AI Article Synopsis

  • Deubiquitinating enzymes (DUBs), linked to cancer processes like gene expression and DNA repair, include the newly discovered protein ZUFSP.
  • The study aims to identify ZUFSP's binding site using bioinformatics and explore how ZUFSP interacts with ubiquitin through molecular dynamics simulations.
  • Results show that the most druggable binding site was identified, and ubiquitin binding reduces ZUFSP motion, suggesting potential therapeutic targets involving ZUFSP.

Article Abstract

Background: Deubiquitinating enzymes (DUBs) protein family have been implicated in some deregulated pathways involved in carcinogeneses, such as cell cycle, gene expression, and DNA damage response (DDR). Zinc finger with UFM1-specific peptidase domain protein (ZUFSP) is one of the recently discovered members of the DUBs.

Objectives: To identify and cross-validate the ZUFSP binding site using the bioinformatic tools, including SiteMap&Metapocket, respectively. To understand the molecular basis of complementary ZUFSP-Ub interaction and associated structural events using MD Simulation.

Methods: In this study, four binding pockets were predicted, characterized, and cross-validated based on physiochemical features such as site score, druggability score, site volume, and site size. Also, a molecular dynamics simulation technique was employed to determine the impact of ubiquitin-binding on ZUFSP.

Results: Site 1 with a site score 1.065, Size 102, D scores 1.00, and size volume 261 was predicted to be the most druggable site. Structural studies revealed that upon ubiquitin-binding, the motional movement of ZUFSP was reduced when compared to the unbound ZUFSP. Also, the ZUFSP helical arm (ZHA) domain orient in such a way that it moves closer to the Ub; this orientation enables the formation of a UBD which is very peculiar to ZUFSP.

Conclusion: The impact of ubiquitin on ZUFSP movement and the characterization of its predicted druggable site can be targeted in the development of therapeutics.

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Source
http://dx.doi.org/10.2174/1386207324666210203175142DOI Listing

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