Literature DB >> 24523504

Mouse mast cell proteases 4 and 5 mediate epidermal injury through disruption of tight junctions.

Lora G Bankova1, Cecilia Lezcano, Gunnar Pejler, Richard L Stevens, George F Murphy, K Frank Austen, Michael F Gurish.   

Abstract

We previously established a mast cell (MC)-dependent thermal injury model in mice with ulceration and scar formation that depended on nonredundant functions of mouse MC protease (mMCP)4 and mMCP5. We hypothesized that MC activation is an early event and now find by histology that exocytosis of granule contents occurred by 2 min after thermal injury in wild-type (WT) C57BL/6 mice and in the mMCP4- or mMCP5-deficient mice. The degranulation was equivalent for MCs in the dermis and hypodermis of all three strains, but only the WT mice showed an appreciable increase in epidermal thickness. There was no loss of total MCs, partially degranulated plus intact, during the 4 h of observation. By electron microscopy, MCs in all strains showed early zonal degranulation at 30 s with marked progression in magnitude by 120 s and no mitochondrial injury or cellular necrosis. Concomitantly there was an increase in intercellular spaces indicative of tight junction (TJ) disruption in WT mice but not in the mMCP4- or mMCP5-deficient strains. The desmosomes were intact in all strains. Immunodetection of the TJ protein claudin 4 in WT and mMCP5-deficient mice indicated a significant reduction after scald injury whereas mMCP4(-/-) mice showed no significant changes. Taken together, these findings reveal that a second-degree burn injury can initiate an immediate novel zonal degranulation of MCs throughout all skin layers and a disruption of the epidermal TJs dependent on the nonredundant presence of mMCP4 and mMCP5.

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Year:  2014        PMID: 24523504      PMCID: PMC3970423          DOI: 10.4049/jimmunol.1301794

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  28 in total

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4.  Rat mast cell protease 4 is a beta-chymase with unusually stringent substrate recognition profile.

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Authors:  N Arizono; S Matsuda; T Hattori; Y Kojima; T Maeda; S J Galli
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10.  Reperfusion injury of ischemic skeletal muscle is mediated by natural antibody and complement.

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Review 1.  Approaches for analyzing the roles of mast cells and their proteases in vivo.

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Review 4.  Novel Insight into the in vivo Function of Mast Cell Chymase: Lessons from Knockouts and Inhibitors.

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5.  Dysregulation of intestinal epithelial CFTR-dependent Cl- ion transport and paracellular barrier function drives gastrointestinal symptoms of food-induced anaphylaxis in mice.

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10.  Mouse mast cells and mast cell proteases do not play a significant role in acute tissue injury pain induced by formalin.

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