| Literature DB >> 30982665 |
Yakubu Princely Abudu1, Serhiy Pankiv2, Benan John Mathai2, Alf Håkon Lystad2, Christian Bindesbøll2, Hanne Britt Brenne1, Matthew Yoke Wui Ng2, Bernd Thiede3, Ai Yamamoto4, Thaddaeus Mutugi Nthiga1, Trond Lamark1, Camila V Esguerra5, Terje Johansen6, Anne Simonsen7.
Abstract
The clearance of damaged or dysfunctional mitochondria by selective autophagy (mitophagy) is important for cellular homeostasis and prevention of disease. Our understanding of the mitochondrial signals that trigger their recognition and targeting by mitophagy is limited. Here, we show that the mitochondrial matrix proteins 4-Nitrophenylphosphatase domain and non-neuronal SNAP25-like protein homolog 1 (NIPSNAP1) and NIPSNAP2 accumulate on the mitochondria surface upon mitochondrial depolarization. There, they recruit proteins involved in selective autophagy, including autophagy receptors and ATG8 proteins, thereby functioning as an "eat me" signal for mitophagy. NIPSNAP1 and NIPSNAP2 have a redundant function in mitophagy and are predominantly expressed in different tissues. Zebrafish lacking a functional Nipsnap1 display reduced mitophagy in the brain and parkinsonian phenotypes, including loss of tyrosine hydroxylase (Th1)-positive dopaminergic (DA) neurons, reduced motor activity, and increased oxidative stress.Entities:
Keywords: ALFY; NDP52; NIPSNAP1; NIPSNAP2; Parkin; TAX1BP1; autophagy; mitophagy; optineurin; p62/SQSTM1
Year: 2019 PMID: 30982665 DOI: 10.1016/j.devcel.2019.03.013
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270