| Literature DB >> 30664732 |
Min Jia1, Xiayan Liu1, Hui Xue1, Yue Wu2,3, Lin Shi2,3, Rui Wang1,4, Yu Chen1, Ni Xu1, Jun Zhao1, Jingxia Shao1, Yafei Qi1, Lijun An1, Jen Sheen2,3, Fei Yu5.
Abstract
Protein homeostasis is essential for cellular functions and longevity, and the loss of proteostasis is one of the hallmarks of senescence. Autophagy is an evolutionarily conserved cellular degradation pathway that is critical for the maintenance of proteostasis. Paradoxically, autophagy deficiency leads to accelerated protein loss by unknown mechanisms. We discover that the ABNORMAL SHOOT3 (ABS3) subfamily of multidrug and toxic compound extrusion transporters promote senescence under natural and carbon-deprivation conditions in Arabidopsis thaliana. The senescence-promoting ABS3 pathway functions in parallel with the longevity-promoting autophagy to balance plant senescence and survival. Surprisingly, ABS3 subfamily multidrug and toxic compound extrusion proteins interact with AUTOPHAGY-RELATED PROTEIN 8 (ATG8) at the late endosome to promote senescence and protein degradation without canonical cleavage and lipidation of ATG8. This non-autophagic ATG8-ABS3 interaction paradigm is probably conserved among dicots and monocots. Our findings uncover a previously unknown non-autophagic function of ATG8 and an unrecognized senescence regulatory pathway controlled by ATG8-ABS3-mediated proteostasis.Entities:
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Year: 2019 PMID: 30664732 PMCID: PMC6368864 DOI: 10.1038/s41477-018-0348-x
Source DB: PubMed Journal: Nat Plants ISSN: 2055-0278 Impact factor: 15.793