The chromatin-specific transcription elongation factor FACT comprises human SPT16 and SSRP1 proteins

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作者
George Orphanides
Wei-Hua Wu
William S. Lane
Michael Hampsey
Danny Reinberg
机构
[1] Howard Hughes Medical Institute,Division of Nucleic Acids Enzymology, Department of Biochemistry
[2] University of Medicine and Dentistry of New Jersey,undefined
[3] Robert Wood Johnson Medical School,undefined
[4] Harvard Microchemistry Facility,undefined
[5] Harvard University,undefined
来源
Nature | 1999年 / 400卷
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摘要
The regulation of gene expression depends critically upon chromatin structure1. Transcription of protein-coding genes can be reconstituted on naked DNA with only the general transcription factors and RNA polymerase II (ref. 2). This minimal system cannot transcribe DNA packaged into chromatin, indicating thataccessory factors may facilitate access to DNA. Two classes of accessory factor, ATP-dependent chromatin-remodelling enzymes3 and histone acetyltransferases4, facilitate transcription initiation from chromatin templates. FACT (for facilitates chromatin transcription) is a chromatin-specific elongation factor required for transcription of chromatin templates in vitro5,6. Here we show that FACT comprises a new human homologue of the Saccharomyces cerevisiae Spt16/Cdc68 protein and the high-mobility group-1-like protein structure-specific recognition protein-1. Yeast SPT16/CDC68 is an essential gene that has been implicated in transcription and cell-cycle regulation. Consistent with our biochemical analysis of FACT, we provide evidence that Spt16/Cdc68 is involved in transcript elongation in vivo. Moreover, FACT specifically interacts with nucleosomes and histone H2A/H2B dimers, indicating that it may work by promoting nucleosome disassembly upon transcription. In support of this model, we show that FACT activity is abrogated by covalently crosslinking nucleosomal histones.
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页码:284 / 288
页数:4
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