Secondary Structure Assignment of Mouse SOCS3 by NMR Defines the Domain Boundaries and Identifies an Unstructured Insertion in the SH2 Domain

Overview

Journal FEBS J

Specialty Biochemistry

Date 2005 Nov 24

PMID 16302975

Citations 26

Authors

Jeffrey J Babon

Shenggen Yao

David P DeSouza

Christopher F Harrison

Louis J Fabri

Edvards Liepinsh

Sergio D Scrofani

Manuel Baca

Raymond S Norton

Affiliations

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Abstract

SOCS3 is a negative regulator of cytokine signalling that inhibits Janus kinase-signal transduction and activator of transcription (JAK-STAT) mediated signal tranduction by binding to phosphorylated tyrosine residues on intracellular subunits of various cytokine receptors, as well as possibly the JAK proteins. SOCS3 consists of a short N-terminal sequence followed by a kinase inhibitory region, an extended SH2 domain and a C-terminal suppressor of cytokine signalling (SOCS) box. SOCS3 and the related protein, cytokine-inducible SH2-containing protein, are unique among the SOCS family of proteins in containing a region of mostly low complexity sequence, between the SH2 domain and the C-terminal SOCS box. Using NMR, we assigned and determined the secondary structure of a murine SOCS3 construct. The SH2 domain, unusually, consists of 140 residues, including an unstructured insertion of 35 residues. This insertion fits the criteria for a PEST sequence and is not required for phosphotyrosine binding, as shown by isothermal titration calorimetry. Instead, we propose that the PEST sequence has a functional role unrelated to phosphotyrosine binding, possibly mediating efficient proteolytic degradation of the protein. The latter half of the kinase inhibitory region and the entire extended SH2 subdomain form a single alpha-helix. The mapping of the true SH2 domain, and the location of its C terminus more than 50 residues further downstream than predicted by sequence homology, explains a number of previously unexpected results that have shown the importance of residues close to the SOCS box for phosphotyrosine binding.

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Williams J, Alotaiq N, Mullen W, Burchmore R, Liu L, Baillie G Nat Commun. 2018; 9(1):168.

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