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Abstract
We have used line HS-2 of Drosophila melanogaster, carrying a silenced transgene in the pericentric heterochromatin, to investigate in detail the chromatin structure imposed by this environment. Digestion of the chromatin with micrococcal nuclease (MNase) shows a nucleosome array with extensive long-range order, indicating regular spacing, and with well-defined MNase cleavage fragments, indicating a smaller MNase target in the linker region. The repeating unit is ca. 10 bp larger than that observed for bulkDrosophila chromatin. The silenced transgene shows both a loss of DNase I-hypersensitive sites and decreased sensitivity to DNase I digestion within an array of nucleosomes lacking such sites; within such an array, sensitivity to digestion by MNase is unchanged. The ordered nucleosome array extends across the regulatory region of the transgene, a shift that could explain the loss of transgene expression in heterochromatin. Highly regular nucleosome arrays are observed over several endogenous heterochromatic sequences, indicating that this is a general feature of heterochromatin. However, genes normally active within heterochromatin (rolled and light) do not show this pattern, suggesting that the altered chromatin structure observed is associated with regions that are silent, rather than being a property of the domain as a whole. The results indicate that long-range nucleosomal ordering is linked with the heterochromatic packaging that imposes gene silencing.
ACKNOWLEDGMENTS
We thank Lori L. Wallrath (University of Iowa) for important contributions during the initial stages of this work and Lori Wallrath, Joel Eissenberg, and members of the Elgin lab for review and discussion of the manuscript. We thank S. Lawrence Zipursky (University of California, Los Angeles) for providing the rolled cDNA probe, Barbara Wakimoto (University of Washington) for providing the light DNA probe, and Sergio Pimpinelli (Rome, Italy) for providing the probes for endogenous transposable elements.
This work was supported by Public Health Service grant HD23844 from the National Institute of Child Health and Human Development to S.C.R.E.