Murakami Takashi, Li Shukuan, Han Qinghong, Tan Yuying, Kiyuna Tasuku, Igarashi Kentaro, Kawaguchi Kei, Hwang Ho Kyoung, Miyake Kentaro, Singh Arun S, Nelson Scott D, Dry Sarah M, Li Yunfeng, Hiroshima Yukihiko, Lwin Thinzar M, DeLong Jonathan C, Chishima Takashi, Tanaka Kuniya, Bouvet Michael, Endo Itaru, Eilber Fritz C, Hoffman Robert M
AntiCancer, Inc., San Diego, California, USA.
Department of Surgery, University of California, San Diego, California, USA.
Oncotarget. 2017 May 30;8(22):35630-35638. doi: 10.18632/oncotarget.15823.
Methionine dependence is due to the overuse of methionine for aberrant transmethylation reactions in cancer. Methionine dependence may be the only general metabolic defect in cancer. In order to exploit methionine dependence for therapy, our laboratory previously cloned L-methionine α-deamino-γ-mercaptomethane lyase [EC 4.4.1.11]). The cloned methioninase, termed recombinant methioninase, or rMETase, has been tested in mouse models of human cancer cell lines. Ewing's sarcoma is recalcitrant disease even though development of multimodal therapy has improved patients'outcome. Here we report efficacy of rMETase against Ewing's sarcoma in a patient-derived orthotopic xenograft (PDOX) model. The Ewing's sarcoma was implanted in the right chest wall of nude mice to establish a PDOX model. Eight Ewing's sarcoma PDOX mice were randomized into untreated control group (n = 4) and rMETase treatment group (n = 4). rMETase (100 units) was injected intraperitoneally (i.p.) every 24 hours for 14 consecutive days. All mice were sacrificed on day-15, 24 hours after the last rMETase administration. rMETase effectively reduced tumor growth compared to untreated control. The methionine level both of plasma and supernatants derived from sonicated tumors was lower in the rMETase group. Body weight did not significantly differ at any time points between the 2 groups. The present study is the first demonstrating rMETase efficacy in a PDOX model, suggesting potential clinical development, especially in recalcitrant cancers such as Ewing's sarcoma.
甲硫氨酸依赖性是由于癌症中异常转甲基化反应对甲硫氨酸的过度使用所致。甲硫氨酸依赖性可能是癌症中唯一普遍存在的代谢缺陷。为了利用甲硫氨酸依赖性进行治疗,我们实验室先前克隆了L-甲硫氨酸α-脱氨基-γ-巯基甲烷裂解酶[EC 4.4.1.11])。克隆的甲硫氨酸酶,称为重组甲硫氨酸酶或rMETase,已在人癌细胞系的小鼠模型中进行了测试。尽管多模式治疗的发展改善了患者的预后,但尤因肉瘤仍然是一种难治性疾病。在此,我们报告了rMETase在患者来源的原位异种移植(PDOX)模型中对尤因肉瘤的疗效。将尤因肉瘤植入裸鼠的右胸壁以建立PDOX模型。八只尤因肉瘤PDOX小鼠被随机分为未治疗的对照组(n = 4)和rMETase治疗组(n = 4)。连续14天,每24小时腹腔注射(i.p.)rMETase(100单位)。在最后一次注射rMETase后24小时,即第15天处死所有小鼠。与未治疗的对照组相比,rMETase有效地抑制了肿瘤生长。rMETase组血浆和超声处理后的肿瘤上清液中的甲硫氨酸水平均较低。两组在任何时间点的体重均无显著差异。本研究首次证明了rMETase在PDOX模型中的疗效,表明其具有潜在的临床开发价值,尤其是在尤因肉瘤等难治性癌症中。
