Analyzing the Functions of Mast Cells &lt;em&gt;In Vivo&lt;/em&gt; Using '&lt;em&gt;Mast Cell Knock-in&lt;/em&gt;' Mice

Gaudenzio, Nicolas; Sibilano, Riccardo; Starkl, Philipp; Tsai, Mindy; Galli, Stephen J.; Reber, Laurent L.

doi:10.3791/52753

Cited by 18 publications

(17 citation statements)

References 67 publications

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“…Other reasons for the more modest phenotype in the Tph1 MCKO mice is the time of testing which was after 8 weeks of high-fat diet compared to the 12 weeks for the Kit Tph1−/− mice. The longer duration of high-fat diet feeding in the Kit Tph1−/− mice was utilized to maximize mast cell engraftment as previously suggested 47 . Therefore, sex and duration of the high-fat diet before testing may explain the differences between models.…”

Section: Discussionmentioning

confidence: 99%

Genetic deletion of mast cell serotonin synthesis prevents the development of obesity and insulin resistance

et al. 2020

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Obesity is linked with insulin resistance and is characterized by excessive accumulation of adipose tissue due to chronic energy imbalance. Increasing thermogenic brown and beige adipose tissue futile cycling may be an important strategy to increase energy expenditure in obesity, however, brown adipose tissue metabolic activity is lower with obesity. Herein, we report that the exposure of mice to thermoneutrality promotes the infiltration of white adipose tissue with mast cells that are highly enriched with tryptophan hydroxylase 1 (Tph1), the rate limiting enzyme regulating peripheral serotonin synthesis. Engraftment of mast celldeficient mice with Tph1 −/− mast cells or selective mast cell deletion of Tph1 enhances uncoupling protein 1 (Ucp1) expression in white adipose tissue and protects mice from developing obesity and insulin resistance. These data suggest that therapies aimed at inhibiting mast cell Tph1 may represent a therapeutic approach for the treatment of obesity and type 2 diabetes.

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Section: Discussionmentioning

confidence: 99%

Genetic deletion of mast cell serotonin synthesis prevents the development of obesity and insulin resistance

et al. 2020

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“…To track mouse movement and determine displacement, the videos were converted into a sequence of still images using MPEG Streamclip (downloaded from http://www.squared5.com) at 8 frames/s and analyzed using the TrackMate plugin for ImageJ. For analysis of c-Kit expression levels on peritoneal mast cells of C57BL/6J mice, the animals were sacrificed 1 h after injections and a peritoneal lavage with 5 ml of ice-cold PBS was performed to harvest the peritoneal cells as previously described (Gaudenzio et al, 2015). The peritoneal cell suspension was centrifuged, resuspended in 1 ml PBS 1% BSA and 200 μl were subsequently stained with 1:200 anti-c-Kit and anti-FcεRIα antibodies on ice for 15 min, analyzed by flow cytometry on an Accuri C6 flow cytometer (BD Biosciences).…”

Section: Star Methods Textmentioning

confidence: 99%

“…Histological analysis of peritoneal mast cells was performed based on a published protocol (Gaudenzio et al, 2015). Briefly, 1 ml of peritoneal cell suspension was centrifuged and the pellet resuspended in 100 μl PBS 1% BSA and spun onto microscopy slides using a Cytospin system (Shandon).…”

Section: Star Methods Textmentioning

confidence: 99%

Decoupling the Functional Pleiotropy of Stem Cell Factor by Tuning c-Kit Signaling

Chhabra

Starkl

et al. 2017

Cell

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SUMMARY Most secreted growth factors and cytokines are functionally pleiotropic because their receptors are expressed on diverse cell types. While important for normal mammalian physiology, pleiotropy limits the efficacy of cytokines and growth factors as therapeutics. Stem cell factor (SCF) is a growth factor that acts through the c-Kit receptor tyrosine kinase to elicit hematopoietic progenitor expansion, but can be toxic when administered in vivo because it concurrently activates mast cells. We engineered a mechanism-based SCF partial agonist that impaired c-Kit dimerization, truncating downstream signaling amplitude. This SCF variant elicited biased activation of hematopoietic progenitors over mast cells in vitro and in vivo. Mouse models of SCF-mediated anaphylaxis, radioprotection, and hematopoietic expansion revealed that this SCF partial agonist retained therapeutic efficacy while exhibiting virtually no anaphylactic off-target effects. The approach of biasing cell activation by tuning signaling thresholds and outputs has applications to many dimeric receptor-ligand systems.

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“…BMCMCs were obtained through in vitro differentiation of bone marrow precursors in WEHI-3-conditioned DMEM, for at least 5 weeks55. Bone marrow cells derived from 4-week-old Tnfrsf14 −/− , Tnfrsf14 +/+ or Mcpt5-eYFP mice were cultured in WEHI-3-conditioned DMEM (DMEM containing 20% supernatant of WEHI-3 cells, 10% FBS, 50 μM β-mercaptoethanol, 2 mM L -glutamine and 1% antibiotic-antimycotic solution), as a source of IL-3, for 4–5 weeks to generate cell populations that contained >99% bone-marrow-derived cultured MCs (BMCMCs).…”

Section: Methodsmentioning

confidence: 99%

A TNFRSF14-FcɛRI-mast cell pathway contributes to development of multiple features of asthma pathology in mice

et al. 2016

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Asthma has multiple features, including airway hyperreactivity, inflammation and remodelling. The TNF superfamily member TNFSF14 (LIGHT), via interactions with the receptor TNFRSF14 (HVEM), can support TH2 cell generation and longevity and promote airway remodelling in mouse models of asthma, but the mechanisms by which TNFSF14 functions in this setting are incompletely understood. Here we find that mouse and human mast cells (MCs) express TNFRSF14 and that TNFSF14:TNFRSF14 interactions can enhance IgE-mediated MC signalling and mediator production. In mouse models of asthma, TNFRSF14 blockade with a neutralizing antibody administered after antigen sensitization, or genetic deletion of Tnfrsf14, diminishes plasma levels of antigen-specific IgG1 and IgE antibodies, airway hyperreactivity, airway inflammation and airway remodelling. Finally, by analysing two types of genetically MC-deficient mice after engrafting MCs that either do or do not express TNFRSF14, we show that TNFRSF14 expression on MCs significantly contributes to the development of multiple features of asthma pathology.

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Analyzing the Functions of Mast Cells <em>In Vivo</em> Using '<em>Mast Cell Knock-in</em>' Mice

Cited by 18 publications

References 67 publications

Genetic deletion of mast cell serotonin synthesis prevents the development of obesity and insulin resistance

Genetic deletion of mast cell serotonin synthesis prevents the development of obesity and insulin resistance

Decoupling the Functional Pleiotropy of Stem Cell Factor by Tuning c-Kit Signaling

A TNFRSF14-FcɛRI-mast cell pathway contributes to development of multiple features of asthma pathology in mice

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