Babichev Yael, Kabaroff Leah, Datti Alessandro, Uehling David, Isaac Methvin, Al-Awar Rima, Prakesch Michael, Sun Ren X, Boutros Paul C, Venier Rosemarie, Dickson Brendan C, Gladdy Rebecca A
Lunenfeld-Tanenbaum Research Institute, Mount Sinai Hospital, Toronto, M5G 1X5, Canada.
Sinai-McLaughlin Assay and Robotic Technologies Facility, Lunenfeld-Tanenbaum Research Institute, Toronto, M5G 1X5, Canada.
J Transl Med. 2016 Mar 8;14:67. doi: 10.1186/s12967-016-0814-z.
Leiomyosarcoma (LMS) is a common type of soft tissue sarcoma that responds poorly to standard chemotherapy. Thus the goal of this study was to identify novel selective therapies that may be effective in leiomyosarcoma by screening cell lines with a small molecule library comprised of 480 kinase inhibitors to functionally determine which signalling pathways may be critical for LMS growth.
LMS cell lines were screened with the OICR kinase library and a cell viability assay was used to identify potentially effective compounds. The top 10 % of hits underwent secondary validation to determine their EC50 and immunoblots were performed to confirm selective drug action. The efficacy of combination drug therapy with doxorubicin (Dox) in vitro was analyzed using the Calcusyn program after treatment with one of three dosing schedules: concurrent treatment, initial treatment with a selective compound followed by Dox, or initial treatment with Dox followed by the selective compound. Single and combination drug therapy were then validated in vivo using LMS xenografts.
Compounds that targeted PI3K/AKT/mTOR pathways (52 %) were most effective. EC50s were determined to validate these initial hits, and of the 11 confirmed hits, 10 targeted PI3K and/or mTOR pathways with EC50 values <1 μM. We therefore examined if BEZ235 and BKM120, two selective compounds in these pathways, would inhibit leiomyosarcoma growth in vitro. Immunoblots confirmed on-target effects of these compounds in the PI3K and/or mTOR pathways. We next investigated if there was synergy with these agents and first line chemotherapy doxorubicin (Dox), which would allow for earlier introduction into patient care. Only combined treatment of BEZ235 and Dox was synergistic in vitro. To validate these findings in pre-clinical models, leiomyosarcoma xenografts were treated with single agent and combination therapy. BEZ235 treated xenografts (n = 8) demonstrated a decrease in tumor volume of 42 % whereas combining BEZ235 with Dox (n = 8) decreased tumor volume 68 % compared to vehicle alone.
In summary, this study supports further investigation into the use of PI3K and mTOR inhibitors alone and in combination with standard treatment in leiomyosarcoma patients.
平滑肌肉瘤(LMS)是一种常见的软组织肉瘤,对标准化疗反应不佳。因此,本研究的目的是通过用包含480种激酶抑制剂的小分子文库筛选细胞系,以功能确定哪些信号通路可能对LMS生长至关重要,从而鉴定出可能对平滑肌肉瘤有效的新型选择性疗法。
用OICR激酶文库筛选LMS细胞系,并使用细胞活力测定法鉴定潜在有效的化合物。对排名前10%的命中化合物进行二次验证以确定其半数有效浓度(EC50),并进行免疫印迹以确认选择性药物作用。在用三种给药方案之一治疗后,使用Calcusyn程序分析阿霉素(Dox)联合药物疗法在体外的疗效:同时治疗、先用选择性化合物治疗后用Dox、或先用Dox治疗后用选择性化合物。然后使用LMS异种移植在体内验证单药和联合药物疗法。
靶向PI3K/AKT/mTOR通路的化合物(52%)最有效。确定EC50以验证这些初始命中化合物,在11种经确认的命中化合物中,10种靶向PI3K和/或mTOR通路,EC50值<1μM。因此,我们研究了这些通路中的两种选择性化合物BEZ235和BKM120是否会在体外抑制平滑肌肉瘤生长。免疫印迹证实了这些化合物在PI3K和/或mTOR通路中的靶向作用。接下来,我们研究了这些药物与一线化疗药物阿霉素(Dox)是否存在协同作用,这将允许更早地应用于患者治疗。仅BEZ235和Dox的联合治疗在体外具有协同作用。为了在临床前模型中验证这些发现,用单药和联合疗法治疗平滑肌肉瘤异种移植。接受BEZ2治疗的异种移植瘤(n = 8)肿瘤体积减少42%,而将BEZ235与Dox联合使用(n = 8)与单独使用载体相比,肿瘤体积减少68%。
总之,本研究支持进一步研究单独使用PI3K和mTOR抑制剂以及与平滑肌肉瘤患者的标准治疗联合使用。
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