NDP52 interacts with mitochondrial RNA poly(A) polymerase to promote mitophagy

Norihiko Furuya; Soichiro Kakuta; Katsuhiko Sumiyoshi; Maya Ando; Risa Nonaka; Ayami Suzuki; Saiko Kazuno; Shinji Saiki; Nobutaka Hattori

doi:10.15252/embr.201846363

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Article

Author Affiliations

Norihiko Furuya (nohuruya{at}juntendo.ac.jp)*,¹,²,³,
Soichiro Kakuta⁴,⁵,
Katsuhiko Sumiyoshi⁶,⁷,
Maya Ando³,
Risa Nonaka⁸,
Ayami Suzuki³,
Saiko Kazuno⁹,
Shinji Saiki¹,³ and
Nobutaka Hattori (nhattori{at}juntendo.ac.jp)*,³

¹Division for Development of Autophagy Modulating Drugs, Juntendo University Graduate School of Medicine, Tokyo, Japan
²Department of Neuroscience for Neurodegenerative Disorders, Juntendo University Graduate School of Medicine, Tokyo, Japan
³Department of Neurology, Juntendo University Graduate School of Medicine, Tokyo, Japan
⁴Laboratory of Morphology and Image Analysis, Biomedical Research Center, Juntendo University Graduate School of Medicine, Tokyo, Japan
⁵Department of Cellular and Molecular Neuropathology, Juntendo University Graduate School of Medicine, Tokyo, Japan
⁶Department of Health and Nutrition Collage of Human Science, Tokiwa University, Ibaraki, Japan
⁷Department of Cardiovascular Medicine, Juntendo University Graduate School of Medicine, Tokyo, Japan
⁸Research Institute for Diseases of Old Age, Juntendo University Graduate School of Medicine, Tokyo, Japan
⁹Laboratory of Proteomics and Biomolecular Science, Research Support Center, Juntendo University Graduate School of Medicine, Tokyo, Japan

↵* Corresponding author. Tel: +81 3 3813 3111; Fax: +81 3 5813 7440; E‐mail: nohuruya{at}juntendo.ac.jp
Corresponding author. Tel: +81 3 3813 3111; Fax: +81 3 5800 0547; E‐mail: nhattori{at}juntendo.ac.jp

View Abstract

Abstract

Parkin‐mediated mitophagy is a quality control pathway that selectively removes damaged mitochondria via the autophagic machinery. Autophagic receptors, which interact with ubiquitin and Atg8 family proteins, contribute to the recognition of damaged mitochondria by autophagosomes. NDP52, an autophagy receptor, is required for autophagic engulfment of damaged mitochondria during mitochondrial uncoupler treatment. The N‐terminal SKICH domain and C‐terminal zinc finger motif of NDP52 are both required for its function in mitophagy. While the zinc finger motif contributes to poly‐ubiquitin binding, the function of the SKICH domain remains unclear. Here, we show that NDP52 interacts with mitochondrial RNA poly(A) polymerase (MTPAP) via the SKICH domain. During mitophagy, NDP52 invades depolarized mitochondria and interacts with MTPAP dependent on the proteasome but independent of ubiquitin binding. Loss of MTPAP reduces NDP52‐mediated mitophagy, and the NDP52–MTPAP complex attracts more LC3 than NDP52 alone. These results indicate that NDP52 and MTPAP form an autophagy receptor complex, which enhances autophagic elimination of damaged mitochondria.

Synopsis

The autophagy receptor NDP52 interacts with mitochondrial RNA poly(A) polymerase (MTPAP), and the NDP52‐MTPAP complex contributes to the ubiquitin‐independent recognition of damaged mitochondria by autophagy.

NDP52 irrupts into mitochondria proteasome‐dependently, and interacts with MTPAP via its N‐terminal SKICH domain upon mitophagy‐inducing conditions.
The NDP52‐MTPAP complex attracts more LC3 to the damaged mitochondria than NDP52 alone.
NDP52 interacts with MTPAP and irrupts into mitochondria ubiquitin‐binding‐independently.