The Centre for Modeling Human Disease Gene Trap resource

doi:10.1093/nar/gkh106

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Nucleic Acids Research, 2004, Vol. 32, Database issue D557-D559
© 2004 Oxford University Press

The Centre for Modeling Human Disease Gene Trap resource

Christine To¹, Trevor Epp¹^,2, Tammy Reid¹^,2, Qing Lan¹^,2, Mei Yu¹^,2, Carol Y. J. Li¹^,2, Minako Ohishi¹^,2, Paula Hant¹, Nora Tsao¹, Guillermo Casallo¹^,3, Janet Rossant¹^,4, Lucy R. Osborne¹^,3^,4 and William L. Stanford^*^,1^,2^,5

¹ Centre for Modeling Human Disease, Samuel Lunenfeld Research Institute, Mount Sinai Hospital, Toronto, Canada, ² Institute of Biomaterials and Biomedical Engineering, ³ Department of Medicine, ⁴ Department of Molecular and Medical Genetics and ⁵ Institute of Medical Science, University of Toronto, Canada

*To whom correspondence should be addressed at Institute of Biomaterials and Biomedical Engineering, University of Toronto, 4 Taddle Creek Road, Room 407, Rosebrugh Building, Toronto, Ontario M5S 3G9, Canada. Tel: +1 416 946 8379; Fax: +1 416 978 4317; Email: william.stanford{at}utoronto.ca
The authors wish it to be known that, in their opinion, the first two authors should be regarded as joint First Authors

Gene trap mutagenesis of mouse embryonic stem cells generatesrandom loss-of-function mutations, which can be identified bya sequence tag and can often report the endogenous expressionof the mutated gene. The Centre for Modeling Human Disease isperforming expression- and sequence-based screens of gene trapinsertions to generate new mouse mutations as a resource forthe scientific community. The gene trap insertions are screenedusing multiplexed in vitro differentiation and induction assays,and sequence tags are generated to complement expression profiles.Researchers may search for insertions in genes expressed intarget cell lineages, under specific in vitro conditions, orbased upon sequence identity via an online searchable database(http://www.cmhd.ca/sub/genetrap.asp). The clones are availableas a resource to researchers worldwide to help to functionallyannotate the mammalian genome and will serve as a source totest candidate loci identified by phenotype-driven mutagenesisscreens.

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