一种基因工程的溶瘤腺病毒可以诱骗并在 S/G2/M 期使静止的癌症干细胞样细胞致死性地陷入陷阱。
A genetically engineered oncolytic adenovirus decoys and lethally traps quiescent cancer stem-like cells in S/G2/M phases.
机构信息
Authors' Affiliations: Department of Gastroenterological Surgery, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences; Center for innovative clinical medicine, Okayama University Hospital, Okayama; Oncolys BioPharma, Inc., Tokyo, Japan; Department of Surgery, University of California San Diego; and AntiCancer, Inc., San Diego, California.
出版信息
Clin Cancer Res. 2013 Dec 1;19(23):6495-505. doi: 10.1158/1078-0432.CCR-13-0742. Epub 2013 Sep 30.
PURPOSE
Because chemoradiotherapy selectively targets proliferating cancer cells, quiescent cancer stem-like cells are resistant. Mobilization of the cell cycle in quiescent leukemia stem cells sensitizes them to cell death signals. However, it is unclear that mobilization of the cell cycle can eliminate quiescent cancer stem-like cells in solid cancers. Thus, we explored the use of a genetically-engineered telomerase-specific oncolytic adenovirus, OBP-301, to mobilize the cell cycle and kill quiescent cancer stem-like cells.
EXPERIMENTAL DESIGN
We established CD133(+) cancer stem-like cells from human gastric cancer MKN45 and MKN7 cells. We investigated the efficacy of OBP-301 against quiescent cancer stem-like cells. We visualized the treatment dynamics of OBP-301 killing of quiescent cancer stem-like cells in dormant tumor spheres and xenografts using a fluorescent ubiquitination cell-cycle indicator (FUCCI).
RESULTS
CD133(+) gastric cancer cells had stemness properties. OBP-301 efficiently killed CD133(+) cancer stem-like cells resistant to chemoradiotherapy. OBP-301 induced cell-cycle mobilization from G0-G1 to S/G2/M phases and subsequent cell death in quiescent CD133(+) cancer stem-like cells by mobilizing cell-cycle-related proteins. FUCCI enabled visualization of quiescent CD133(+) cancer stem-like cells and proliferating CD133(-) non-cancer stem-like cells. Three-dimensional visualization of the cell-cycle behavior in tumor spheres showed that CD133(+) cancer stem-like cells maintained stemness by remaining in G0-G1 phase. We showed that OBP-301 mobilized quiescent cancer stem-like cells in tumor spheres and xenografts into S/G2/M phases where they lost viability and cancer stem-like cell properties and became chemosensitive.
CONCLUSION
Oncolytic adenoviral infection is an effective mechanism of cancer cell killing in solid cancer and can be a new therapeutic paradigm to eliminate quiescent cancer stem-like cells.
目的
由于放化疗选择性地靶向增殖的癌细胞,静止的癌症干细胞样细胞具有抗性。使静止的白血病干细胞进入细胞周期可使其对细胞死亡信号敏感。然而,尚不清楚使细胞周期活跃是否可以消除实体瘤中的静止癌症干细胞样细胞。因此,我们探索使用一种经过基因工程改造的端粒酶特异性溶瘤腺病毒 OBP-301 来使细胞周期活跃并杀死静止的癌症干细胞样细胞。
实验设计
我们从人胃癌 MKN45 和 MKN7 细胞中建立了 CD133(+)癌症干细胞样细胞。我们研究了 OBP-301 对静止的癌症干细胞样细胞的疗效。我们使用荧光泛素化细胞周期指示剂(FUCCI)可视化 OBP-301 杀死休眠肿瘤球体和异种移植物中静止的癌症干细胞样细胞的治疗动态。
结果
CD133(+)胃癌细胞具有干细胞特性。OBP-301 有效地杀死了对放化疗有抗性的 CD133(+)癌症干细胞样细胞。OBP-301 通过动员细胞周期相关蛋白,将静止的 CD133(+)癌症干细胞样细胞从 G0-G1 期动员到 S/G2/M 期,并随后导致细胞死亡。FUCCI 使静止的 CD133(+)癌症干细胞样细胞和增殖的 CD133(-)非癌症干细胞样细胞可视化。肿瘤球体中细胞周期行为的三维可视化显示,CD133(+)癌症干细胞样细胞通过保持在 G0-G1 期来维持干细胞特性。我们表明,OBP-301 使肿瘤球体和异种移植物中的静止癌症干细胞样细胞进入 S/G2/M 期,在这些阶段它们失去活力和癌症干细胞样细胞特性,并变得对化疗敏感。
结论
溶瘤腺病毒感染是实体瘤中癌细胞杀伤的有效机制,可能成为消除静止癌症干细胞样细胞的新治疗范例。
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