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Open AccessJournal ArticleDOI

Eosinophil peroxidase-induced mast cell secretion.

TLDR
The stimulation of mast cell mediator release by the EPO-H2O2-halide system and the formation of MCG/EPO complexes with augmented cytotoxic activity may influence the adjacent inflammatory response.
Abstract
Eosinophil peroxidase (EPO) at relatively low levels (4-30 mU), when supplemented with H2O2 and a halide, induced mast cell degranulation. Histamine release occurred without concomitant release of the cytoplasmic marker lactic dehydrogenase (LDH), and this, together with ultrastructural studies, indicated a noncytotoxic effect comparable with that induced by other mast cell secretagogues. At pH 7.4, iodide was effective at concentrations down to 10(-5) M, and although chloride alone was ineffective at 0.1 M, a combination of 0.1 M chloride and 10(-6) iodide could meet the halide requirement. Chloride alone was effective at pH 6.5 and 6.0. EPO could be replaced by myeloperoxidase. When the EPO level was increased to 100 mU, combination with H2O2- and iodide-induced cytotoxic histamine release as indicated by concomitant LDH release and ultrastructural evidence of cell disruption. This cytotoxic response reverted to a secretory one on the addition of albumin. Peroxidase was detected on the surface of extruded granules by diaminobenzidine cytochemistry. The mast cell granule (MCG)/EPO complex when supplemented with H2O2 and iodide was more effective than free EPO in the stimulation of mast cell secretion. The stimulation of mast cell mediator release by the EPO-H2O2-halide system and the formation of MCG/EPO complexes with augmented cytotoxic activity may influence the adjacent inflammatory response.

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Citations
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Journal ArticleDOI

Myeloperoxidase: friend and foe

TL;DR: It is concluded that the MPO system plays an important role in the microbicidal activity of phagocytes and the role of theMPO system in tissue injury.
Book ChapterDOI

The Eosinophilic Leukocyte: Structure and Function

TL;DR: The evidence reviewed here indicates that the eosinophil has the ability to kill many species of helminths and likely does so during worm infection and also participate in inflammation in human disease especially asthma, skin diseases, and heart disease.
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The eosinophil and bronchial asthma: Current understanding

TL;DR: Des proteines majeures basiques (MBP) dont la concentration est elevee dans les lavages bronchoalveolaires des patients, ont ete etudiees en effets physiologiques and pathologiques des eosinophiles dans the asthmes bronchiques.
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The eosinophil and the pathophysiology of asthma

TL;DR: These and other findings suggest the hypothesis that the eosinophil mediates damage to the respiratory epithelium and is the prime effector cell in the pathophysiology of asthma.
Journal ArticleDOI

The immunobiology of eosinophils.

TL;DR: Tinctorial properties remain the routine basis for identifying and enumerating these leukocytes in blood and tissues, and eosinophilia, characterized by both heightened production of eosInophils in bone marrow and the accumulation of eOSinophils, is characterized.
References
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Book ChapterDOI

The assay of catalases and peroxidases.

TL;DR: Two methods are described for the catalase assay by disappearance of peroxide are: ultraviolet spectrophotometry and permanganate titration and indirect measurements of the decrease of light absorption caused by the decomposition of hydrogen peroxide byCatalase.
Journal ArticleDOI

Calcium Ionophores and Movement of Calcium Ions following the Physiological Stimulus to a Secretory Process

TL;DR: The fact that labelled calcium can be seen to enter sensitized cells during histamine secretion in the presence of antigen suggests that the entry of calcium into the mast cell may be the trigger for the release of histamine.
Journal Article

Release of histamine from rat mast cells by the complement peptides C3a and C5a.

TL;DR: In this paper, the histamine-releasing actions of anaphylatoxins C3A and C5a were studied in rat mast cells and the peptides, derived from human or porcine complement proteins C3 and C 5, were less potent than 48/80 but more potent than bradykinin.
Journal ArticleDOI

Electron microscope studies on the degranulation of rabbit peritoneal leukocytes during phagocytosis.

TL;DR: It has been proposed that the release of material to the outside of the cell or the discharge of material into intracellular vacuoles, events involving membrane fusion, be termed "exoplasmosis."
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