Biomedical Science and Engineering Interdisciplinary Program, Korea Advanced Institute of Science and Technology (KAIST), Daejeon, Republic of Korea.
Center for Vascular Research, Institute for Basic Science, Daejeon, Republic of Korea.
Int J Radiat Oncol Biol Phys. 2018 Nov 1;102(3):609-618. doi: 10.1016/j.ijrobp.2018.06.401. Epub 2018 Jul 11.
Several clinical trials have combined antiangiogenic agents and radiation therapy (RT), but evidence of its clinical benefit is insufficient. In this study, we rationalized and investigated the combination of vascular endothelial growth factor-Grab (VEGF-Grab), an antiangiogenic drug that inhibits VEGF-A and placental growth factor (PlGF) and radiotherapy for anti-cancer therapy.
To observe for changes in PlGF after radiation, HCT116, HCT15, SW480, BxPC3, and RAW264.7 cells and Lewis lung carcinoma (LLC) and BxPC3 tumors were given 10 Gy of radiation, and changes in the expression of PlGF were analyzed. Patients scheduled for RT for solid tumor mass were recruited, and their plasma VEGF-A and PlGF were analyzed at baseline and 2 and 4 weeks after the start of radiotherapy. To assess the effects of combining VEGF-Grab and radiotherapy, mice bearing LLC tumors were given 10 Gy of radiation once and 25 mg/kg of VEGF-Grab every 2 days for 5 rounds. To show that VEGF-Grab is effective in human tumors, mice bearing BxPC3 xenografts were given 2 doses of 15 mg/kg of VEGF-Grab or VEGF-Trap. To assess the efficacy of combination therapy in BxPC3 xenografts, the same experiment used in the LLC model was performed.
We demonstrated that PlGF is increased as a direct consequence of irradiation in vitro and in vivo and in the plasma of patients being treated with radiation. Using a syngeneic tumor model, we showed that the combination of VEGF-Grab and RT most effectively inhibited tumor growth through antiangiogenesis, tumor vessel normalization, and tumor-associated macrophage polarization from protumorigenic M2-type to antitumorigenic M1-type. Finally, we demonstrated similar enhanced antitumor effects using a human xenograft model.
This study shows that PlGF is a potential target in patients being treated with RT and suggests VEGF-Grab as a viable therapeutic option in the context of inhibiting secondarily activated pathways responsible for tumor recurrence.
几项临床试验将抗血管生成药物与放射治疗(RT)联合应用,但临床获益的证据不足。本研究旨在合理设计并探讨血管内皮生长因子-Grab(VEGF-Grab)与放疗联合治疗癌症的效果,VEGF-Grab 是一种抗血管生成药物,可抑制 VEGF-A 和胎盘生长因子(PlGF)。
为观察辐射后 PlGF 的变化,我们对 HCT116、HCT15、SW480、BxPC3 和 RAW264.7 细胞以及 Lewis 肺癌(LLC)和 BxPC3 肿瘤进行了 10 Gy 的照射,并分析 PlGF 的表达变化。招募计划接受实体瘤放射治疗的患者,在基线和放射治疗开始后 2 周和 4 周时分析其血浆 VEGF-A 和 PlGF。为评估 VEGF-Grab 与放疗联合应用的效果,我们对荷 LLC 肿瘤的小鼠单次给予 10 Gy 照射,并每 2 天给予 25mg/kg 的 VEGF-Grab 共 5 轮。为证明 VEGF-Grab 对人肿瘤有效,我们对荷 BxPC3 异种移植瘤的小鼠给予 2 次 15mg/kg 的 VEGF-Grab 或 VEGF-Trap。为评估联合治疗在 BxPC3 异种移植瘤中的疗效,我们在 LLC 模型中进行了相同的实验。
我们证明了 PlGF 是照射后体外和体内以及接受放疗的患者血浆中直接增加的,使用同种异体肿瘤模型,我们表明 VEGF-Grab 与 RT 的联合最有效地通过抗血管生成、肿瘤血管正常化以及肿瘤相关巨噬细胞从促肿瘤 M2 型向抗肿瘤 M1 型极化来抑制肿瘤生长。最后,我们在人异种移植瘤模型中也证明了类似的增强抗肿瘤作用。
本研究表明 PlGF 是接受 RT 治疗的患者的一个潜在靶点,并提示 VEGF-Grab 是抑制继发激活的导致肿瘤复发的途径的可行治疗选择。
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