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Circadian Genes as Exploratory Biomarkers in DMD : Results From Both the mdx Mouse Model and Patients

Authors :
Rossi, Rachele
Falzarano, Maria Sofia
Osman, Hana
Armaroli, Annarita
Scotton, Chiara
Mantuano, Paola
Boccanegra, Brigida
Cappellari, Ornella
Schwartz, Elena
Yuryev, Anton
Mercuri, Eugenio
Bertini, Enrico
D'Amico, Adele
Mora, Marina
Johansson, Camilla
Al-Khalili Szigyarto, Cristina
De Luca, Annamaria
Ferlini, Alessandra
Rossi, Rachele
Falzarano, Maria Sofia
Osman, Hana
Armaroli, Annarita
Scotton, Chiara
Mantuano, Paola
Boccanegra, Brigida
Cappellari, Ornella
Schwartz, Elena
Yuryev, Anton
Mercuri, Eugenio
Bertini, Enrico
D'Amico, Adele
Mora, Marina
Johansson, Camilla
Al-Khalili Szigyarto, Cristina
De Luca, Annamaria
Ferlini, Alessandra
Publication Year :
2021

Abstract

Duchenne muscular dystrophy (DMD) is a rare genetic disease due to dystrophin gene mutations which cause progressive weakness and muscle wasting. Circadian rhythm coordinates biological processes with the 24-h cycle and it plays a key role in maintaining muscle functions, both in animal models and in humans. We explored expression profiles of circadian circuit master genes both in Duchenne muscular dystrophy skeletal muscle and in its animal model, the mdx mouse. We designed a customized, mouse-specific Fluidic-Card-TaqMan-based assay (Fluid-CIRC) containing thirty-two genes related to circadian rhythm and muscle regeneration and analyzed gastrocnemius and tibialis anterior muscles from both unexercised and exercised mdx mice. Based on this first analysis, we prioritized the 7 most deregulated genes in mdx mice and tested their expression in skeletal muscle biopsies from 10 Duchenne patients. We found that CSNK1E, SIRT1, and MYOG are upregulated in DMD patient biopsies, consistent with the mdx data. We also demonstrated that their proteins are detectable and measurable in the DMD patients' plasma. We suggest that CSNK1E, SIRT1, and MYOG might represent exploratory circadian biomarkers in DMD.<br />QC 20220301

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1280633984
Document Type :
Electronic Resource
Full Text :
https://doi.org/10.3389.fphys.2021.678974