand, LYN can also inhibit excessively activated B cells. BLK is involved in the proliferation, differentiation, and immune tolerance of B lymphocytes, and further affects the function of B cells, which may lead to autoreactive or regulatory cellular responses, increasing the risk of autoimmune diseases. Fyn may affect the development of autoimmune disorders via the differentiation of B cells in the early stage of B cell development. This article reviews the recent advances of SFKs in B lymphocytes in autoimmune diseases.

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Differential Lyn-dependence of the SHIP1-deficient mast cell phenotype

Cited by 13 publications

References 48 publications

Stimulus strength determines the BTK-dependence of the SHIP1-deficient phenotype in IgE/antigen-triggered mast cells

Stimulus strength determines the BTK-dependence of the SHIP1-deficient phenotype in IgE/antigen-triggered mast cells

Lyn prevents aberrant inflammatory responses to Pseudomonas infection in mammalian systems by repressing a SHIP-1-associated signaling cluster

Src Family Protein Kinase Controls the Fate of B Cells in Autoimmune Diseases

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