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NMS-P937, an Orally Available, Specific Small-Molecule Polo-like Kinase 1 Inhibitor with Antitumor Activity in Solid and Hematologic Malignancies

PLK1 癌症研究 药理学 激酶 Polo样激酶 有丝分裂 细胞周期检查点 个人识别码1 癌症 医学 生物 细胞周期 内科学 丝氨酸 生物化学 细胞生物学
作者
Barbara Valsasina,Italo Beria,Cristina Alli,Rachele Alzani,Nilla Avanzi,Dario Ballinari,Paolo Cappella,Michele Caruso,Alessia Casolaro,Antonella Ciavolella,Ulisse Cucchi,Anna De Ponti,E. Felder,Francesco Fiorentini,Arturo Galvani,Laura Gianellini,Maria Laura Giorgini,Antonella Isacchi,J. Lansen,Enrico Pesenti,Simona Rizzi,Maurizio Rocchetti,Francesco Sola,Jürgen Moll
出处
期刊:Molecular Cancer Therapeutics [American Association for Cancer Research]
卷期号:11 (4): 1006-1016 被引量:91
标识
DOI:10.1158/1535-7163.mct-11-0765
摘要

Polo-like kinase 1 (PLK1) is a serine/threonine protein kinase considered to be the master player of cell-cycle regulation during mitosis. It is indeed involved in centrosome maturation, bipolar spindle formation, chromosome separation, and cytokinesis. PLK1 is overexpressed in a variety of human tumors and its overexpression often correlates with poor prognosis. Although five different PLKs are described in humans, depletion or inhibition of kinase activity of PLK1 is sufficient to induce cell-cycle arrest and apoptosis in cancer cell lines and in xenograft tumor models. NMS-P937 is a novel, orally available PLK1-specific inhibitor. The compound shows high potency in proliferation assays having low nanomolar activity on a large number of cell lines, both from solid and hematologic tumors. NMS-P937 potently causes a mitotic cell-cycle arrest followed by apoptosis in cancer cell lines and inhibits xenograft tumor growth with clear PLK1-related mechanism of action at well-tolerated doses in mice after oral administration. In addition, NMS-P937 shows potential for combination in clinical settings with approved cytotoxic drugs, causing tumor regression in HT29 human colon adenocarcinoma xenografts upon combination with irinotecan and prolonged survival of animals in a disseminated model of acute myelogenous leukemia in combination with cytarabine. NMS-P937, with its favorable pharmacologic parameters, good oral bioavailability in rodent and nonrodent species, and proven antitumor activity in different preclinical models using a variety of dosing regimens, potentially provides a high degree of flexibility in dosing schedules and warrants investigation in clinical settings.

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