Please use this identifier to cite or link to this item: http://hdl.handle.net/123456789/1060
Title: BLM Potentiates c-Jun Degradation and Alters Its Function as an Oncogenic Transcription Factor
Authors: Sengupta, Sagar
Attri, Preeti
Priyadarshini, Raina
Hussain, Mansoor
Madhavan, Vinoth
Chowdhury, Shantanu
Kaur, Ekjot
Priya, Swati
Tripathi, Vivek
Dhapola, Parashar
Saha, Dhurjhoti
Keywords: AP-1 transcription factor; Bloom helicase; ChIP-seq; Fbw7α; RecQ helicase; SCF(Fbw7) complex; adaptor functions; c-Jun; c-Jun targets; mutants.
Issue Date: Jul-2018
Publisher: Elsevier Inc.
Abstract: Mutations in BLM helicase predispose Bloom syndrome (BS) patients to a wide spectrum of cancers. We demonstrate that MIB1-ubiquitylated BLM in G1 phase functions as an adaptor protein by enhancing the binding of transcription factor c-Jun and its E3 ligase, Fbw7α. BLM enhances the K48/K63-linked ubiquitylation on c-Jun, thereby enhancing the rate of its subsequent degradation. Functionally defective Fbw7α mutants prevalent in multiple human cancers are reactivated by BLM. However, BS patient-derived BLM mutants cannot potentiate Fbw7α-dependent c-Jun degradation. The decrease in the levels of c-Jun in cells expressing BLM prevents effective c-Jun binding to 2,584 gene promoters. This causes decreases in the transcript and protein levels of c-Jun targets in BLM-expressing cells, resulting in attenuated c-Jun-dependent effects during neoplastic transformation. Thus, BLM carries out its function as a tumor suppressor by enhancing c-Jun turnover and thereby preventing its activity as a proto-oncogene.
URI: http://hdl.handle.net/123456789/1060
Appears in Collections:Signal Transduction-II, Publications

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