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Autophagic regulation of P62 is critical for cancer therapy

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dc.contributor.author Ariful, Islam
dc.contributor.author Sooro, MA
dc.date.accessioned 2023-06-16T06:12:20Z
dc.date.available 2023-06-16T06:12:20Z
dc.date.issued 2018-05-08
dc.identifier.uri http://hdl.handle.net/20.500.14155/1775
dc.description.abstract Sequestosome1 (p62/SQSTM 1) is a multidomain protein that interacts with the autophagy machinery as a key adaptor of target cargo. It interacts with phagophores through the LC3-interacting (LIR) domain and with the ubiquitinated protein aggregates through the ubiquitin-associated domain (UBA) domain. It sequesters the target cargo into inclusion bodies by its PB1 domain. This protein is further the central hub that interacts with several key signaling proteins. Emerging evidence implicates p62 in the induction of multiple cellular oncogenic transformations. Indeed, p62 upregulation and/or reduced degradation have been implicated in tumor formation, cancer promotion as well as in resistance to therapy. It has been established that the process of autophagy regulates the levels of p62. Autophagy-dependent apoptotic activity of p62 is recently being reported. It is evident that p62 plays a critical role in both autophagy and apoptosis. Therefore in this review we discuss the role of p62 in autophagy, apoptosis and cancer through its different domains and outline the importance of modulating cellular levels of p62 in cancer therapeutics. en
dc.description.sponsorship Self en
dc.language.iso en en
dc.publisher International Journal of Molecular Sciences en
dc.subject P62, PBI, self-oligomerization, autophagy, apoptotis, cancer, therapy en
dc.title Autophagic regulation of P62 is critical for cancer therapy en
dc.type Article en


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