Bhandari, Poonam ; Shashidhara, L. S. (2001) Studies on human colon cancer gene APC by targeted expression in Drosophila Oncogene, 20 (47). pp. 6871-6880. ISSN 0950-9232
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Official URL: http://www.nature.com/onc/journal/v20/n47/full/120...
Abstract
Mutations in human Adenomatous Polyposis Coli (APC) gene are associated with both familial and sporadic colorectal tumors. APC is known to down regulate β-catenin levels, a transducer of Wnt signaling. The aim of this study is to provide transgenic Drosophila expressing either full-length or truncated forms of human APC (hAPC) protein and methods for using them in functional genomics and drug screening. Consistent with its biochemical properties, targeted expression of either full-length hAPC or its β-catenin binding domain alone negatively regulated the function of the β-catenin homologue, Armadillo (Arm) and thereby, inhibited Wnt/Wg signaling during fly development. hAPC inhibited Arm function even in the absence of GSK-3β activity, although the latter was required to mediate the degradation of Arm. Consistent with this, hAPC suppressed the phenotypes induced by the over-expression of degradation-resistant forms of Arm. Subsequently, using hAPC-induced eye phenotypes as the assay in a suppressor-enhancer screen, we have identified two new loci in Drosophila, which modulate Wnt/Wg signaling. In addition, an anti-colon cancer drug, indomethacin, specifically enhanced hAPC-induced phenotypes.
Item Type: | Article |
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Source: | Copyright of this article belongs to Nature Publishing Group. |
ID Code: | 49658 |
Deposited On: | 20 Jul 2011 14:07 |
Last Modified: | 20 Jul 2011 14:07 |
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