K858, a Novel Inhibitor of Mitotic Kinesin Eg5 and Antitumor Agent, Induces Cell Death in Cancer Cells

Nakai, Ryuichiro; Iida, Susumu; Takahashi, Takeshi; Tsujita, Tetsuya; Okamoto, Seiho; Takada, Chie; Akasaka, Kazuhito; Ichikawa, S.; Ishida, Hiroyuki; Kusaka, Hideaki; Akinaga, Shiro; Murakata, Chikara; Honda, Shoji; Nitta, Masayuki; Saya, Hideyuki; Yamashita, Yoshihisa

doi:10.1158/0008-5472.can-08-4373

Cited by 84 publications

(72 citation statements)

References 36 publications

(47 reference statements)

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“…Sources of the cancer cell lines used for the in vivo xenograft tumor model studies at Kyowa Hakko Kirin as summarized in Table 1 1998. These cancer cell lines at Kyowa Hakko Kirin were not authenticated and were maintained as previously described (32).…”

Section: Cancer Cell Lines Reagents and Treatmentsmentioning

confidence: 99%

“…RNAi, compound handling and treatment, immunoblotting, flow cytometry, and immunofluorescence microscopy were performed as previously described (32,33). Assays for ATPase activity of kinesins and in vitro microtubule polymerization and depolymerization were also done as previously described (32).…”

Section: Cancer Cell Lines Reagents and Treatmentsmentioning

confidence: 99%

“…Assays for ATPase activity of kinesins and in vitro microtubule polymerization and depolymerization were also done as previously described (32).…”

Section: Cancer Cell Lines Reagents and Treatmentsmentioning

confidence: 99%

“…Antitumor efficacy in subcutaneous xenograft tumor-bearing mice with 10 mice per treatment group from either established cancer cell lines or fragments of human tumor explants was evaluated as tumor volume by serial caliper measurements and was calculated as described previously (32,34). The p388 syngeneic tumor model was developed for high-content imaging analysis using female BDF1 mice, weighing 20 to 23 g, which were purchased from Charles River and acclimated in-house for one week before their use in experiments.…”

Section: Animal Models and In Vivo Pharmacologymentioning

confidence: 99%

“…We describe here the discovery and characterization of LY2523355, a selective allosteric inhibitor of human Eg5, derived through an extensive structure-activity relationship program from a precursor compound identified by a phenotype-based screening for mitotic arrest of HCT116 cells (32). We demonstrate that inhibition of Eg5 in cancer cells by LY2523355 causes rapid apoptosis following SAC-dependent mitotic arrest.…”

Section: Introductionmentioning

confidence: 99%

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A Novel Eg5 Inhibitor (LY2523355) Causes Mitotic Arrest and Apoptosis in Cancer Cells and Shows Potent Antitumor Activity in Xenograft Tumor Models

Fan

Horn

et al. 2015

Molecular Cancer Therapeutics

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Intervention of cancer cell mitosis by antitubulin drugs is among the most effective cancer chemotherapies. However, antitubulin drugs have dose-limiting side effects due to important functions of microtubules in resting normal cells and are often rendered ineffective by rapid emergence of resistance. Antimitotic agents with different mechanisms of action and improved safety profiles are needed as new treatment options. Mitosis-specific kinesin Eg5 represents an attractive anticancer target for discovering such new antimitotic agents, because Eg5 is essential only in mitotic progression and has no roles in resting, nondividing cells. Here, we show that a novel selective Eg5 inhibitor, LY2523355, has broad target-mediated anticancer activity in vitro and in vivo. LY2523355 arrests cancer cells at mitosis and causes rapid cell death that requires sustained spindle-assembly checkpoint (SAC) activation with a required threshold concentration. In vivo efficacy of LY2523355 is highly dose/schedule-dependent, achieving complete remission in a number of xenograft tumor models, including patient-derived xenograft (PDX) tumor models. We further establish that histone-H3 phosphorylation of tumor and proliferating skin cells is a promising pharmacodynamic biomarker for in vivo anticancer activity of LY2523355.

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Section: Cancer Cell Lines Reagents and Treatmentsmentioning

confidence: 99%

Section: Cancer Cell Lines Reagents and Treatmentsmentioning

confidence: 99%

“…Assays for ATPase activity of kinesins and in vitro microtubule polymerization and depolymerization were also done as previously described (32).…”

Section: Cancer Cell Lines Reagents and Treatmentsmentioning

confidence: 99%

Section: Animal Models and In Vivo Pharmacologymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A Novel Eg5 Inhibitor (LY2523355) Causes Mitotic Arrest and Apoptosis in Cancer Cells and Shows Potent Antitumor Activity in Xenograft Tumor Models

Fan

Horn

et al. 2015

Molecular Cancer Therapeutics

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Design, Synthesis, and Evaluation of Biological Activity of Ferrocene‐Ispinesib Hybrids: Impact of a Ferrocenyl Group on the Antiproliferative and Kinesin Spindle Protein Inhibitory Activity

Kowalczyk

Błauż

Ayine-Tora

et al. 2023

Chemistry A European J

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With the aim to combine more than one biologically-active component in a single molecule, derivatives of ispinesib and its (S) analogue were prepared that featured ferrocenyl moieties or bulky organic substituents. Inspired by the strong kinesin spindle protein (KSP) inhibitory activity of ispinesib, the compounds were investigated for their antiproliferative activity. Among these compounds, several derivatives demonstrated significantly higher antiproliferative activity than ispinesib with nanomolar IC 50 values against cell lines. Further evaluation indicated that the antiproliferative activity is not directly correlated with their KSP inhibitory activity while docking suggested that several of the derivatives may bind in a manner similar to ispinesib. In order to investigate the mode of action further, cell cycle analysis and reactive oxygen species formation were investigated. The improved antiproliferative activity of the most active compounds may be assigned to synergic effects of various factors such as KSP inhibitory activity due to the ispinesib core and ability to generate ROS and induce mitotic arrest.

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Kinesin Spindle Protein (KSP) Inhibitors in Combination with Chemotherapeutic Agents for Cancer Therapy

et al. 2013

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A diverse group of proteins, the activities of which are precisely orchestrated during mitosis, have emerged as targets for cancer therapeutics; these include the Aurora kinases (AKs), Polo-like kinases (PLKs), and the kinesin spindle protein (KSP). KSP is essential for the proper separation of spindle poles during mitosis. Agents that target KSP selectively act on cells undergoing cell division, which means that KSP inhibitors are mitosis-specific drugs, and have demonstrated remarkable activities in vitro. However, a significant obstacle to the success of KSP inhibitors is that these compounds, with tremendous efficacy in vitro, have demonstrated little or even no antitumor activity in vivo. Accumulated data suggest that a combination of KSP inhibitors with various cytostatic drugs will result in a more powerful tumor-killing effect than monotherapy. Combination therapies might predominate and represent the next frontier in the discovery research of KSP inhibitors as potential anticancer drugs. Few published studies have reviewed combination therapy using KSP inhibitors. Herein we provide a comprehensive review of the literature on KSP inhibitor monotherapy and therapeutic combinations. The current state and problems are also discussed.

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K858, a Novel Inhibitor of Mitotic Kinesin Eg5 and Antitumor Agent, Induces Cell Death in Cancer Cells

Cited by 84 publications

References 36 publications

A Novel Eg5 Inhibitor (LY2523355) Causes Mitotic Arrest and Apoptosis in Cancer Cells and Shows Potent Antitumor Activity in Xenograft Tumor Models

A Novel Eg5 Inhibitor (LY2523355) Causes Mitotic Arrest and Apoptosis in Cancer Cells and Shows Potent Antitumor Activity in Xenograft Tumor Models

Design, Synthesis, and Evaluation of Biological Activity of Ferrocene‐Ispinesib Hybrids: Impact of a Ferrocenyl Group on the Antiproliferative and Kinesin Spindle Protein Inhibitory Activity

Kinesin Spindle Protein (KSP) Inhibitors in Combination with Chemotherapeutic Agents for Cancer Therapy

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