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CpG islands in human X-inactivation

CpG islands in human X-inactivation
CpG islands in human X-inactivation
Sequence comparison analyses have been carried out for 19 genes escaping X-inactivation versus 73 genes subject to X-inactivation, and 100 randomly chosen X chromosome genes versus 100 randomly chosen autosomal genes. The coding sequence of the genes and their upstream and downstream flanking sequences were investigated using a series of windows (1 kb, 2 kb, 5 kb, 10 kb and 100 kb). No significant difference in number of LINE-L1 elements was observed in genes escaping X-inactivation compared to genes subject to X-inactivation. This result, therefore, does not support the suggestion that lack of LINE repeat elements is a key factor for genes escaping X-inactivation. However, significantly reduced numbers of CpG islands and SINE MIR elements were found to be associated with genes escaping X-inactivation. Compared to genes known to be inactivated, genes escaping X-inactivation were observed to have fewer CpG islands, particularly within the 2 kb upstream flanking sequence close to the coding region. The results suggest that CpG islands may play a role in the process of X-inactivation by providing sufficient DNA methylation targets for the maintenance of X-inactivation. Lack of CpG islands may be a major reason for genes escaping X-inactivation regulation.
0003-4800
242-249
Ke, X.
7ce19883-4155-4457-b239-efe78e8087ff
Collins, A.
7daa83eb-0b21-43b2-af1a-e38fb36e2a64
Ke, X.
7ce19883-4155-4457-b239-efe78e8087ff
Collins, A.
7daa83eb-0b21-43b2-af1a-e38fb36e2a64

Ke, X. and Collins, A. (2003) CpG islands in human X-inactivation. Annals of Human Genetics, 67 (3), 242-249. (doi:10.1046/j.1469-1809.2003.00038.x).

Record type: Article

Abstract

Sequence comparison analyses have been carried out for 19 genes escaping X-inactivation versus 73 genes subject to X-inactivation, and 100 randomly chosen X chromosome genes versus 100 randomly chosen autosomal genes. The coding sequence of the genes and their upstream and downstream flanking sequences were investigated using a series of windows (1 kb, 2 kb, 5 kb, 10 kb and 100 kb). No significant difference in number of LINE-L1 elements was observed in genes escaping X-inactivation compared to genes subject to X-inactivation. This result, therefore, does not support the suggestion that lack of LINE repeat elements is a key factor for genes escaping X-inactivation. However, significantly reduced numbers of CpG islands and SINE MIR elements were found to be associated with genes escaping X-inactivation. Compared to genes known to be inactivated, genes escaping X-inactivation were observed to have fewer CpG islands, particularly within the 2 kb upstream flanking sequence close to the coding region. The results suggest that CpG islands may play a role in the process of X-inactivation by providing sufficient DNA methylation targets for the maintenance of X-inactivation. Lack of CpG islands may be a major reason for genes escaping X-inactivation regulation.

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Published date: May 2003

Identifiers

Local EPrints ID: 24803
URI: http://eprints.soton.ac.uk/id/eprint/24803
ISSN: 0003-4800
PURE UUID: fb8c0b35-bfde-4906-abe2-1c872e8c0714
ORCID for A. Collins: ORCID iD orcid.org/0000-0001-7108-0771

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Date deposited: 04 Apr 2006
Last modified: 16 Mar 2024 02:42

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Contributors

Author: X. Ke
Author: A. Collins ORCID iD

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