| Literature DB >> 34479963 |
M Nieves Calvo-Vidal1, Nahuel Zamponi1, Jan Krumsiek2, Max A Stockslager3, Maria V Revuelta1, Jude M Phillip1, Rossella Marullo1, Ekaterina Tikhonova4, Nikita Kotlov4, Jayeshkumar Patel1, Shao Ning Yang1, Lucy Yang5, Tony Taldone6, Catherine Thieblemont7,8, John P Leonard1, Peter Martin1, Giorgio Inghirami9, Gabriela Chiosis6, Scott R Manalis3,5,10, Leandro Cerchietti11.
Abstract
HSP90 is critical for maintenance of the cellular proteostasis. In cancer cells, HSP90 also becomes a nucleating site for the stabilization of multiprotein complexes including signaling pathways and transcription complexes. Here we described the role of this HSP90 form, referred to as oncogenic HSP90, in the regulation of cytosolic metabolic pathways in proliferating B-cell lymphoma cells. Oncogenic HSP90 assisted in the organization of metabolic enzymes into non-membrane-bound functional compartments. Under experimental conditions that conserved cellular proteostasis, oncogenic HSP90 coordinated and sustained multiple metabolic pathways required for energy production and maintenance of cellular biomass as well as for secretion of extracellular metabolites. Conversely, inhibition of oncogenic HSP90, in absence of apparent client protein degradation, decreased the efficiency of MYC-driven metabolic reprogramming. This study reveals that oncogenic HSP90 supports metabolism in B-cell lymphoma cells and patients with diffuse large B-cell lymphoma, providing a novel mechanism of activity for HSP90 inhibitors. SIGNIFICANCE: The oncogenic form of HSP90 organizes and maintains functional multienzymatic metabolic hubs in cancer cells, suggesting the potential of repurposing oncogenic HSP90 selective inhibitors to disrupt metabolism in lymphoma cells. ©2021 The Authors; Published by the American Association for Cancer Research.Entities:
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Year: 2021 PMID: 34479963 PMCID: PMC8530929 DOI: 10.1158/0008-5472.CAN-21-2734
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701