학술논문
Mitochondrial dysfunction reactivates α-fetoprotein expression that drives copper-dependent immunosuppression in mitochondrial disease models
Document Type
article
Author
Kimberly A. Jett; Zakery N. Baker; Amzad Hossain; Aren Boulet; Paul A. Cobine; Sagnika Ghosh; Philip Ng; Orhan Yilmaz; Kris Barreto; John DeCoteau; Karen Mochoruk; George N. Ioannou; Christopher Savard; Sai Yuan; Osama H.M.H. Abdalla; Christopher Lowden; Byung-Eun Kim; Hai-Ying Mary Cheng; Brendan J. Battersby; Vishal M. Gohil; Scot C. Leary
Source
The Journal of Clinical Investigation, Vol 133, Iss 1 (2023)
Subject
Language
English
ISSN
1558-8238
Abstract
Signaling circuits crucial to systemic physiology are widespread, yet uncovering their molecular underpinnings remains a barrier to understanding the etiology of many metabolic disorders. Here, we identified a copper-linked signaling circuit activated by disruption of mitochondrial function in the murine liver or heart that resulted in atrophy of the spleen and thymus and caused a peripheral white blood cell deficiency. We demonstrated that the leukopenia was caused by α-fetoprotein, which required copper and the cell surface receptor CCR5 to promote white blood cell death. We further showed that α-fetoprotein expression was upregulated in several cell types upon inhibition of oxidative phosphorylation. Collectively, our data argue that α-fetoprotein may be secreted by bioenergetically stressed tissue to suppress the immune system, an effect that may explain the recurrent or chronic infections that are observed in a subset of mitochondrial diseases or in other disorders with secondary mitochondrial dysfunction.