Characterization of novel MPS1 inhibitors with preclinical anticancer activity

Jèmaà, Mohamed; Galluzzi, Lorenzo; Kepp, Oliver; Senovilla, Laura; Brands, Michael; Boemer, Ulf; Koppitz, Marcus; Lienau, Philip; Prechtl, Stefan; Schulze, Volker; Siemeister, Gerhard; Wengner, Antje M.; Mumberg, Dominik; Ziegelbauer, Karl; Abrieu, Ariane; Castedo, Maria; Vitale, Ilio

doi:10.1038/cdd.2013.105

Cited by 99 publications

(128 citation statements)

References 60 publications

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“…Furthermore, MPS1 is also required for chromosome alignment and error correction (3)(4)(5). Thus, following the inhibition of MPS1 kinase activity, cells prematurely exit mitosis with mis-attached/unaligned chromosomes, which causes severe chromosome mis-segregation, aneuploidy, and cell death (6)(7)(8)(9)(10).…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, breast cancer cell lines deficient in the tumor-suppressor protein PTEN have been reported to be more sensitive to MPS1 depletion or kinase inhibition (18). As a result, MPS1 has attracted considerable attention as a potential drug target for anticancer therapy, with a number of small-molecule inhibitors recently identified and under development (6)(7)(8)(9)(10)19), or entering the clinic (BAY-1161909; clinical trial ID NCT02138812).…”

Section: Introductionmentioning

confidence: 99%

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Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

et al. 2015

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Acquired resistance to therapy is perhaps the greatest challenge to effective clinical management of cancer. With several inhibitors of the mitotic checkpoint kinase MPS1 in preclinical development, we sought to investigate how resistance against these inhibitors may arise so that mitigation or bypass strategies could be addressed as early as possible. Toward this end, we modeled acquired resistance to the MPS1 inhibitors AZ3146, NMS-P715, and CCT251455, identifying five point mutations in the kinase domain of MPS1 that confer resistance against multiple inhibitors. Structural studies showed how the MPS1 mutants conferred resistance by causing steric hindrance to inhibitor binding. Notably, we show that these mutations occur in nontreated cancer cell lines and primary tumor specimens, and that they also preexist in normal lymphoblast and breast tissues. In a parallel piece of work, we also show that the EGFR p.T790M mutation, the most common mutation conferring resistance to the EGFR inhibitor gefitinib, also preexists in cancer cells and normal tissue. Our results therefore suggest that mutations conferring resistance to targeted therapy occur naturally in normal and malignant cells and these mutations do not arise as a result of the increased mutagenic plasticity of cancer cells. Cancer Res; 75(16); 3340-54. Ó2015 AACR.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

et al. 2015

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“…CFI-402257 shows strong antineoplastic activity on a broad panel of human cancer-derived cell lines, and causes effects consistent with depletion or inhibition of Mps1 (4,(9)(10)(11)(12). Oral administration of CFI-402257 as a single agent to mice bearing human cancer xenografts results in inhibition of tumor growth at doses that are well-tolerated.…”

mentioning

confidence: 99%

“…Mps1 is also required for chromosome alignment and error correction (6)(7)(8). Inhibition of Mps1 activity causes cells to prematurely exit mitosis with unattached chromosomes, resulting in severe chromosome missegregation, aneuploidy, and ultimately cell death (4,(9)(10)(11)(12). Mps1 is expressed during mitosis in proliferating cells.…”

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confidence: 99%

Functional characterization of CFI-402257, a potent and selective Mps1/TTK kinase inhibitor, for the treatment of cancer

Mason

Wei

Fletcher

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

103

120

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Loss of cell-cycle control is a hallmark of human cancer. Cell-cycle checkpoints are essential for maintaining genome integrity and balanced growth and division. They are specifically deregulated in cancer cells and contain regulators that represent potential therapeutic targets. Monopolar spindle 1 (Mps1; also known as TTK protein kinase) is a core component of the spindle assembly checkpoint (SAC), a genome-surveillance mechanism that is important for cell survival, and has emerged as a candidate target for anticancer therapy. Here, we report the cellular and antitumor effects of CFI-402257, a potent (Mps1 K i = 0.09 ± 0.02 nM; cellular Mps1 EC 50 = 6.5 ± 0.5 nM), highly selective, and orally active small-molecule inhibitor of Mps1 that was identified through a drug-discovery program. Human cancer cells treated with CFI-402257 exhibit effects consistent with Mps1 kinase inhibition, specifically SAC inactivation, leading to chromosome missegregation, aneuploidy, and ultimately cell death. Oral administration of CFI-402257 in monotherapy or in combination with an anti-programmed cell death 1 (PD-1) antibody in mouse models of human cancer results in inhibition of tumor growth at doses that are well-tolerated. Our findings provide a rationale for the clinical evaluation of CFI-402257 in patients with solid tumors.Mps1/TTK | inhibitor | CFI-402257 | cancer

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“…Among these compounds, NMS-P715, MPI-0479605, Mps-BAY2b and Mps1-IN-3 showed promising results in pre-clinical studies with rodent xenograft models. [12][13][14][15] Apart from these pre-clinical compounds, the small-molecule Mps1 inhibitors reversine and AZ3146 have drawn attention as important tools to decipher Mps1 functions in mitosis. 10,16,17 The strategy of targeting kinases with small-molecule kinase inhibitors in cancer therapy has been specifically successful to treat cells overexpressing or containing hyperactivated alleles of the tyrosine kinases BCR-ABL and epidermal growth factor receptor (EGFR) (reviewed in Barouch-Bentov and Sauer 18 ).…”

Section: Introductionmentioning

confidence: 99%

Predicting drug resistance before it occurs

Behjati

2015

Sci. Transl. Med.

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A Koch, A Maia, A Janssen 1 and RH MedemaMps1/TTK is a dual-specificity kinase, with an essential role in mitotic checkpoint signaling, which has emerged as a potential target in cancer therapy. Several Mps1/TTK small-molecule inhibitors have been described that exhibit promising activity in cell culture and xenograft models. Here, we investigated whether cancer cells can develop resistance to these drugs. To this end, we treated various cancer cell lines with sublethal concentrations of a potent Mps1/TTK inhibitor in order to isolate inhibitor-resistant monoclonal cell lines. We identified four point mutations in the catalytic domain of Mps1/TTK that gave rise to inhibitor resistance but retained wildtype catalytic activity. Interestingly, cross-resistance of the identified mutations to other Mps1/TTK inhibitors is limited. Our studies predict that Mps1/TTK inhibitor-resistant tumor cells can arise through the acquisition of mutations in the adenosine triphosphatebinding pocket of the kinase that prevent stable binding of the inhibitors. In addition, our results suggest that combinations of inhibitors could be used to prevent acquisition of drug resistance. Interestingly, cross-resistance seems nonspecific for inhibitor scaffolds, a notion that can be exploited in future drug design to evict possible resistance mutations during clinical treatment.

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Characterization of novel MPS1 inhibitors with preclinical anticancer activity

Cited by 99 publications

References 60 publications

Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Functional characterization of CFI-402257, a potent and selective Mps1/TTK kinase inhibitor, for the treatment of cancer

Predicting drug resistance before it occurs

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