Energy deficit-independent stress response in the Frataxin-depleted heart: evidence that Integrated Stress Response can predominate over mTORC1 activation

Cesar Vasquez,Monika Patel,Aishwarya Sivaramakrishnan,Carmen Bekeova,Lauren Anderson-Pullinger,Nadan Wang,Hsin-Yao Tang,Erin L. Seifert

Energy deficit-independent stress response in the Frataxin-depleted heart: evidence that Integrated Stress Response can predominate over mTORC1 activation

2021

Cesar Vasquez
Monika Patel
Aishwarya Sivaramakrishnan
Carmen Bekeova
Lauren Anderson-Pullinger
Nadan Wang
Hsin-Yao Tang
Erin L. Seifert

Friedreich ataxia (FRDA) is an inherited disorder caused by depletion of frataxin (FXN), a mitochondrial protein required for iron-sulfur cluster (ISC) biogenesis. Cardiac dysfunction is the main cause of death. Yet pathogenesis, and, more generally, how the heart adapts to FXN loss, remain poorly understood, though are expected to be linked to an energy deficit. We modified a transgenic (TG) mouse model of inducible FXN depletion that permits phenotypic evaluation of the heart at FXN levels 8 weeks with FXN levels

Keywords:

Frataxin
Cell biology
Transgene
Pathogenesis
Biogenesis
Phenotype
Ataxia
Biology
Integrated stress response
mTORC1

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