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  Heat-Shock Protein 90 Controls the Expression of Cell-Cycle Genes by Stabilizing Metazoan-Specific Host-Cell Factor HCFC1

Antonova, A., Hummel, B., Khavaran, A., Redhaber, D. M., Aprile-Garcia, F., Rawat, P., et al. (2019). Heat-Shock Protein 90 Controls the Expression of Cell-Cycle Genes by Stabilizing Metazoan-Specific Host-Cell Factor HCFC1. Cell Reports, 29, 1645-1659. doi:org/10.1016/j.celrep.2019.09.084.

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 Creators:
Antonova, Aneliya1, Author
Hummel, Barbara1, Author
Khavaran, Ashkan1, Author
Redhaber, Desiree M.2, Author
Aprile-Garcia, Fernando1, Author
Rawat, Prashant1, Author
Gundel, Kathrin1, Author
Schneck, Megan1, Author
Hansen, Erik C.1, Author
Mitschke, Jan2, Author
Mittler, Gerhard1, Author
Miething, Cornelius2, Author
Sawarkar, Ritwick1, Author           
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1Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society, ou_2243642              
2External Organizations, ou_persistent22              

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 Abstract: Molecular chaperones such as heat-shock proteins (HSPs) help in protein folding. Their function in the cytosol has been well studied. Notably, chaperones are also present in the nucleus, a compartment where proteins enter after completing de novo folding in the cytosol, and this raises an important question about chaperone function in the nucleus. We performed a systematic analysis of the nuclear pool of heat-shock protein 90. Three orthogonal and independent analyses led us to the core functional interactome of HSP90. Computational and biochemical analyses identify host cell factor C1 (HCFC1) as a transcriptional regulator that depends on HSP90 for its stability. HSP90 was required to maintain the expression of HCFC1-targeted cell-cycle genes. The regulatory nexus between HSP90 and the HCFC1 module identified in this study sheds light on the relevance of chaperones in the transcription of cell-cycle genes. Our study also suggests a therapeutic avenue of combining chaperone and transcription inhibitors for cancer treatment.

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Language(s): eng - English
 Dates: 2019-11-05
 Publication Status: Issued
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 Rev. Type: Peer
 Identifiers: DOI: org/10.1016/j.celrep.2019.09.084
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Title: Cell Reports
Source Genre: Journal
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Publ. Info: Maryland Heights, MO : Cell Press
Pages: - Volume / Issue: 29 Sequence Number: - Start / End Page: 1645 - 1659 Identifier: ISSN: 2211-1247
CoNE: https://pure.mpg.de/cone/journals/resource/2211-1247