| Literature DB >> 24648944 |
Kiyoko Umene1, Kouji Banno1, Iori Kisu1, Megumi Yanokura1, Yuya Nogami1, Kosuke Tsuji1, Kenta Masuda1, Arisa Ueki1, Yusuke Kobayashi1, Wataru Yamagami1, Hiroyuki Nomura1, Eiichiro Tominaga1, Nobuyuki Susumu1, Daisuke Aoki1.
Abstract
Chemotherapy and surgery are important treatment strategies for gynecologic malignant tumors such as ovarian, cervical and endometrial cancer. However, many anticancer drugs currently available are cytotoxic and cause strong adverse reactions in patients. Aurora kinases have attracted increasing attention in recent years as serine/threonine kinases with various roles in cell division, including chromosomal agglutination and segregation, functions of centromeres, centrosomal maturation, spindle formation and cytokinesis. Aurora kinases are overexpressed in a number of cancers and recent studies have shown that they are involved in onco genesis and cause an aberrant increase in centrosome number, emergence of polykaryocytes and failure of cancer inhibition mechanisms. Thus, drugs that inhibit Aurora kinases are likely to exert anticancer effects in various fields, including the gynecologic field. Aurora kinase inhibitors exert antitumor effects in monotherapy and synergistic effects in combination therapy with taxane-based anticancer agents for gynecologic tumors and are likely to increase the efficacy of existing anticancer drugs. Current Aurora kinase inhibitors include ZM447439, Hesperadin, VX-680/MK-0457, AT9283 and Barasertib, and clinical trials are ongoing to verify the effects of these inhibitors.Entities:
Keywords: Aurora kinase A; Aurora kinase inhibitor; VX-680; ZM447439; gynecologic cancer; hesperadin
Year: 2013 PMID: 24648944 PMCID: PMC3917679 DOI: 10.3892/br.2013.91
Source DB: PubMed Journal: Biomed Rep ISSN: 2049-9434