Structure and Regulation of the C-Fes Protein-tyrosine Kinase

Overview

Journal Front Biosci (Landmark Ed)

Specialty Biology

Date 2011 May 31

PMID 21622225

Citations 3

Authors

Sabine Hellwig

Thomas E Smithgall

Affiliations

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Abstract

The c-Fes protein-tyrosine kinase is the normal cellular ortholog of several avian and feline retroviral oncoproteins. Unlike its transforming viral counterparts, c-Fes tyrosine kinase activity is tightly regulated in vivo through a mechanism involving coiled-coil oligomerization domains and other unique structural features found in its long N-terminal region. This review is focused on the regulatory features and structural biology of c-Fes, which has been implicated in normal cellular growth regulation, the innate immune response, and tumorigenesis.

Citing Articles

Dual inhibition of Fes and Flt3 tyrosine kinases potently inhibits Flt3-ITD+ AML cell growth.

Weir M, Hellwig S, Tan L, Liu Y, Gray N, Smithgall T PLoS One. 2017; 12(7):e0181178.

PMID: 28727840 PMC: 5519068. DOI: 10.1371/journal.pone.0181178.

Constitutive MHC class I molecules negatively regulate TLR-triggered inflammatory responses via the Fps-SHP-2 pathway.

Xu S, Liu X, Bao Y, Zhu X, Han C, Zhang P Nat Immunol. 2012; 13(6):551-9.

PMID: 22522491 DOI: 10.1038/ni.2283.

Small-molecule inhibitors of the c-Fes protein-tyrosine kinase.

Hellwig S, Miduturu C, Kanda S, Zhang J, Filippakopoulos P, Salah E Chem Biol. 2012; 19(4):529-40.

PMID: 22520759 PMC: 3334838. DOI: 10.1016/j.chembiol.2012.01.020.