| Literature DB >> 24931331 |
Marco Loddo1, Joanna Andryszkiewicz, Sara Rodriguez-Acebes, Kai Stoeber, Allison Jones, Dimitra Dafou, Sophia Apostolidou, Alex Wollenschlaeger, Martin Widschwendter, Richard Sainsbury, Slavica Tudzarova, Gareth Haydn Williams.
Abstract
Aberrant mitosis is a common feature of cancer, yet little is known about the altered genes causing mitotic defects. We screened human tumours for cells with morphological signatures of highly specific mitotic defects previously assigned to candidate genes in a genome-wide RNA interference screen carried out in HeLa cells (www.mitocheck.org). We discovered a striking enrichment of early mitotic configurations indicative of prophase/prometaphase delay in breast cancer. Promoter methylation analysis of MitoCheck candidate genes assigned to the corresponding 'mitotic delay' class linked this defect to epigenetic silencing of the gene encoding pregnancy-associated plasma protein-A (PAPPA), a secreted protease. PAPPA silencing was highly prevalent in precursor lesions and invasive breast cancer. Experimental manipulation of PAPPA protein levels in human mammary epithelial cells and in breast cancer cell lines demonstrates that progression through early mitosis is dependent on PAPPA function, and that breast cancer cells become more invasive after down-regulation of this protease. PAPPA regulates mitotic progression through modulating the IGF-1 signalling pathway resulting in activation of the forkhead transcription factor FoxM1, which drives a transcriptional cluster of essential mitotic genes. Our results show that PAPPA has a critical function in normal cell division and is targeted early in breast cancer development.Entities:
Keywords: FoxM1; Foxo3a; IGF-1; MitoCheck; PAPPA; breast cancer; cell cycle; epigenetic silencing; mitosis
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Year: 2014 PMID: 24931331 DOI: 10.1002/path.4393
Source DB: PubMed Journal: J Pathol ISSN: 0022-3417 Impact factor: 7.996