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  Human chromosome 21 gene expression atlas in the mouse.

Reymond, A., Marigo, V., Yaylaoglu, M. B., Leoni, A., Ucla, C., Scamuffa, N., et al. (2002). Human chromosome 21 gene expression atlas in the mouse. Nature, 420(6915), 582-586. doi:10.1038/nature01178.

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Reymond, A., Author
Marigo, V., Author
Yaylaoglu, M. B., Author
Leoni, A., Author
Ucla, C., Author
Scamuffa, N., Author
Cacciopolli, C., Author
Dermitzakis, E. T., Author
Lyle, R., Author
Banfi, S., Author
Eichele, G.1, Author           
Antonarakis, S. E., Author
Ballabio, A., Author
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1Department of Molecular Embryology, Max Planck Institute for Experimental Endocrinology, Max Planck Society, ou_1565140              

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 Abstract: Genome-wide expression analyses have a crucial role in functional genomics. High resolution methods, such as RNA in situ hybridization provide an accurate description of the spatiotemporal distribution of transcripts as well as a three-dimensional 'in vivo' gene expression overview(1-5). We set out to analyse systematically the expression patterns of genes from an entire chromosome. We chose human chromosome 21 because of the medical relevance of trisomy 21 (Down's syndrome)(6). Here we show the expression analysis of all identifiable murine orthologues of human chromosome 21 genes (161 out of 178 confirmed human genes) by RNA in situ hybridization on whole mounts and tissue sections, and by polymerase chain reaction with reverse transcription on adult tissues. We observed patterned expression in several tissues including those affected in trisomy 21 phenotypes (that is, central nervous system, heart, gastrointestinal tract, and limbs). Furthermore, statistical analysis suggests the presence of some regions of the chromosome with genes showing either lack of expression or, to a lesser extent, co-expression in either lack of expression or, to a lesser extent, co-expression in specific tissues. This high resolution expression 'atlas' of an entire human chromosome is an important step towards the understanding of gene function and of the pathogenetic mechanisms in Down's syndrome.

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Language(s): eng - English
 Dates: 2002-12-05
 Publication Status: Issued
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 Rev. Type: Peer
 Identifiers: DOI: 10.1038/nature01178
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Title: Nature
Source Genre: Journal
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Pages: - Volume / Issue: 420 (6915) Sequence Number: - Start / End Page: 582 - 586 Identifier: -