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A nanobody-based molecular toolkit for ubiquitin–proteasome system explores the main role of survivin subcellular localization

Hui Miao, Chang Liu, Hao Ouyang, Peiwen Zhang, Yuping Liu, Chen Zhang, Changping Deng, Yunhui Fu, Jinping Niu, Wenyun Zheng, Fang You, Yi Yang, Xingyuan Ma

2023Frontiers in Bioengineering and Biotechnology15 citationsDOIOpen Access PDF

Abstract

Targeted protein degradation is a powerful tool for determining the function of specific proteins nowadays. Survivin is the smallest member of the inhibitor of the apoptosis protein (IAP) family. It exists in the cytoplasm and nucleus of cells, but the exact function of survivin in different subcellular locations retained unclear updates due to the lack of effective and simple technical means. In this study, we created a novel nanoantibody-based molecular toolkit, namely, the ubiquitin-proteasome system (Nb4A-Fc-T2A-TRIM21), that can target to degrade survivin localized in cytoplasmic and cell nuclear by ubiquitinating, and by which to verify the potential roles of survivin subcellular localization. Also, the results showed that the cytoplasmic survivin mainly plays an anti-apoptotic function by directly or indirectly inhibiting the caspase pathway, and the nuclear survivin mainly promotes cell proliferation and participates in the regulation of the cell cycle. In addition, the Nb4A-Fc-T2A-TRIM21 system can degrade the endogenous survivin protein in a large amount by the ubiquitin-proteasome pathway, and the system can provide theoretical support for ubiquitination degradation targeting other endogenous proteins.

Topics & Concepts

SurvivinProteasomeSubcellular localizationUbiquitinCell biologyCytoplasmFunction (biology)Nuclear export signalInhibitor of apoptosisProtein degradationNuclear localization sequenceApoptosisChemistryProtein subcellular localization predictionCell nucleusBiologyBiochemistryProgrammed cell deathGeneCell death mechanisms and regulationUbiquitin and proteasome pathwaysAutophagy in Disease and Therapy