Competition between linker histones and HMG1 for binding to four-way junction DNA: implications for transcription.

Both lysine-rich histones and high mobility group proteins 1 and 2 bind to linker DNA in chromatin. While the members of the histone H1 class are considered general repressors of transcription, HMG1/2 are viewed as activators. Using stable four-way junction DNA as a model for cross-overs of linker DNA at the entry and exit to nucleosomes, we show that HMG1 can compete efficiently with H1 for binding to four-way junctions. In contrast, the erythrocyte-specific histone H5 seems to be refractory to displacement by HMG1. The results suggest that replacement of histone H1 by HMG1 may be part of the transcriptional activation by HMG1.