Journal article

Discovery and characterization of ZUFSP/ZUP1, a distinct deubiquitinase class important for genome stability

Abstract:: Deubiquitinating enzymes (DUBs) are important regulators of ubiquitin signaling. Here, we report the discovery of deubiquitinating activity in ZUFSP/C6orf113. High-resolution crystal structures of ZUFSP in complex with ubiquitin reveal several distinctive features of ubiquitin recognition and catalysis. Our analyses reveal that ZUFSP is a novel DUB with no homology to any known DUBs, leading us to classify ZUFSP as the seventh DUB family. Intriguingly, the minimal catalytic domain does not cleave polyubiquitin. We identify two ubiquitin binding domains in ZUFSP: a ZHA (ZUFSP helical arm) that binds to the distal ubiquitin and an atypical UBZ domain in ZUFSP that binds to polyubiquitin. Importantly, both domains are essential for ZUFSP to selectively cleave K63-linked polyubiquitin. We show that ZUFSP localizes to DNA lesions, where it plays an important role in genome stability pathways, functioning to prevent spontaneous DNA damage and also promote cellular survival in response to exogenous DNA damage.

Publication status:: Published

Peer review status:: Peer reviewed

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APA Style

Kwasna, D., Rehman, S. A., Natarajan, J., Matthews, S., Madden, R., De Cesare, V., Weidlich, S., Virdee, S., Ahel, I., Gibbs-Seymour, I., & Kulathu, Y. (2018). Discovery and characterization of ZUFSP/ZUP1, a distinct deubiquitinase class important for genome stability. Molecular Cell, 70(1), 150–164.e6.

MLA Style

Kwasna, D., et al. “Discovery and Characterization of ZUFSP/ZUP1, a Distinct Deubiquitinase Class Important for Genome Stability.” Molecular Cell, vol. 70, no. 1, Elsevier, 2018, pp. 150–64.e6.

Chicago Style

Kwasna, D, SA Rehman, J Natarajan, S Matthews, R Madden, V De Cesare, S Weidlich, et al. 2018. “Discovery and Characterization of ZUFSP/ZUP1, a Distinct Deubiquitinase Class Important for Genome Stability.” Molecular Cell 70 (1): 150–64.e6.
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Files:: 1-s2.0-S1097276518301424-mmc2-3.pdf

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Publisher copy:: 10.1016/j.molcel.2018.02.023

Authors

+ Kwasna, D More by this author

Role:: Author

+ Rehman, SA More by this author

Role:: Author

+ Natarajan, J More by this author

Role:: Author

+ Matthews, S More by this author

Role:: Author

+ Madden, R More by this author

Role:: Author

More authors...

+ European Research Council More from this funder

Grant:: 677623

+ Medical Research Council More from this funder

Grant:: MC_UU_12016/6

+ Cancer Research UK More from this funder

Grant:: C35050/A22284

+ Wellcome Trust More from this funder

Grant:: 101794

+ European Commission More from this funder

Grant:: 281739

Publisher:: Elsevier
Journal:: Molecular Cell More from this journal
Volume:: 70
Issue:: 1
Pages:: 150-164.e6
Publication date:: 2018-03-22
Acceptance date:: 2018-02-15
DOI:: 10.1016/j.molcel.2018.02.023
EISSN:: 1097-4164
ISSN:: 1097-2765
Pmid:: 29576527

Language:: English
Keywords:: FFR
Pubs id:: pubs:833761
UUID:: uuid:024b479e-8954-4019-9dc6-836f56d052c1
Local pid:: pubs:833761
Source identifiers:: 833761
Deposit date:: 2019-07-01

Terms of use

Copyright holder:: Kwasna et al
Copyright date:: 2018
Notes:: © The Authors. Published by Elsevier Inc. This is an open access article under the CC BY license.

Licence:: CC Attribution (CC BY)

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