Selective inhibition of pancreatic ductal adenocarcinoma cell growth by the mitotic MPS1 kinase inhibitor NMS-P715

dc.contributor.authorSlee, Roger B.
dc.contributor.authorGrimes, Brenda R.
dc.contributor.authorBansal, Ruchi
dc.contributor.authorGore, Jesse
dc.contributor.authorBlackburn, Corinne
dc.contributor.authorBrown, Lyndsey
dc.contributor.authorGasaway, Rachel
dc.contributor.authorJeong, Jaesik
dc.contributor.authorVictorino, Jose
dc.contributor.authorMarch, Keith L.
dc.contributor.authorColombo, Riccardo
dc.contributor.authorHerbert, Brittney-Shea
dc.contributor.authorKorc, Murray
dc.contributor.departmentDepartment of Medical and Molecular Genetics, IU School of Medicineen_US
dc.date.accessioned2016-05-02T19:46:11Z
dc.date.available2016-05-02T19:46:11Z
dc.date.issued2014-02
dc.description.abstractMost solid tumors, including pancreatic ductal adenocarcinoma (PDAC), exhibit structural and numerical chromosome instability (CIN). Although often implicated as a driver of tumor progression and drug resistance, CIN also reduces cell fitness and poses a vulnerability that can be exploited therapeutically. The spindle assembly checkpoint (SAC) ensures correct chromosome-microtubule attachment, thereby minimizing chromosome segregation errors. Many tumors exhibit upregulation of SAC components such as MPS1, which may help contain CIN within survivable limits. Prior studies showed that MPS1 inhibition with the small molecule NMS-P715 limits tumor growth in xenograft models. In cancer cell lines, NMS-P715 causes cell death associated with impaired SAC function and increased chromosome missegregation. Although normal cells appeared more resistant, effects on stem cells, which are the dose-limiting toxicity of most chemotherapeutics, were not examined. Elevated expression of 70 genes (CIN70), including MPS1, provides a surrogate measure of CIN and predicts poor patient survival in multiple tumor types. Our new findings show that the degree of CIN70 upregulation varies considerably among PDAC tumors, with higher CIN70 gene expression predictive of poor outcome. We identified a 25 gene subset (PDAC CIN25) whose overexpression was most strongly correlated with poor survival and included MPS1. In vitro, growth of human and murine PDAC cells is inhibited by NMS-P715 treatment, whereas adipose-derived human mesenchymal stem cells are relatively resistant and maintain chromosome stability upon exposure to NMS-P715. These studies suggest that NMS-P715 could have a favorable therapeutic index and warrant further investigation of MPS1 inhibition as a new PDAC treatment strategy.en_US
dc.eprint.versionAuthor's manuscripten_US
dc.identifier.citationSlee, R. B., Grimes, B. R., Bansal, R., Gore, J., Blackburn, C., Brown, L., … Korc, M. (2014). Selective inhibition of pancreatic ductal adenocarcinoma cell growth by the mitotic MPS1 kinase inhibitor, NMS-P715. Molecular Cancer Therapeutics, 13(2), 307–315. http://doi.org/10.1158/1535-7163.MCT-13-0324en_US
dc.identifier.issn1538-8514en_US
dc.identifier.urihttps://hdl.handle.net/1805/9494
dc.language.isoen_USen_US
dc.publisherAmerican Association for Cancer Researchen_US
dc.relation.isversionof10.1158/1535-7163.MCT-13-0324en_US
dc.relation.journalMolecular Cancer Therapeuticsen_US
dc.rightsPublisher Policyen_US
dc.sourcePMCen_US
dc.subjectCell Cycle Proteinsen_US
dc.subjectantagonists & inhibitorsen_US
dc.subjectCell Proliferationen_US
dc.subjectdrug effectsen_US
dc.subjectProtein-Tyrosine Kinasesen_US
dc.subjectPyrazolesen_US
dc.subjectpharmacologyen_US
dc.titleSelective inhibition of pancreatic ductal adenocarcinoma cell growth by the mitotic MPS1 kinase inhibitor NMS-P715en_US
dc.typeArticleen_US
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