AI Article Synopsis

  • The human genome comprises around 600 ubiquitin E3 ligases, with many being single-subunit E3s (ssE3s) that interact with both substrates and ubiquitin-loaded E2 enzymes.
  • RNF4, a specific ssE3 ligase, features a disordered N-terminal region with SIMs crucial for binding SUMO-modified substrates, while maintaining a compact structure despite lacking secondary structure.
  • Findings demonstrate that distinct charged regions in RNF4's N-terminus facilitate its proper configuration, essential for efficient substrate ubiquitination, and mutations that alter this shape reduce its activity.

Article Abstract

The human genome contains an estimated 600 ubiquitin E3 ligases, many of which are single-subunit E3s (ssE3s) that can bind to both substrate and ubiquitin-loaded E2 (E2~Ub). Within ssE3s structural disorder tends to be located in substrate binding and domain linking regions. RNF4 is a ssE3 ligase with a C-terminal RING domain and disordered N-terminal region containing SUMO Interactions Motifs (SIMs) required to bind SUMO modified substrates. Here we show that, although the N-terminal region of RNF4 bears no secondary structure, it maintains a compact global architecture primed for SUMO interaction. Segregated charged regions within the RNF4 N-terminus promote compaction, juxtaposing RING domain and SIMs to facilitate substrate ubiquitination. Mutations that induce a more extended shape reduce ubiquitination activity. Our result offer insight into a key step in substrate ubiquitination by a member of the largest ubiquitin ligase subtype and reveal how a defined architecture within a disordered region contributes to E3 ligase function.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7393505PMC
http://dx.doi.org/10.1038/s41467-020-17647-xDOI Listing

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