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. 2010 Oct 8;584(19):4163-8.
doi: 10.1016/j.febslet.2010.09.006. Epub 2010 Sep 8.

A disulfide driven domain swap switches off the activity of Shigella IpaH9.8 E3 ligase

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A disulfide driven domain swap switches off the activity of Shigella IpaH9.8 E3 ligase

Arefeh Seyedarabi et al. FEBS Lett. .
Free article

Abstract

We show that the monomeric form of Shigella IpaH9.8 E3 ligase catalyses the ubiquitination of human U2AF35 in vitro, providing a molecular mechanism for the observed in vivo effect. We further discover that under non-reducing conditions IpaH9.8 undergoes a domain swap driven by the formation of a disulfide bridge involving the catalytic cysteine and that this dimer is unable to catalyse the ubiquitination of U2AF35. The crystal structure of the domain-swapped dimer is presented. The redox inactivation of IpaH9.8 could be a mechanism of regulating the activity of the IpaH9.8 E3 ligase in response to cell damage so that the host cell in which the bacteria resides is maintained in a benign state suitable for bacterial survival.

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