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  5. Caspase-4: A Therapeutic Target for Peptic Ulcer Disease

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Article
English
2020

Caspase-4: A Therapeutic Target for Peptic Ulcer Disease

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0 Files

English
2020
ImmunoHorizons
Vol 4 (10)
DOI: 10.4049/immunohorizons.2000080

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Luke O'neill
Luke O'neill

Trinity College Dublin

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Zbigniew Zasłona
Ewelina Flis
Ciara Nulty
+7 more

Abstract

Peptic ulcers are caused by the interaction between bacterial and host factors. This study demonstrates enhanced expression of caspase-4 in peptic ulcer patient biopsies, indicating that pyroptosis and noncanonical inflammasome activity may be processes involved in peptic ulcer disease. We show that primary murine macrophages infected with Helicobacter pylori upregulate caspase-11 (the ortholog of human caspase-4), activate caspase-1, and secrete IL-1β. We demonstrate that misoprostol (a stable PGE1 analogue) decreased IL-1β secretion and delayed lethality in vivo in a murine peritonitis model. PGE2 was shown to inhibit caspase-11–driven pyroptosis and IL-1β secretion in macrophages. Overall, we provide evidence for a pathological role of caspase-4/11 in peptic ulcer disease and propose that targeting caspase-4 or inhibiting pyroptosis may have therapeutic potential in the management of peptic ulcers.

How to cite this publication

Zbigniew Zasłona, Ewelina Flis, Ciara Nulty, Jay Kearney, Rebecca Fitzgerald, Atiyekeogbebe Rita Douglas, Deirdre McNamara, Sinead Smith, Luke O'neill, Emma M. Creagh (2020). Caspase-4: A Therapeutic Target for Peptic Ulcer Disease. ImmunoHorizons, 4(10), pp. 627-633, DOI: 10.4049/immunohorizons.2000080.

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Publication Details

Type

Article

Year

2020

Authors

10

Datasets

0

Total Files

0

Language

English

Journal

ImmunoHorizons

DOI

10.4049/immunohorizons.2000080

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