自噬
生物
细胞生物学
过氧化物酶体
泛素
受体
生物化学
基因
细胞凋亡
作者
Elizabeth Deosaran,Kenneth Bowitz Larsen,Rong Hua,Graeme Sargent,Yuqing Wang,Sarah Kim,Trond Lamark,Miluska Jauregui,Kelsey B. Law,Jennifer Lippincott-Schwartz,Andreas Brech,Terje Johansen,Peter K. Kim
摘要
Selective macro-autophagy is an intracellular process by which large cytoplasmic materials are selectively sequestered and degraded in the lysosomes. Substrate selection is mediated by ubiquitination and recruitment of ubiquitin-binding autophagic receptors such as p62, NBR1, NDP52 and Optineurin. Although it has been shown that these receptors act cooperatively to target some types of substrates to nascent autophagosomes, their precise roles are not well understood. Here, we examined selective autophagic degradation of peroxisomes (pexophagy), and found that NBR1 is necessary and sufficient for pexophagy. Mutagenesis studies of NBR1 showed that the amphipathic α-helical J domain, the ubiquitin-associated (UBA) domain, the LC3 interacting region and the coiled-coil domain are necessary to mediate pexophagy. Strikingly, substrate selectivity is partly achieved by NBR1 itself by coincident binding of the J and UBA domains to peroxisomes. Although p62 is not required when NBR1 is in excess, its binding to NBR1 increases the efficiency of NBR1 mediated pexophagy. Together, these results suggest that NBR1 is the specific autophagy receptor for pexophagy.
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