Reference: Kemble DJ, et al. (2013) Structure of the Spt16 middle domain reveals functional features of the histone chaperone FACT. J Biol Chem 288(15):10188-94

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Abstract


The histone chaperone FACT is an essential and abundant heterodimer found in all eukaryotes. Here we report a crystal structure of the middle domain of the large subunit of FACT (Spt16-M) to reveal a double pleckstrin homology architecture. This structure was found previously in the Pob3-M domain of the small subunit of FACT and in the related histone chaperone Rtt106, although Spt16-M is distinguished from these structures by the presence of an extended α-helix and a C-terminal addition. Consistent with our finding that the double pleckstrin homology structure is common to these three histone chaperones and reports that Pob3 and Rtt106 double pleckstrin homology domains bind histones H3-H4, we also find that Spt16-M binds H3-H4 with low micromolar affinity. Our structure provides a framework for interpreting a large body of genetic data regarding the physiological functions of FACT, including the identification of potential interaction surfaces for binding histones or other proteins.

Reference Type
Journal Article | Research Support, N.I.H., Extramural
Authors
Kemble DJ, Whitby FG, Robinson H, McCullough LL, Formosa T, Hill CP
Primary Lit For
SPT16
Additional Lit For
HHF1 | HHT1 | HHF2 | HHT2 | POB3 | RTT106

Interaction Annotations


Genetic Interactions

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Interactor Interactor Allele Assay Annotation Action Phenotype SGA score P-value Source Reference

Physical Interactions 1 entry for 2 genes

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InteractorInteractorAssayAnnotationActionModification

Bound to Xenopus laevus H3-H4 histones

SPT16POB3Reconstituted Complexmanually curatedBait-HitNo Modification
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