Affiliation:
1. Programme in Developmental Genetics, The Babraham Institute, Cambridge CB2 4AT, United Kingdom
Abstract
ABSTRACT
The mouse
H19
gene is expressed from the maternal chromosome exclusively. A 2-kb region at 2 to 4 kb upstream of
H19
is paternally methylated throughout development, and these sequences are necessary for the imprinted expression of both
H19
and the 5′-neighboring
Igf2
gene. In particular, on the maternal chromosome this element appears to insulate the
Igf2
gene from enhancers located downstream of
H19
. We analyzed the chromatin organization of this element by assaying its sensitivity to nucleases in nuclei. Six DNase I hypersensitive sites (HS sites) were detected on the unmethylated maternal chromosome exclusively, the two most prominent of which mapped 2.25 and 2.75 kb 5′ to the
H19
transcription initiation site. Five of the maternal HS sites were present in expressing and nonexpressing tissues and in embryonic stem (ES) cells. They seem, therefore, to reflect the maternal origin of the chromosome rather than the expression of
H19
. A sixth maternal HS site, at 3.45 kb upstream of
H19
, was detected in ES cells only. The nucleosomal organization of this element was analyzed in tissues and ES cells by micrococcal nuclease digestion. Specifically on the maternal chromosome, an unusual and strong banding pattern was obtained, suggestive of a nonnucleosomal organization. From our studies, it appears that the unusual chromatin organization with the presence of HS sites (maternal chromosome) and DNA methylation (paternal chromosome) in this element are mutually exclusive and reflect alternate epigenetic states. In addition, our data suggest that nonhistone proteins are associated with the maternal chromosome and that these might be involved in its boundary function.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
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Mammalian Genetics Unit Harwell
United Kingdom World Wide Web (http://www.mgu.har.mrc.ac.uk
)
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64 articles.
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