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Monitoring of inflammation using novel biosensor mouse model reveals tissue- and sex-specific responses to Western diet
Author(s) -
Sarah Talley,
Raiza Bonomo,
Chaitanya K. Gavini,
Jomana Hatahet,
Emily Gornick,
Tyler Cook,
Ben Chun,
Pete Kekenes-Huskey,
Grégory Aubert,
E. M. Campbell,
Virginie MansuyAubert
Publication year - 2022
Publication title -
disease models and mechanisms
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.327
H-Index - 83
eISSN - 1754-8411
pISSN - 1754-8403
DOI - 10.1242/dmm.049313
Subject(s) - inflammation , adipose tissue , butyrate , in vivo , biology , white adipose tissue , immunology , microbiology and biotechnology , endocrinology , biochemistry , genetics , fermentation
Obesity is an epidemic, and it is characterized by a state of low-grade systemic inflammation A key component of inflammation is the activation of inflammasomes, multiprotein complexes that form in response to danger signals and that lead to activation of caspase-1. Previous studies have found that a Westernized diet induces activation of inflammasomes and production of inflammatory cytokines. Gut microbiota metabolites, including the short-chain fatty acid butyrate, have received increased attention as underlying some obesogenic features, but the mechanisms of action by which butyrate influences inflammation in obesity remain unclear. We engineered a caspase-1 reporter mouse model to measure spatiotemporal dynamics of inflammation in obese mice. Concurrent with increased capsase-1 activation in vivo, we detected stronger biosensor signal in white adipose and heart tissues of obese mice ex vivo and observed that a short-term butyrate treatment affected some but not all the inflammatory responses induced by Western diet. Through characterization of inflammatory responses and computational analyses, we identified tissue- and sex-specific caspase-1 activation patterns and inflammatory phenotypes in obese mice, offering new mechanistic insights underlying the dynamics of inflammation.

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