Receptor-mediated mitophagy regulates EPO production and protects against renal anemia

Erythropoietin (EPO) drives erythropoiesis and is secreted mainly by the kidney upon hypoxic or anemic stress. The paucity of EPO production in renal EPO-producing cells (REPs) causes renal anemia, one of the most common complications of chronic nephropathies. Although mitochondrial dysfunction is c...

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Published ineLife Vol. 10
Main Authors Geng, Guangfeng, Liu, Jinhua, Xu, Changlu, Pei, Yandong, Chen, Linbo, Mu, Chenglong, Wang, Ding, Gao, Jie, Li, Yue, Liang, Jing, Zhao, Tian, Zhang, Chuanmei, Zhou, Jiaxi, Chen, Quan, Zhu, Yushan, Shi, Lihong
Format Journal Article
LanguageEnglish
Published England eLife Science Publications, Ltd 04.05.2021
eLife Sciences Publications Ltd
eLife Sciences Publications, Ltd
Subjects
Anemia
Apoptosis
B cells
Blood
Bone marrow
Cell Biology
Cytokines
Erythropoiesis
Erythropoietin
Flow cytometry
Fundc1
Homeostasis
Hypoxia
Inflammation
Kidney diseases
Kidneys
Kinases
Mitochondria
Mitophagy
Quality control
Reactive oxygen species
renal EPO-producing cells
Spleen
stress erythropoiesis
mouse
mitophagy
cell biology
Fundc1
inflammation
stress erythropoiesis
renal EPO-producing cells
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Summary:Erythropoietin (EPO) drives erythropoiesis and is secreted mainly by the kidney upon hypoxic or anemic stress. The paucity of EPO production in renal EPO-producing cells (REPs) causes renal anemia, one of the most common complications of chronic nephropathies. Although mitochondrial dysfunction is commonly observed in several renal and hematopoietic disorders, the mechanism by which mitochondrial quality control impacts renal anemia remains elusive. In this study, we showed that FUNDC1, a mitophagy receptor, plays a critical role in EPO-driven erythropoiesis induced by stresses. Mechanistically, EPO production is impaired in REPs in Fundc1 -/- mice upon stresses, and the impairment is caused by the accumulation of damaged mitochondria, which consequently leads to the elevation of the reactive oxygen species (ROS) level and triggers inflammatory responses by up-regulating proinflammatory cytokines. These inflammatory factors promote the myofibroblastic transformation of REPs, resulting in the reduction of EPO production. We therefore provide a link between aberrant mitophagy and deficient EPO generation in renal anemia. Our results also suggest that the mitochondrial quality control safeguards REPs under stresses, which may serve as a potential therapeutic strategy for the treatment of renal anemia.
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These authors contributed equally to this work.
ISSN:2050-084X
2050-084X
DOI:10.7554/eLife.64480